Endocrine Abstracts 9th European Congress of Endocrinology

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28th April – 2 May 2007 Budapest, Hungary
ea of Endocri
9th European Congress
of Endocrinology
9th Euro
April 2007 Volume 14
ISSN 1470-3947 (print) ISSN 1479-68-48 (online)
Budapest - Hungary - 28 April - 2 May
Online version available at
3/29/07 4:11:55 PM
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Endocrine Abstracts
Volume 14
April 2007
9th European Congress of
28 April–2 May 2007, Budapest, Hungary
Abstract Book
9th European Congress of Endocrinology, Budapest, Hungary, 2007
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Endocrine Abstracts (2007) Vol 14
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9th European Congress of Endocrinology, Budapest, Hungary, 2007
9th European Congress of Endocrinology 2007
European Journal of Endocrinology Prize Lecture . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . EJE1
Geoffrey Harris Prize Lecture . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . GH1
Reading beyond the sequence – the plasticity of the LH/CG-LH receptor system . . . . . . . .
Reciprocal regulations of bone and energy metabolisms . . . . . . . . . . . . . . . . . . . . . .
Importance of transporters for cellular entry of thyroid hormone . . . . . . . . . . . . . . . .
Metabolic syndrome: a cultural exercise or clinical entity? . . . . . . . . . . . . . . . . . . . .
The coordination of circadian time in brain and peripheral organs . . . . . . . . . . . . . . . .
Initial work-up & long term follow-up in patients with pheochromocytomas & paragangliomas
Nuclear receptors: from molecular mechanisms to biological functions . . . . . . . . . . . . .
. S1.1– S1.4
. S2.1– S2.4
. S3.1– S3.4
. S4.1– S4.4
. S5.1– S5.4
. S6.1– S6.4
. S7.1– S7.4
. S8.1– S8.4
. S9.1– S9.4
S10.1– S10.4
S11.1– S11.4
S12.1– S12.4
S13.1– S13.4
S14.1– S14.4
S15.1– S15.4
S16.1– S16.4
S17.1– S17.4
S18.1– S18.4
S19.1– S19.4
S20.1– S20.4
S21.1– S21.4
S22.1– S22.4
S23.1– S23.4
S24.1– S24.4
S25.1– S25.4
Hypopituitarism . . . . . . . . . . . . . . . . . . . . . . . . . . . .
Hormones and the brain . . . . . . . . . . . . . . . . . . . . . . .
Signaling and regulation of G-protein-coupled hormone receptors
Gastroenteropancreatic endocrine tumors . . . . . . . . . . . . .
Novel bioactive peptides – lessons from animals . . . . . . . . . .
Diabetes and insulin . . . . . . . . . . . . . . . . . . . . . . . . .
Thyroid cell biology . . . . . . . . . . . . . . . . . . . . . . . . . .
Advances in adrenal hypersecretory disorders . . . . . . . . . . .
Imaging in endocrinology . . . . . . . . . . . . . . . . . . . . . .
GH and prolactin at their targets . . . . . . . . . . . . . . . . . .
Polycystic ovary syndrome . . . . . . . . . . . . . . . . . . . . . .
Hypothalamic network controlling food intake . . . . . . . . . . .
Glucocorticosteroids . . . . . . . . . . . . . . . . . . . . . . . . .
Trojan horses for steroids . . . . . . . . . . . . . . . . . . . . . .
Novel bone hormones and regulators . . . . . . . . . . . . . . . .
Immune-endocrine turmoil of pregnancy . . . . . . . . . . . . . .
Somatostatin receptors in health and disease . . . . . . . . . . . .
Puberty and hypogonadism . . . . . . . . . . . . . . . . . . . . .
Pituitary cell biology . . . . . . . . . . . . . . . . . . . . . . . . .
Thyroid . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . .
Pheromones, odorant and taste receptors . . . . . . . . . . . . . .
Bone . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . .
Reproductive endocrinology/andrology . . . . . . . . . . . . . . .
Obesity . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . .
Novel hormones . . . . . . . . . . . . . . . . . . . . . . . . . . .
MEET THE EXPERT SESSIONS . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . ME1 –ME12
Thyroid clinical . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . OC1.1 – OC1.7
Bone & calcium metabolism . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . OC2.1 – OC2.7
Endocrine tumors & neoplasia . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . OC3.1 – OC3.7
Endocrine Abstracts (2007) Vol 14
9th European Congress of Endocrinology, Budapest, Hungary, 2007
Neuroendocrinology basic . .
Thyroid basic . . . . . . . . .
Cardiovascular endocrinology
Reproductive endocrinology I
Neuroendocrinology clinical .
Signal transduction . . . . . .
Obesity & metabolism . . . .
Reproductive endocrinology II
Diabetes . . . . . . . . . . . .
. . OC4.1 – OC4.7
. . OC5.1 – OC5.7
. . OC6.1 – OC6.7
. . OC7.1 – OC7.7
. . OC8.1 – OC8.7
. . OC9.1 – OC9.7
OC10.1 – OC10.7
OC11.1 – OC11.7
OC12.1 – OC12.7
POSTER PRESENTATIONS . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . P1 –P662
Endocrine Abstracts (2007) Vol 14
9th European Congress of Endocrinology, Budapest, Hungary, 2007
Prize Lectures and
Biographical Notes
Endocrine Abstracts (2007) Vol 14
9th European Congress of Endocrinology, Budapest, Hungary, 2007
European Journal of Endocrinology Prize Lecture
Brian Walker, UK
Brian Walker is Professor of Endocrinology at the University of Edinburgh in Scotland where he is
administrative head of a 60-strong multidisciplinary research group in the Centre for Cardiovascular
He graduated in medicine in Edinburgh in 1986 and completed his clinical training in Glasgow and
Edinburgh. Since 1996 he has practised as an honorary consultant in Diabetes & Endocrinology at the
Western General Hospital in Edinburgh, recently transferring his activities to the Royal Infirmary
following the opening of the Queen’s Medical Research Institute at the new Little France campus.
Brian’s research interest in cortisol and cardiovascular disease began in 1989 as an MRC Training
Fellow, and developed as a Lecturer and British Heart Foundation Senior Research Fellow. The focus of
his group has been on translating findings in animal models into detailed mechanistic experiments in
humans. He published the original studies elucidating the role of 11b-HSD type 1 as a therapeutic target
in obesity and diabetes, and was influential in the studies linking activation of the HPA axis with low
birthweight and adult cardiovascular risk factors.
Previous awards include the Dorothy Hodgkin Lecture from Diabetes UK, the ‘Hot Topic’ Plenary
Lecture at the Nutrition Society, and the Society for Endocrinology Medal.
Endocrine Abstracts (2007) Vol 14
9th European Congress of Endocrinology, Budapest, Hungary, 2007
Cortisol and cardiovascular disease
Brian R Walker
Endocrinology Unit, Centre for Cardiovascular Science,
University of Edinburgh, UK
Similarities between the metabolic syndrome and Cushing’s syndrome, and reversibility of the features
of Cushing’s syndrome, suggest that cortisol may contribute to pathophysiology in both conditions and
that reducing cortisol action may provide a novel therapeutic approach in metabolic syndrome.
There is substantial evidence that circulating cortisol concentrations are higher in people with
hypertension and glucose intolerance. The basis for this activation of the hypothalamic-pituitary-adrenal
(HPA) axis remains uncertain, but it may be attributable to ‘programming’ effects of events in early life
since it is associated with low birth weight.
In people who become obese, intracellular cortisol levels within adipose tissue are further amplified
by increased local re-generation of cortisol by the enzyme 11b-HSD type 1. Recent evidence highlights
the role of nutrition and inflammation in regulating 11b-HSD1 in rodents and in humans. In mice,
transgenic manipulations of 11b-HSD1 have potent effects on obesity and associated features of the
metabolic syndrome. Promising pre-clinical data suggest that novel 11b-HSD1 inhibitors will have a
role in lowering intra-cellular cortisol levels as a treatment for metabolic syndrome.
In addition to their metabolic effects, glucocorticoids act in the blood vessel wall.
Pharmacoepidemiological studies suggest that glucocorticoid excess is an independent risk factor for
cardiovascular disease. Recent data in rodents suggest that 11b-HSD1 within the blood vessel wall
influences vascular remodelling and angiogenesis, for example in the myocardium following coronary
artery occlusion.
Thus, HPA axis hyperactivity may provide a lifelong susceptibility to metabolic syndrome which is
amplified by altered cortisol metabolism in obesity. Glucocorticoid signalling provides a potentially
tractable system to influence both risk factors for, and the outcome of, type 2 diabetes and
cardiovascular disease.
Endocrine Abstracts (2007) Vol 14
9th European Congress of Endocrinology, Budapest, Hungary, 2007
Geoffrey Harris Prize Lecture
Hubert Vaudry, France
Dr Hubert Vaudry is Director of Research at the Institut National de la Santé et de la Recherche
Médicale (INSERM), the French National Institute for Health, and Director of the Laboratory of
Cellular and Molecular Neuroendocrinology at the University of Rouen. He was born in February 1946
in Le Havre, Normandy, and obtained his PhD at the University of Rouen in 1974. He then worked in
Canada for two years as a post-doctoral fellow, at Queen’s University (Kingston, Ontario) and Laval
University (Quebec). He obtained a Doctor of Science degree in 1979 at the University of Rouen and
has developed one of the most productive groups in the field of neuroendocrinology.
Dr Vaudry is involved in a number of International Committees and Advisory Boards. He is the
author of 800 publications in first rank scientific journals and has presented over 1450 communications
or lectures in international congresses. Previous awards include the Descartes-Huygens Prize for
scientific cooperation between France and the Netherlands, and the Prize of the Académie Nationale de
Médecine. He has been appointed as Invited Professor in several Universities including the Catholic
University of Nijmegen, Netherlands (1982–1983), Waseda University in Tokyo, Japan (1986), and the
University of Turin, Italy (1989).
Dr Vaudry is the Chairman of the European Institute for Peptide Research, a major multidisciplinary
institute working in the field of biologically active peptides. He is also the Chairman of the Research
and Education Network for Neuroscience (LARC-Neuroscience network). He is a former President of
the International Federation of Comparative Endocrinology Societies (1997–2001), the European
Society for Comparative Endocrinology (1998–2002) and the Société de Neuroendocrinologie
Endocrine Abstracts (2007) Vol 14
9th European Congress of Endocrinology, Budapest, Hungary, 2007
Neuroendocrine control of steroid biosynthesis within the hypothalamus
Hubert Vaudry1, Jean-Luc Do Rego1, Delphine Beaujean1, Ludovic Galas1, Dan Larhammar2,
Jae Young Seong3, Van Luu-The4, Georges Pelletier4 & Marie-Christine Tonon1, 1INSERM U413,
Univ. Rouen, France, 2Dept Neuroscience, Univ. Uppsala, Sweden, 3Lab. G Protein-Coupled
Receptors, Korea Univ. College of Medicine, Seoul, Korea, 4Lab. Molecular Endocrinology and
Oncology, Laval Univ. Medical Center, Quebec, Canada
Neuroactive steroids synthesized in the brain, referred to as neurosteroids, have gained particular
attention as they appear to be involved in the modulation of various neuroendocrine, behavioral and
pathophysiological processes. Thus, the distribution of steroidogenic enzymes and the identification of
the biochemical pathways leading to neurosteroid formation have now been almost completely
elucidated in various groups of vertebrates. In contrast however, the neuronal mechanisms controlling
the activity of neurosteroid-producing cells in the brain have received little attention. Therefore, we
have investigated the effects of neurotransmitters and neuropeptides on the biosynthesis of
neurosteroids, using the frog brain as an experimental model. We have first observed that steroidsynthesizing neurons express several subunits of the GABAA/central-type benzodiazepine receptor
(CBR) complex, and we have found that GABA, acting through GABAA receptors, inhibits the
synthesis of neurosteroids. We have shown that glial cells containing the octadecaneuropeptide (ODN;
endogenous ligand of CBR)-like immunoreactivity make contact with neurosteroid-producing neurons,
and that ODN stimulates steroid biosynthesis in hypothalamic neurons in a dose-dependent manner
through activation of CBR. Steroid-producing neurons are also innervated by vasotocin (VT)-containing
fibers, and they are gathered in hypothalamic regions which actively express the V1a receptor subtype
and mesotocin (MT) receptor (MTR). We have found that VT and MT, acting on V1a and MTR
respectively, are potent stimulators of neurosteroidogenesis. Finally, we have shown that steroidogenic
neurons are innervated by NPY and GnRH fibers, and that the nuclei where these neurons are located
are enriched with NPY Y1 and Y5 receptors, and GnRHR1/3 receptors. We have observed that NPY,
acting through Y1 receptors, inhibits neurosteroid biosynthesis, while GnRH stimulates the production
of neurosteroids probably via GnRHR1/3 receptors. Taken together, these data suggest that some of the
activities exerted by neurotransmitters and neuropeptides in the brain may be mediated via the
regulation of neurosteroid production.
Supported by INSERM (U413), the Regional Platform for Cell Imaging, a France-Québec exchange
program (INSERM-FRSQ), a France-Korean exchange program (STAR) and the Conseil Régional de
Endocrine Abstracts (2007) Vol 14
9th European Congress of Endocrinology, Budapest, Hungary, 2007
Endocrine Abstracts (2007) Vol 14
9th European Congress of Endocrinology, Budapest, Hungary, 2007
Traumatic brain injury-induced hypopituitarism: whom and when
to test
Chris Thompson
Beaumont Hospital/RCSI Medical School, Dublin, Ireland.
A large body of evidence has accumulated to indicate that between 20–30% of
survivors of acute traumatic brain injury (TBI) develop permanent pituitary
dysfunction. Growth hormone (GH) deficiency is the commonest abnormality
documented in most studies followed by ACTH and gonadotrophin deficiency
and hyperprolactinaemia, with TSH deficiency least common. In contrast to other
forms of pituitary disease, the classical hierarchy of pituitary hormone failure is
not always seen and there is a higher proportion of single hormone defects. Many
of the symptoms of chronic TBI are similar to those of untreated hypopituitarism,
which suggests that identification and appropriate treatment of hypopituitarism
offers a valuable service to survivors of TBI. Who should be tested? Most studies
have been confined to survivors of moderate to severe TBI and the rationale for
investigation is currently confined to this subgroup. There is little relationship
between severity of TBI, neuro-imaging studies or operative intervention and the
likelihood of hypopituitarism so until better guidance is available from
prospective studies, all survivors should be tested. The choice of dynamic stimuli
for ACTH and GH are centre-dependent. The timing of testing is important.
In the acute phase of TBI the key deficiency to identify is ACTH; patients who
develop hypotension, hypoglycaemia or hyponatraemia should be systematically
screened for ACTH deficiency. Studies of the natural history of pituitary
dysfunction after TBI suggest a dynamic process, with many acute abnormalities
recovering within 3–6 months of TBI, while new deficiencies may manifest in this
period. New deficiencies are rare after 6 months. Most authorities therefore
recommend formal dynamic testing at 3–6 months following TBI. Clinicians
should be aware of occasional late recovery of function. Prospective studies are
needed to better identify those at greatest risk of hypopituitarism, in order to
improve the logistics of post-TBI pituitary hormone assessment.
replacement is beneficial is still debated. Some studies showed positive effects on
the quality of life of 50 mg of DHEA but others fail to confirm this. A therapeutic
trial of 3–6 months in patients, particularly women, with relevant symptoms may
be justified.
Familial neurogenic diabetes insipidus
Soren Rittig
Skejby University Hospital, Aarhus, Denmark.
Although molecular research has contributed significantly to our knowledge of
familial neurohypophyseal diabetes insipidus (FNDI) for more than a decade, the
genetic background and the pathogenesis still is not understood fully. FNDI is, in
87 of 89 kindreds known, caused by mutations in the arginine vasopressin (AVP)
gene, the pattern of which seems to be largely revealed as only few novel
mutations have been identified in recent years. The mutation pattern, together
with evidence from clinical, cellular, and animal studies, points toward a
pathogenic cascade of events, initiated by protein misfolding, involving
intracellular protein accumulation, and ending with degeneration of the AVP
producing magnocellular neurons. Molecular research has also provided an
important tool in the occasionally difficult differential diagnosis of DI and the
opportunity to perform presymptomatic diagnosis. Although FNDI is treated
readily with exogenous administration of deamino-D-arginine vasopressin
(dDAVP), other treatment options such as gene therapy and enhancement of
the endoplasmic reticulum protein quality control could become future treatment
Hormones and the brain – S2
Morbidity and mortality
BA Bengtsson
Abstract unavailable
Stylianos Tsagarakis
Department of Endocrinology, Athens Polyclinic, Athens, Greece.
Hypocorticotropism refers to ACTH insufficiency, which may be partial or
complete, isolated or combined, genetic or acquired, pituitary or hypothalamic in
origin. As a result it leads to secondary adrenal failure. Adrenal secretion of
cortisol and of adrenal androgens is mainly affected; aldosterone secretion is
normal. Symptoms of hypocorticotropism include progressive malaise and weight
loss. Because aldosterone secretion is intact salt wasting, volume contraction and
hypokalemia are not present. Hypoglycemia due to defective neoglucogenesis
may occur and is particularly common in children. Symptoms may be more
dramatic in the case of abrupt onset. Laboratory assessment includes baseline
measurements of ACTH and cortisol and dynamic tests. A low morning value of
cortisol (i.e. !3 mg/dl) associated with a low ACTH is diagnostic of severe
hypococorticotropism. A value of 9am cortisol over 18 mg/dl excludes
hypococorticotropism. For all other values dynamic tests are required. The gold
standard test is the insulin stress test (IST). Alternative tests are the glucagon, the
metyrapone and the standard (SST) and low Synacthen (LST) tests. The
Synacthen tests because of their simplicity and safety have superseded the gold
standard IST. Although the LST was considered as a more sensitive test than the
SST recent data suggest that there is no difference. A cut-off of 18 mg/dl is
considered as a “pass” and is safe assuming that assessment is not close to recent
pituitary failure. Confirmation of hypocorticotropism requires replacement
therapy. Hydrocortisone is the preferred medication. It is better given in 3
divided doses to a total daily dose of 10–20 mg. Co-administration of GH may
increase the dose requirements of hydrocortisone. The dose should also be
increased during stress and surgery. The question of whether adrenal androgen
Endocrine Abstracts (2007) Vol 14
Thyroid hormone regulation of neural and oligodendrocyte precursors
in the mature brain: a possibility for remyelination and neuroprotection
Laura Calzà
University of Bologna, Ozzano Emilia, Bologna, Italy.
Re-myelination in the adult CNS has been demonstrated in different experimental
models of demyelinating diseases. However, there is no clear evidence that
re-myelination is effective in multiple sclerosis (MS), the most diffuse
demyelinating disease. Moreover, chronic disabilities in MS are believed to be
due to remyelination failure and consequent neuron damage and degeneration.
Due to the presence of numerous oligodendrocyte precursors inside demyelination plaques, reasons for remyelination failure are unknown. Data from
embryonic development and in vitro studies supports the primary role of thyroid
hormone in oligodendrocyte formation from neural precursors and maturation.
We have obtained positive results in promoting re-myelination and neuroprotection in chronic experimental allergic encephalomyelitis (EAE), a widely used
experimental model of MS, by recruiting progenitors and channelling them into
oligodendroglial lineage through administration of thyroid hormone. Experiments
performed in rats and confirmed in the primate Callithrix Jacchus have generated
a phase 2 clinical trial that is in progress. We have also explored the role of
thyroid hormone in regulating neural precursors cells in the subventricular zone of
mature brain by in vivo and in vitro experiments (neurosphere assay), with regard
to cell cycle and lineage regulation. Finally, we are exploring the possibility that
prenatal events disturbing thyroid function, like endocrine disruptors exposure
(dioxin family), might affect oligodendrocyte development and susceptibility to
demyelinating agents.
Neuroprotective actions of estrogens in the central nervous system
Luis Garcia-Segura & Iñigo Azcoitia
Instituto Cajal, CSIC, Madrid, Spain.
Sex hormones act both as endocrine signals as well as local paracrine or autocrine
factors in the nervous system. In addition to target to classical endocrine and
reproductive brain areas, sex hormones and its metabolites affect learning and
cognition and regulate the development and plasticity of brain regions that are not
directly related to reproduction. Estrogen and progesterone exert neuroprotective
9th European Congress of Endocrinology, Budapest, Hungary, 2007
effects in the central nervous system and may affect the onset and progression of
several neurodegenerative and affective disorders, as well as the recovery from
traumatic neurological injury. Recent studies have shown that the brain
up-regulates both estradiol synthesis and estrogen receptor expression in reactive
astroglia at sites of injury. Genetic or pharmacological inhibition of brain
aromatase, the enzyme involved in estradiol synthesis, results in marked neuronal
death after different forms of mild neurodegenerative stimuli that do not
compromise neuronal survival under control conditions. This finding strongly
suggest that local formation of estradiol in the CNS is neuroprotective and that the
induction of aromatase and the consecutive increase in the local production of
estradiol are part of the program triggered by the neural tissue to cope with
neurodegenerative insults. Proteins involved in the intra-mitochondrial trafficking
of cholesterol, the first step in steroidogenesis, such as the peripheral-type
benzodiazepine receptor (PBR) and the steroidogenic acute regulatory protein
(StAR), are also up-regulated in the brain after injury, together with the first
enzyme in the steroidogenic pathway (P450scc). This suggests that brain
steroidogenesis may be modified in adaptation to neurodegenerative conditions
and to the brain aging process. Recent studies have shown that Ro5-4864, a PBR
ligand that increases brain steroidogenesis is neuroprotective. Therefore, StAR,
PBR and aromatase are attractive pharmacological targets to promote
neuroprotection in the aged brain.
Supported by MEC, Spain (SAF 2005-00272) and the European Union (EWA
project: LSHM-CT-2005-518245).
Estrogen receptor signalling and cerebrovascular disease
Tommy Olsson, Magnus Strand & Ingegerd Söderström
Department of Medicine, Umeå University Hospital, Umeå, Sweden.
The transition to the postmenopausal stage is associated with an increased risk for
vascular diseases, including myocardial infarction and stroke. This has been
linked to a decrease in estrogen production. Estrogens mediate their effects on the
brain to a major extent through binding to nuclear receptors, estrogen receptor
alpha and beta. It is possible that positive and adverse effects of estrogens are
related to interactions between receptor genotypes and hormones. Notably, the
estrogen receptor alpha polymorphism c 454-397T/T is associated with increased
risk of hemorrhagic stroke, with a synergistic relationship between this genotype
and hypertension. In experimental stroke settings estrogens influence recovery of
cognitive functions, possibly via induction of neurotrophic factors and specific
transcription factors including NGFI-A. This may be related to increased
neuroplasticity in the hippocampal formation, a key area for memory processing.
Individualized treatment with estrogen receptor medulators may be beneficial for
individuals with an increased risk for stroke. Estrogens may also improve
recovery after stroke.
Immunesenescence and steroid hormones
Wiebke Arlt1 & Janet M Lord2
Division of Medical Sciences, University of Birmingham, Birmingham,
United Kingdom; 2MRC Centre for Immune Regulation, University of
Birmingham, Bimringham, United Kingdom.
Ageing is associated with a decline in immunity, also termed immunesenescence. This is paralleled by a decline in the production of several hormones as
typically illustrated by the menopausal loss of ovarian oestrogen production.
This lecture will give a brief overview of the physiology and pathophysiology of
steroid hormones that decline with ageing. Therein a specific focus will be laid
on the ageing-associated decline in adrenal dehydroepiandrosterone (DHEA)
production, an event commonly termed as “adrenopause”. However, this term is
rather imprecise as the other major outputs of adrenal corticosteroid production,
cortisol and aldosterone secretion, do not change with ageing. The regulatory
processes involved in the initiation and progression of “adrenopause” still
remain elusive. Current research efforts importantly aim at clarifying whether
“adrenopause” contributes to immunesenescence, also addressing the issue of an
altered glucocorticoid/DHEA balance that necessarily occurs if cortisol remains
unchanged while DHEA steadily declines. Previous research has shown that an
increased cortisol/DHEA ratio increases the likelihood of early postoperative
infections requiring hospitalisation in elderly patients with hip fracture and that
these changes are associated with an impairment of neutrophil function. The
lecture will summarise most recent results on differential effects of DHEA and
cortisol on components of the immune response, including neutrophil and
natural killer cell function, including first conclusive data on underlying
mechanisms. Further understanding of immune-endocrine links in the
pathophysiology of immunesenescence will hopefully help to develop clinical
tools for improving health in our rapidly ageing population.
Signaling and regulation of G-protein-coupled hormone
receptors – S3
Trafficking and signaling of angiotensin receptors
László Hunyady, Eszter Karip, Gábor Turu & László Szidonya
Department of Physiology, Semmelweis University, Budapest, Hungary.
The octapeptide hormone angiotensin II (Ang II) exerts its major biological
effects via angiotensin AT1 receptors (AT1Rs). Signaling of AT1Rs is regulated
by ß-arrestins, which bind to activated AT1Rs, uncouple them form G proteins,
and initiate their internalization via clathrin-coated pits and cause G protein
independent MAP kinase activation. It has been shown previously that AT1Rs
internalize via ß-arrestin-dependent and independent mechanisms, whereas
angiotensin AT2 receptors, which are unable to internalize, do not bind
ß-arrestins. To study the role of G protein independent MAP kinase activation
in cells, which endogenously express AT1Rs, a mutant receptor (S109Y) was
created, which is unable to bind candesartan. On the other hand, the Ang II
binding and Ang II-induced functional responses of the S109Y mutant receptor
are completely normal. This mutation was combined with a mutation
(DRY/AAY), which can bind to ß-arrestin2, but its G protein coupling is
completely impaired. The receptors were expressed in C9 cells, which express
endogenous AT1Rs. In the presence of candesartan the Ca2C signal and MAP
kinase activation of the endogenous AT1R was completely eliminated. However,
the Ca2C signal generation and MAP-kinase activation of the S109Y mutant
receptor was readily detectable. in the presence of candesartan, which inhibits the
endogenous AT1Rs, the combined S109Y and DRY/AAY mutant receptor was
unable to induce Ca2C signal generation, whereas it mediated Ang II-induced
MAP kinase activation with a slow kinetics. These data suggest that G protein
independent MAP kinase activation can occur in C9 cells.
This work was supported by OTKA T46445 and ETT 447/2006.
Pharmacological chaperones rescue the membrane expression and
function of a mutant of the vasopressin V1b/V3 receptor
Eric Clauser, Jessica Robert, Colette Auzan & Marie Ange Ventura
Institut Cochin, INSERM U567, Paris, France, CNRS UMR8104, Paris,
France; University Paris V, Paris, France.
The majority of loss-of function mutations of G protein coupled receptors, leading
to diseases, such as diabetes insipidus (V2 vasopressin receptor) or retinitis
pigmentosa (rhodopsin) are consecutive to retention of the receptor in the
endoplasmic reticulum (ER). Cell surface expression and biological function can
be restored by membrane-permeable ligands called pharmacological chaperones.
The V1b/V3R, one of the 3 subtypes of vasopressin receptors, is involved in the
regulation of the corticotroph axis during stress. Using an original assay for cell
surface expression of the receptor, we have demonstrated that a mutation of the
hydropobic 341FNX2LLX3L350 motif in the C-terminus of the human pituitary
V1b/V3R (MUT V3R) leads to its retention in the ER. The precise role of this
motif was further investigated using SSR149415, a nonpeptide V1b/V3R
The absence of the mutated receptor at the plasma membrane is linked to its
prolonged association with the molecular chaperone, calnexine, in the ER and
to its intensive degradation by the ubiquitin-proteasomal machinery. However,
this ER retention is not a consequence of a lack of oligomerization of the
mutant, which can be identified as dimers in the ER with BRET technique.
Treatment with SSR149415 restores expression of the mutated receptor at
the cell surface and its correct maturation, resulting into the functional
recovery of its signaling properties. SSR149415 acts by stabilizing the nativelike conformation of the V1b/V3R, reducing its association with calnexin and
favoring a secretory pathway rather than the proteasomal degradation
In conclusion, the 341FNX2LLX3L350 sequence is an important motif for
the V1b/V3R conformation and the misfolfding resulting from its mutation
alters the receptor export but can be reverted by SSR149415, which behaves
as a pharmacological chaperone.
Endocrine Abstracts (2007) Vol 14
9th European Congress of Endocrinology, Budapest, Hungary, 2007
Functional impact of GPCR heterodimerzation
Heike Biebermann
Institute of Experimental Pediatric Endocrinology, Charité Campus
Virchow, Universitätsmedizin Berlin, Berlin, Germany.
For over two decades the hypothesis of dimerization of G protein coupled
receptors (GPCR) exist. But only in 1999 it became clear by investigation of
GABA B receptors that dimerization is the prerequisite for function. Since then
our understanding of GPCR function is widened by the fact that nearly all
GPCRs form dimers or higher order oligomers. This formation of GPCR
homodimers or heterodimers influence the functional properties of a GPCR
from that we know of a monomer in its ability to traffic to the cell surface, to
bind one or even a variety of ligands, to initiate one or several signalling
pathways, to be internalized, or not, and at least to be a therapeutical target.
This receptor cross-talk seems to be crucial for fine-tuning of receptor function
in controlling physiological processes of a cell. A very large number of GPCRs
are known that form heterodimers/oligomers but the functional impact for a lot
of these dimers still remains unclear and functional consequences of GPCR
heterodimerization are nor predictable. For some GPCR dimers the functional
impact is solved, e.g. for GABA B1 and GABA B2 receptors it is known that
dimerization is necessary for cell surface expression and function; the taste
sensation of sweet or umami is dependent on the formation of taste receptor
T1R1, T1R2 and T1R3 complexes and the formation of dopamine 2
receptor/cannabinoid 1 receptor heterodimers result in activation of the Gs
instead of Gi when expressed alone.
What do these data contribute to our overall understanding of physiological
processes? As long as we have no other hints we have to accept that all possible
interactions of GPCRs that are expressed on a given cell type are possible and
therefore have to be investigated. to clarify their physiological significance.
Especially this counts for the estimation of drug pharmacology targeting a
Our group is interested in understanding the physiological processes of
hypothalamic weight regulation. Therefore we set out to investigate the
interaction of GPCR that are expressed on neurons of the nucleus arcuatus and
nucleus paraventricularis. For example we are able to show that the MC3R
forms dimers with the ghrelin receptor both are expressed on NPY/AGRP
neuron of the nucleus arcuatus. The functional consequences of these dimers
have to be investigated.
The determination of GPCR heterodimer function is a great challenge and
will provide explanation for so far not understood cellular processes.
Ago-allosteric effects of agonist drugs on 7TM receptors and their
endogenous hormones – example from the ghrelin receptor
Thue W. Schwartz
University of Copenhagen, Copenhagen, Denmark.
Conventionally, an allosteric modulator is neutral in respect of efficacy and binds
to a receptor site distant from the orthosteric site of the endogenous agonist.
However, recently compounds being ago-allosteric modulators have been
described i.e. compounds acting both as agonists on their own and as enhancers
for the endogenous agonists in both increasing agonist potency and often
providing additive efficacy - superagonism. The additive efficacy can also be
observed with agonists, which are neutral or even negative modulators of the
potency of the endogenous ligand. Based on the prevailing dimeric dogma for
7TM receptors, it is proposed that the ago-allosteric modulators often bind in the
orthosteric binding site, but – importantly – in the “other” or allosteric protomer
of the dimer. Hereby, they can act both as additive co-agonists, and through intermolecular cooperative effects between the protomers, they may influence the
potency of the endogenous agonist. It is of interest that at least some endogenous
agonists can only occupy one protomer of a dimeric 7TM receptor complex at a
time and thereby they leave the orthosteric binding site in the allosteric protomer
free, potentially for binding of exogenous, allosteric modulators. If the allosteric
modulator is an agonist, it is an ago-allosteric modulator; if it is neutral, it is a
classical enhancer. Molecular mapping in hetero-dimeric class-C receptors,
where the endogenous agonist clearly binds only in one protomer, supports the
notion that allosteric modulators can act through binding in the “other” protomer.
It is suggested that for the in vivo, clinical setting a positive ago-allosteric
modulator should be the preferred agonist drug.
T.W. Schwartz & B. Holst: Ago-allosteric modulation and other types of
allostery in 7TM dimeric receptors. J. Recept. Signal. Transduct. Res. (2006)
26: 107–128.
Endocrine Abstracts (2007) Vol 14
Gastroenteropancreatic endocrine tumors (GEP ET) – S4
Pathological classification of GEP neuroendocrine tumors
Mauro Papotti, Luisella Righi & Marco Volante
University of Turin, Torino, Italy.
In the gastroentero-pancreatic tract, a spectrum of neuroendocrine tumors (NET)
exists, including low grade tumors (carcinoid), intermediate grade malignant
carcinoid, and high grade poorly differentiated carcinomas of the small and large
cell types. In year 2000, the WHO presented a classification scheme for all NETs,
but mostly applied to gastroentero-pancreatic tumors. This term carcinoid was
replaced by (neuro)endocrine tumor, malignant carcinoid by well differentiated
(neuro)endocrine carcinoma, and the term “small cell carcinoma” was confirmed
for poorly differentiated NE neoplasms. The new terminology induced some
confusion in the routine application and interpretation of some NETs, especially
those of intermediate grade (which underwent major changes in the new
classification). New diagnostic criteria pose problems to the pathologist (e.g.
correct diagnosis on scarce biopsy or cytological material) and to the clinician
(choice of the appropriate therapy for single histological types). The
characterization of NETs includes the immunoprofiling of NE differentiation
markers and hormonal products, but also the analysis of prognostic (i.e. Ki67) and
therapeutic factors. The latter include somatostatin receptor expression profile
(possible in surgical, biopsy or cytology specimens by immunohistochemistry), to
identify possible targets of somatostatin analogs. Finally, apart from pure
endocrine tumors, NE differentiation occurs also in non-endocrine tumors (see
review in Volante M, Virchows Arch 449:499, 2006). “Mixed endocrine-exocrine
carcinomas”, as well as gastric, colorectal and pancreatic adenocarcinomas with
foci of NE differentiation have been described. These latter tumors can account for
up to 20% of cases, depending on the method used to assess the NE phenotype (eg
chromogranin A immunostaining), but to date they were not found to bear any
prognostic significance (as opposed to the well established prognostic role of NE
differentiated prostate cancer), with the possible exception of gastric cancer,
according to a recent study by Japanese authors (Jiang SX, Am J Surg Pathol
30:945, 2006).
Biological, morphological work-up and screening for inherited disease
Britt Skogseid
Uppsala University, Uppsala, Sweden.
Pancreatic endocrine tumors (EPT) may occur sporadically or in association with the
rare autosomal dominantly inherited tumor syndromes; multiple endocrine neoplasia
type 1 (MEN1) and von Hipple Lindau (VHL). The genes causing these syndromes
have been identified, and genotyping is possible which enables the laborious clinical
investigations for diagnosis of lesions to be restricted to 50% of family members. For
MEN1, no clinically useful genotype-phenotype correlation as been discovered and
in a majority of patients the EPT will undergo malignant transformation. Timely
identification and intervention by surgery before development of metastases
currently represents the only cure of the disease. Thus, repeated extensive
biochemical and radiological investigations for early recognition of small EPT
in situ should be considered in asymptomatic gene carriers. Efficacies of genetic and
hormonal screening programs as well as imaging will be discussed.
Prognosis of GEP ET
E. Baudin
Abstract unavailable
Therapeutic management of GEP ET
P. Ruszniewski
Abstract unavailable
9th European Congress of Endocrinology, Budapest, Hungary, 2007
Novel bioactive peptides – lessons from animals – S5
Discovery of novel bioactive peptides: the uniquely important
contribution of amphibians to mammalian neuropeptidology
Hubert Vaudry1, Hervé Tostivint1, Isabelle Lihrmann1, Nicolas Chartrel1,
Alain Fournier2, Jérôme Leprince1, Marie-Christine Tonon1 &
J. Michael Conlon3
INSERM U413, Laboratory of Cellular and Molecular Neuroendocrinology, IFRMP23, University of Rouen, Mont-Saint-Aignan, France;
INRS – Institut Armand-Frappier, Univeristy of Québec, Montreal,
Canada; 3Department Biochemistry, Faculty Medicine and Health Sciences,
UAE University, Al Ain, United Arab Emirates.
The concentration of many neuropeptides in the brains of ectothermic
vertebrates is several orders of magnitude higher than in the brains of
mammals. We have taken advantage of this singular situation to isolate from
the brain of the European green frog, Rana esculenta, a number of regulatory
peptides that are orthologous to mammalian neuroendocrine peptides. These
include a-MSH, g-MSH, two tachykinins, two GnRH variants, CRH,
PACAP, NPY, CGRP, CNP, GRP, and ODN. This peptidomics project has
also led to the discovery of several novel neuroendocrine peptides that were
first isolated from frog brain tissue but have subsequently been identified in
mammals. In particular, we have characterized (1) the somatostatin-14 (S-14)
isoform [Pro2, Met13]S-14 as well as authentic S-14, thereby providing the
first evidence for the occurrence of two somatostatin variants in the brain of
a single species, (2) the first tetrapod urotensin II, a peptide that had long
been thought to be produced only in the caudal neurosecretory system of
fish, (3) secretoneurin, a peptide derived from the post-translational
processing of secretogranin II, and (4) 26RFa, a novel member of the
Arg-Phe-NH2 family of biologically active peptides. Orthologs of all these
frog neuropeptides have now been identified in man and have been shown to
exert important regulatory effects in mammals.
Supported by grants from INSERM (U413), the European Institute for
Peptide Research (IFRMP23), the Platform for Cell Imaging of HauteNormandie (PFRRICHN), the Conseil Régional de Haute-Normandie and the
Laboratoire International Associé Samuel de Champlain.
Bioactive peptides in invertebrate model organisms
Liliane Schoofs, Inge Mertens, Geert Baggerman, Peter Verleyen &
Elke Clynen
K.U.Leuven, Leuven, Belgium.
Genome sequence projects in combination with advances in mass
spectrometry and bioinformatics have created several new possibilities for
comparative endocrinology. In 2001 we introduced the peptidomics
technology that allows the identification of the complement of native
(neuro)peptides in cells, tissues, organs and organisms. Especially when
genome sequence information is available (D. melanogaster, A. mellifera, C.
elegans.), neuropeptidomes were successfully identified and compared in
different physiological conditions.
Synthetic libraries of newly sequenced peptides can be used to screen
orphan neuropeptide G-protein coupled receptors in cell-based assays that
express the receptor. This has boosted receptor identification in insects and
other invertebrates. One of the advantages of model organisms, such as C.
elegans and Drosophila is their amenability for genetic manipulations and
the availability of knockouts as a result of (ongoing) gene disruption
In this presentation, we show how all these technological developments
contributed to the discovery of novel neuropeptide signalling systems in
Drosophila and in C. elegans. In the nematode worm, we will focus on the
functional characterisation of neuropeptide processing enzymes and two
neuropeptide GPCR signalling systems, respectively related to the mammalian GnRH receptor and the VPAC receptor in vertebrates. We will discus
the implications of these findings with respect to the evolutionary
conservation of these signalling systems.
Comparative approaches to resolve the complexities of human appetite
Dan Larhammar
Uppsala University, Uppsala, Sweden.
The regulatory processes of appetite and metabolism have turned out to be
exceedingly complex and involve numerous hormones and neurotransmitters,
particularly peptides. Evolutionary studies in our laboratory have shown that
many genes encoding peptides and receptors were duplicated in the early stages of
vertebrate evolution through chromosome duplications. Thus, many of the
components have existed for 400–500 million years, for instance the various
members of the families of NPY-like peptides, opioid peptides, tachykinins,
glycoprotein hormone beta subunits (FSH, LH and TSH) and others. The
chromosome duplications also explain the origin of many peptide receptors, for
instance the NPY-family receptors, opioid receptors, oxytocin-vasopressin
receptors, tachykinin receptors and CRF receptors. Also the glucocorticoidmineralcorticoid receptors arose through a chromosome duplication. These
observations of ancient chromosome duplications explain a great deal of the
complexity of the vertebrate endocrine and neuronal networks. Duplication of
complete genes in this manner means that the duplicates initially had identical
gene regulation. This makes it particularly intriguing that some duplicates now
have opposing functional roles. One striking example is the peptide hormone
PYY, released from gut endocrine cells after meals, which acts as an appetite
inhibitor on the Y2 receptor in the hypothalamus. In contrast, the related peptide
NPY is the body’s most potent stimulator of appetite, acting on receptor subtypes
Y1 and Y5. Probably the switch in function occurred when the duplicated genes
became expressed in different cell types. We have functionally studied the roles of
the NPY-family peptides in a herbivorous species with frequent meals, the
guinea-pig, and a carnivore with rare meals, the dog. The role of NPY appears to
be the same in the guinea pig as in intermittent feeders like rats. We are presently
evaluating the role of PYY as an appetite inhibitor in dogs. Functional studies in
different species will provide a firmer basis for predicting and testing the
functions of these peptides in humans as well as their possible roles in states of
obesity and anorexia.
Somatostatin, cortistatin and their new and old receptors: from
comparative to translational endocrinology
Justo P. Castaño, Mario Durán-Prado, Rafael Vázquez-Martı́nez, Antonio
J. Martı́nez-Fuentes, Manuel D. Gahete, Raul M. Luque & Maria
M. Malagón
Department Cell Biology, Physiology and Immunology. Univ. Córdoba,
Cordoba, Spain.
omatostatin, originally isolated from ovine hypothalami in 1973, and
cortistatin, identified a decade ago in amphibians and then in human and
rodents, are two highly related peptides thought to derive from a common
ancestor gene. Owing to their high structural homology, both peptides bind
with similar affinity to the five so-called somatostatin receptors (sst1-sst5),
and exert virtually undistinguishable effects on several physiological targets,
including inhibition of endocrine secretions. Yet, each peptide also shows
distinctive, specific functions, which should involve different receptors and/or
signalling mechanisms still to be defined, and also display divergent patterns
of expression in normal and tumoral tissues. In particular, cortistatin
selectively regulates locomotion- and sleep-related processes and exerts
potent antiinflammatory effects with a promising therapeutic potential. In this
context, recent work from our group has aimed at characterizing the response
of pituitary somatotrope cells to cortistatin and somatostatin, and to isolate
sst receptors in a domestic species, the pig. This led to us to demonstrate
that both peptides similarly exert a dual, inhibitory and stimulatory effect on
GH release in vitro, which likely involve sst1/sst2 and sst5, respectively.
Furthermore, while cloning porcine sst5, we discovered two new truncated
isoforms of this receptor, termed psst5B and psst5C, which display distinct
tissue distribution and, when expressed in clonal cell lines, show selective
functional responses to somatostatin (psst5B) and cortistatin (psst5C).
Interestingly, FRET studies revealed that these novel receptors functionally
interact with their full-length counterpart psst5A, as well as with the rest of
pig sst. Moreover, we recently cloned two similar human sst5 truncated
isoforms (hsst5B and hsst5C) that also show selective functional response to
somatostatin and cortistatin, functionally interact with and modulate hsst5A
and hsst2, and are differentially distributed in normal and tumoral human
tissues, suggesting a possible pathophysiological role for these novel
Endocrine Abstracts (2007) Vol 14
9th European Congress of Endocrinology, Budapest, Hungary, 2007
Diabetes and insulin – S6
Perspectives of islet cell transplantations
B Keymeulen
Abstract unavailable
Cytokines as pathogenetic effectors in type 1 and type 2 diabetes
Thomas Mandrup-Poulsen
Steno Diabetes Center, Gentofte, Denmark; Karolinska Institute, Stockholm, Sweden.
The pro-inflammatory cytokine interleukin-1 is selectively cytotoxic to rodent
and human beta-cells in vitro, and anti-IL-1 therapies reduce diabetes incidence in
animal prevention models: (1) IL-1 alone or in combination with other
inflammatory cytokines causes beta-cell destruction in rodent and human islets
and in perfused pancreas via MAPK and NFkB signaling, (2) IL-1 given i.p. to
non-diabetes prone animals causes transient insulinopenic diabetes (3) IL-1 is
expressed early in islets of the non-obese diabetic (NOD) mouse, a model of
spontaneous autoimmune diabetes (4) anti-IL-1 intervention prevents diabetes
development in animal models of Type 1 diabetes and islet graft destruction and
(5) transgenic mice with knock-out of the IL-1 receptor reduces diabetes
We recently completed a 13-week clinical study of IL-1 Receptor Antagonist
(IL-1Ra, anakinra, KineretR, Amgen) therapy in Type 2 diabetics based on the
rationale that in vitro glucotoxicity to human beta-cells can be prevented with IL1Ra, and that glucose induces islet IL-1 production, which causes beta-cell
apoptosis by pathways similar to those believed to operate in Type 1 diabetes.
This study provided proof-of-principle that inhibition of IL-1 signalling can
improve glycemia and beta-cell function in humans. Interestingly, maximal effect
on glycosylated hemoglobin with anakinra was seen after 4 weeks, and fasting
blood glucose was significantly reduced already after 1 week, suggesting rapid
effects on beta-cell secretory capacity. These preclinical and clinical studies
warrant studies to investigate the effect of IL-1 blockade in patients with recentonset Type 1 diabetes mellitus.
GLP-1 as a drug target
JJ Holst
Transplanted animals correct hyperglycaemia within 1 week and restore body
weight in four weeks. Graft removal rescued the diabetic condition. Glucose
tolerance test (IPGTT) and blood glucose normalization after a challenge meal
was similar in control and in transplanted mice. More recently, progenitors from
peripheral human blood cells (PCMO) have been convinced to acquire an insulinproducing phenotype which normalize blood glucose of immunocompromised
(SCID) diabetic mice, an option with tentative applications in regenerative
medicine. This approach opens new possibilities for tissue transplantation in the
treatment diabetes mellitus.
1. Soria B et al. (2000) Diabetes 49: 157–162.
2. Soria B et al. (2001) Diabetologia 44: 407–415.
3. León-Quinto T et al. (2004) Diabetologia 47(8): 1442–1451.
4. Runhke M et al. (2005) Gastroenterology 128(7): 1774–1786.
5. Vaca P et al. (2006) Stem Cells 24(2): 258–265.
Thyroid cell biology – S7
New insights from zebrafish: the molecular and cellular base of thyroid
Burkhard Alt, Dejan Adzic, Osama Elsalini & Klaus Rohr
University of Köln, Institute for Developmental Biology, Köln, Germany.
Due to experimental advantages such as its rapid development, transparent
embryos, and accessibility for genetic analysis as well as embryonic
manipulation, the zebrafish is a useful model organism for research on
organogenesis. My lab has established that the basic mechanisms of thyroid
development are essentially conserved on the morphological as well as on the
molecular level between fish and mammals. We use zebrafish to identify as yet
unknown factors involved in thyroid development. In this talk, I will give an
overview about new, unique approaches to understand thyroid development in
zebrafish. I will touch different aspects such as genetics of early induction, the
molecular base of cellular behaviour in primordial relocalisation, and
morphogenesis of the gland. Concentrating on selected molecules, I will
exemplify how research on zebrafish contributes to a general understanding of
thyroid development that sheds new light on the causes of congenital
Involvement of cardiovascular development and non-cell autonomous
signaling in mouse thyroid organogenesis
Henrik Fagman
Institute of Biomedicine, The Sahlgrenska Academy at Göteborg
University, Göteborg, Sweden.
Abstract unavailable
Engineering beta cells to recover insulin function
Bernat Soria, A Hmadcha, JR Tejedo, FJ Bedoya & F Martin
Andalusian Center for Molecular Biology and Regenerative Medicine,
Seville, Spain.
Stem cells are clonogenic cells capable of both self-renewal and multilineage
differentiation. Therefore, these cells have the potential to proliferate and
differentiate into any type of cell and to be genetically modified ‘in vitro’, thus
providing cells which can be isolated and used for transplantation. Moreover,
these derived cells have proven to be useful in different animal models. Using a
combination of several directed differentiation methods (nicotinamide, sonic
hedgehog signalling inhibition, soluble factors from pancreatic buds] and a ‘cell
trapping’ system, we have obtained insulin-secreting cells from undifferentiated
embryonic stem cells. Lineage-trapping constructs used allows the expression of a
neomycin selection system under the control of the regulatory regions of insulin
gene and other B-cell genes, such as Nkx6.1. Selection of differentiated cells
exclude non-differentiated cells which use to be present and are teratogenic.
Endocrine Abstracts (2007) Vol 14
Thyroid dysgenesis (comprising agenesis, hemiagenesis or ectopic localization)
is the major cause of congenital hypothyroidism in humans. Recent
experimental observations indicate that thyroid dysgenesis may be a polygenic
disease with variable penetrance depending on genetic background. Also,
thyroid dysgenesis might be one manifestation of syndromic malformations.
The molecular mechanisms of thyroid dysgenesis in humans are largely
unknown; so far genes encoding thyroid transcription factors that are required
for normal thyroid development in mouse, i.e. Titf1/Nkx2.1 (also known as
TTF-1), Foxe1 (also known as TTF-2) and Pax8, have been found to be
mutated only in a minority of patients. The underlying molecular mechanism is
in most cases unknown, but the frequent co-incidence of cardiac anomalies
(3–12%) suggests that the thyroid morphogenetic process may be linked to
cardiovascular development.
I will give an overview about critical steps in murine thyroid
morphogenesis. Emphasis will be put on proliferative patterns and the
possible relationship between shaping of the thyroid and development of the
of pharyngeal arch artery system. In this context, recent results from our
laboratory providing a mechanistic explanation to thyroid dysgenesis
incidentally reported to occur in children with the DiGeorge syndrome will
be discussed. The role of non-cell-autonomous factors (Shh, Tbx1) in thyroid
development will be put in relation to other transgenic models where thyroid
dysgenesis has been described. Finally, possible clinical implications of the
findings will be discussed.
9th European Congress of Endocrinology, Budapest, Hungary, 2007
Thyroglobulin deposition and cathepsin-dependent Tg mobilization
Klaudia Brix1, Sasa Jenko-Kokalj2, Dusan Turk2, Dieter Brömme3,
Nicole Kühl1 & Silvia Jordans1
Jacobs University Bremen, School of Engineering and Science, Bremen,
Germany; 2Jozef-Stefan Institute, Ljubljana, Slovenia; 3University of
British Columbia, Vancouver, BC, Canada.
Thyroid hormones thyroxine and triiodothyronine are essential for development,
growth and metabolism. The prohormone thyroglobulin (Tg) is stored in high
concentrations and in covalently cross-linked form within the lumen of thyroid
follicles. Thyroid hormones are liberated from Tg in a regulated manner in that
TSH triggers the secretion of lysosomal enzymes into the extracellular follicle
lumen where they solubilize covalently cross-linked Tg and liberate thyroxine
by partial Tg degradation. Using mice deficient in cysteine cathepsins B, K,
and/or L, we showed that liberation of thyroid hormones from within Tg is based
on the concerted action of a protease network. Cathepsins B and L are key
players in conversion of cross-linked Tg-globules to soluble Tg. Moreover,
assessment of thyroid morphology and serum thyroxine levels of cathepsin Kand L-deficient mice revealed impaired mobilization of Tg. The respective mice
exhibited a phenotype reminiscent of hypothyroidism, proving the importance of
cathepsins K and L for the liberation of thyroid hormones. Tg storage and Tg
mobilization both occur extracellularly. Hence, the conditions for Tg processing
are non-favorable for the proteolytic activity of lysosomal cysteine cathepsins.
Therefore, we set-up an in vitro degradation assay that simulates the in vivo
situation. Indeed, in such assays the cysteine cathepsins B, K, L and S were able
to partially degrade their natural substrate Tg even at neutral pH and oxidizing
conditions. Analysis of the cleavage sites of cysteine cathepsins under
extracellular conditions revealed that sub-cellular and sub-follicular localization
of the proteases as well as the timing of proteolysis are crucial steps in the
regulation of thyroid hormone liberation from Tg. Any interference with the
delicate protease network in the thyroid may result in impaired function.
Role of the complex Megalin-RAP in thyroglobulin trafficking
M Marino
Abstract unavailable
Advances in adrenal hypersecretory disorders – S8
Autocrine-paracrine pathways in primary adrenal disorders
Hervé Lefebvre1, Vincent Contesse1, Dorthe Cartier1,
Véronique Perraudin1, Catherine Delarue1, Hubert Vaudry1,
Jérôme Bertherat2, Pierre-François Plouin3, Jean-Marc Kuhn4 &
Estelle Louiset1
INSERM U413, IFRMP23, Laboratory of Cellular and Molecular
Neuroendocrinology, University of Rouen, Mont Saint Aignan, France;
Department of Endocrinology, CHU Cochin & Institut Cochin, INSERM
U567, CNRS UMR8104, IFR 116, University of Paris V-René Descartes,
Paris, France; 3Hypertension Unit, European Hospital Georges Pompidou,
University of Paris V-René Descartes, Paris, France; 4Department of
Endocrinology, University Hospital of Rouen, Rouen, France.
It is now well demonstrated that, in the human adrenal gland, aldosterone and
cortisol productions are stimulated by autocrine/paracrine factors, like serotonin
(5-HT) and arginine vasopressin (AVP). Several data indicate that these signals
may also be involved in the regulation of corticosteroidogenesis in adrenocortical
hyperplasias and tumors. 5-HT is detected in clusters of steroidogenic cells in
aldosterone-producing adrenocortical adenomas (APAs), and in both ACTHindependent macronodular adrenal hyperplasias (AIMAHs) and adenomas
responsible for Cushing’s syndrome. In these lesions, 5-HT stimulates
steroidogenesis through activation of overexpressed eutopic 5-HT4 and/or ectopic
5-HT7 receptors. Immunohistochemical studies have shown the occurrence of
AVP in a subpopulation of steroidogenic cells in APAs and AIMAHs. In APAs,
AVP activates aldosterone production through the eutopic V1a receptor whereas
its stimulatory effect on cortisol secretion from AIMAH tissues is mediated by
both overexpressed V1a and/or ectopic V1b and V2 receptors. Interestingly,
administration of V1a antagonists to patients with APA induces an aldosterone
response to the upright stimulation test, indicating that, in these tumors, inhibition
of the vasopressinergic tone sensitizes the tissues to the action of postureresponsive hormones. Finally, the presence of ACTH has been observed in
AIMAH tissues and the ACTH receptor antagonist corticostatin inhibits basal
cortisol secretion from AIMAH explants, demonstrating that glucocorticoid
production is dependent on the paracrine action of intraadrenal ACTH in some
primary adrenal disorders causing Cushing’s syndrome. In conclusion,
autocrine/paracrine regulatory factors are produced within adrenocortical
hyperplasias and tumors in which they play an important role in the control of
steroidogenesis. These local factors may therefore represent promising targets
for the treatment of primary adrenal disorders. This work was supported
by INSERM, the University Hospital of Rouen, the Conseil Régional de
Haute-Normandie and the COMETE network (PHRC AOM 02068).
Carney complex and primary pigmented nodular adrenocortical
Jérôme Bertherat
Institut Cochin, INSERM U567, Paris, France.
The Carney complex (CNC) is a dominantly inherited syndrome characterized by
spotty skin pigmentation, endocrine overactivity and myxomas. The most
common endocrine gland manifestations are acromegaly, thyroid tumors,
testicular tumors, and ACTH-independent Cushing’s syndrome due to primary
pigmented nodular adrenocortical disease (PPNAD). PPNAD, a rare cause of
Cushing’s syndrome, is due to primary bilateral adrenal defect that can be also
observed in some patients without other CNC manifestations nor familial history
of the disease. Myxomas can be observed in the heart, skin and breast. Cardiac
myxomas can develop in any cardiac chamber and may be multiple. One of the
putative CNC genes located on 17q22-24, (PRKAR1A), has been identified to
encode the regulatory subunit (R1A) of protein kinase A. Heterozygous
inactivating mutations of PRKAR1A were reported initially in 45 to 65% of
CNC index cases, and may be present in about 80% of the CNC families
presenting mainly with Cushing’s syndrome. PRKAR1A is a key component of
the cAMP signaling pathway that has been implicated in endocrine tumorigenesis
and could, at least partly, function as a tumor suppressor gene. More recently,
germline inactivating mutations of PDE11A4 have been identified in patients with
isolated primary nodular adrenocortrical disease. This underlines the importance
of the cAMP signalling pathway in the pathophysiology of secreting endocrine
tumors. Somatic PRKAR1A mutations have been observed in adrenal adenomas
responsible for Cushing syndrome. In vitro and transgenic models have been
developped to study the consequences of PRKAR1A inactivation. In these models
dysregulation of the cAMP pathway, but also others signalling pathways, have
been observed. The new insights coming from the genetics of CNC and these
experimental models in the pathophysiology of endocrine tumorigenesis will be
Diagnosis of primary aldosteronism
GP Rossi
Abstract unavailable
Adrenocortical carcinoma: current and future therapeutic options
Martin Fassnacht1, Stefanie Hahner1, Sarah Johanssen1,
Ann-Cathrin Koschker1, Marcus Quinkler2 & Bruno Allolio1
Dept. of Medicine, University Hospital Wuerzburg, Wuerzburg, Germany;
Dept. of Medicine, Charite University, Berlin, Germany.
Adrenocortical carcinoma (ACC) is a rare and heterogeneous malignancy with
incompletely understood pathogenesis and poor prognosis. Recent data from
the German ACC Registry (nZ377) demonstrate an overall 5-year survival of
46%. Survival is clearly stage-dependent (P!0.01) with a 5-year survival of
Endocrine Abstracts (2007) Vol 14
9th European Congress of Endocrinology, Budapest, Hungary, 2007
85% in stage 1, 56% in stage 2, 42% in stage 3, and 16% in stage 4,
In stages I –III open surgery by an expert surgeon aiming at a R0 resection
is the treatment of choice. However even after R0 resection, only 37% of the
patients are disease-free after 5 years. Therefore, adjuvant treatment options are
urgently needed. In a recent series including 177 patients from Italy and
Germany, adjuvant mitotane prolonged significantly disease-free survival
compared to observational follow-up. In addition, adjuvant radiotherapy of
the tumor bed is a promising option to prevent local recurrence.
In tumor recurrence and metastatic disease, surgery should be considered if
complete resection is feasible. In patients not amenable to surgery, mitotane
(alone or in combination with cytotoxic drugs) remains the treatment of choice.
Monitoring of drug levels (therapeutic range 14–20 mg/l) is mandatory for
optimum results. In advanced disease, the most promising therapeutic options
(etoposide, doxorubicin, cisplatin plus mitotane and streptozotocin plus
mitotane) are currently compared in an international phase III trial (www.
firm-act.org). In 2006, we have administered EGFR inhibitors and VEGF
antibody as salvage therapy in a small series of patients – so far without
significant success. However, in 2007 the Collaborative group for Adrenocortical Carcinoma Therapy (CO-ACT) will initiate three new trials for salvage
therapies investigating two multi-targeted tyrosine kinase inhibitors and an
IGF-1 receptor antibody, respectively, leading hopefully to improved clinical
outcome. Future advances in the management of ACC will depend on a better
understanding of the molecular pathogenesis of ACC facilitating the use of
new targeted therapies.
techniques that allow to visualize the skeleton at different scales: from the
organ level to tissue, cellular, and subcellular levels, depicting morphology and
function. Progress in the field of imaging technologies resulted in methods
suited for clinical investigation of patients in vivo, non-invasive methods for
preclinical animal studies and sophisticated functional and molecular imaging
methods for both in vivo and ex vivo characterization of bone status have been
At the macroscopic scale the mechanical function of individual bones can
now be assessed by 3-D volumetric spiral CT approaches. The image-data
collected can be analyzed using Finite Element Models to calculate breaking
strength under simulated impacting forces. This allows more accurate
identification of subjects at risk for fracture and the monitoring of progress
in fracture healing.
At the microscopic scale micro-CT has seen impressive advances with ever
increasing image resolution – some devices are now suited for nano-CT
imaging. This technology allows studies on the effects of bone turnover in
normal and diseased tissue, including metabolic bone disorders such as
osteoporosis but also of arthritis and skeletal tumours and metastases.
Examinations of living animals enable the non-invasive longitudinal monitoring
of skeletal effects of therapeutic interventions.
Finally, molecular imaging, i.e. the visualization of molecular, biochemical
or cellular processes with radiological methods: to date this method is mostly
restricted to animal studies. However, the achievements seen here are
impressive: localized visualization of molecular and physiological information,
e.g. imaging of labelled osteoblasts and their precursors, monitoring of the
effects of hormones or gene therapy, or an earlier identification of skeletal
metastases. Substantial research is still required to bring these advances to the
clinic but the prospects for better individualized patient care based on combined
molecular imaging and therapy are most exciting.
Imaging in endocrinology – S9
PET in diagnostics of metabolic alterations and endocrinological
Pirjo Nuutila
University of Turku, Turku, Finland.
Positron emission tomography (PET) is an imaging technique that enables direct
observation of tissue radioactivity concentration over time in vivo. Unlimited
number of natural substrates (e.g. glucose, fatty acid), substrate analogs can be
labelled for use with PET. PET combined with tracer kinetic models measures
blood flow, membrane transport, metabolism, ligand receptor interactions and
recently also gene expression noninvasively and quantitatively.
An abnormal action of insulin and handling glucose and fatty acids in
muscle, heart, liver, brain and visceral and subcutaneous adipose tissue have
been studied in vivo in humans. This tissue specific assessment has increased
the understanding of the pathophysiology of metabolic syndrome, obesity and
diabetes and the differences in tissue specific action in vivo. The effects of
insulin, free fatty acids, exercise and diet have been evaluated. PET is powerful
tool for the assessment of tissue specific action of drugs targeted to metabolic
disorders. The hybrid PET/CT scanners enable correlation of anatomic and
functional information.
The clinical use of PET is rapidly expanding. In addition to (18)F-labelled
deoxyglucose (FDG) which is routine used in oncology for diagnosis of
cancer, many more specific tracers have been shown to improve diagnostics
of neuroendocrinological tumours (NETs). The most promising of those is
(18)F-fluorodihydroxyphenylalanine (FDOPA). It appears to be more useful
in carcinoid tumours than scintigraphic imaging and might replace it. It is
more sensitive than CT or MRI in detection of insulinomas and has quickly
replaced other methods in the assessment of focal form of congenital
hyperinsulinism of infancy (CHI). FDOPA-PET improves diagnostics and
prediction of prognosis, and be used to assess patients’ response to treatment
for NETs.
Macro-, micro-, and molecular imaging of bone
Claus-C. Glüer
Medizinische Physik, Klinik f. Diagnostische Radiologie, Universitätsklinikum Schleswig-Holstein, Campus Kiel, Germany.
The clinical diagnostic examination of patients and the research-oriented
investigation of the pathophysiology of skeletal disorders require imaging
Endocrine Abstracts (2007) Vol 14
New tracers for neuroendocrine tumors
Marcel Stokkel
LUMC, Leiden, Netherlands.
Neuroendocrine tumors (NET) comprise a wide variety of neoplasms that have
certain characteristics in common. However, they are defined not by site but
by molecular characteristics. The most common forms arise in the
gastrointestinal tract, but there are NET which are not directly related to
this site, such as medullary cell carcinoma or small-cell lung cancer. Different
secretory syndromes have also resulted in certain subtypes receiving names as
carcinoid if they produce serotonin or insulinoma if they produce insulin, etc.
It has to be realized however, that 50% are described as non-secretors. With
respect to nuclear medicine techniques available, many reports have focussed
on the use of meta-Iodobenzylguanidine (MIBG) and radiolabelled somatostatin analogs, such as Indium-111-octreotide. Especially In-111-octreotide has
a reported sensitivity ranging from 65% for medullary thyroid cancer to
almost 100% in small-cell lung cancers and pancreatic neuroendocriene
tumors. Many other potential receptors other than the somatostatin receptors,
such as GRP-R, CCK2, GLP-1-R, NK1 and VPAC1, have been developed and
studied over the past years. It has been suggested that the simultaneous
expression of multiple of these peptide receptors in NET provide the
molecular basis for in vivo multireceptor targeting, thus improving the efficacy
of radiolabelled peptides for diagnosing, staging and treating NET. Most of
the peptides under study directed against the previously mentioned receptors
were labelled with Indium-111 or Technetium-99m, both easily applicable in
clinical practice. Despite optimal results of positron emission tomography
(PET) using F18-deoxyglucose in many malignant tumors, its role in NET is
still limited. In contrast, PET using F18-DOPA and Ga-68-DOTA octreotate
has shown promise. C11-5-hyroxytryptophan (C11-5-HTP) has demonstrated
specific and irreversibly entrapment by serotonin-producing tumors, but it has
been shown that non-functioning or poorly differentiated tumors or necrotic
ones cannot be detected accurately. Highly important improvements have been
made by the introduction of hybrid cameras such as SPECT/CT or PET/CT.
The combination of both techniques allows whole body imaging quickly
providing functional and anatomic information. A close clinical relation
between imaging and treatment with radiolabelled peptides has been
established over the past decades. Many studies have reported good and/or
promising results with respect to Lutetium-177 (Lu-177) and Yttrium-90
(Y-90) labelled peptides, such as Y-90 DOTATOC or Lu-177-lanreotide.
In current presentation, an overview is given on the nuclear medicine
diagnostic and therapeutic options and developments in neuroendocrine
9th European Congress of Endocrinology, Budapest, Hungary, 2007
Echoendoscopy for the diagnosis of pancreatic endocrine tumors
Claudio De Angelis
Gastrohepatology Department, San Giovanni Battista Hospital, University
of Turin, Turin, Italy.
GH receptor signalling
Gunnar Norstedt, Petra Tollet Egnell & Amilcar Flores Morales
Karolinska Institutet, Stockholm, Sweden.
Pancreatic neuroendocrine tumors (NET) have always represented a complex
dilemma for diagnostic imaging. This is mainly due to their small size and
brought during the years to a complex range of diagnostic proposals. A correct
preoperative detection and staging are mandatory in order to choose
management options and to optimize surgical treatment. Endoscopic Ultrasound
(EUS) has been claimed to be the best technique for imaging the pancreas, it
High resolution images of the main pancreatic duct and surrounding
parenchyma. One of the more relevant advantages of EUS compared with
US, CT and MRI was indeed the superior parenchymal resolution, that gives
reason for the results of several studies that established the superior
sensitivity of EUS (98%) for the diagnosis of pancreatic tumors in
comparison to all the other imaging modalities. The results of EUS were
even better in small tumors, less than 3 or 2 cm, where sensitivity of US and
CT decreased to only 29%. However the introduction of multidetector helical
CT has today revolutionized the field of pancreatic imaging. More recent
data on pancreatic NETs confirmed that the distance between helical-CT and
EUS has nearly been annulled. EUS remains the best method for the
detection of small pancreatic insulinomas and gastrinomas, but the first
imaging modality to be used today in the suspicion of a pancreatic NET
must be a multislice CT. EUS is needed as a second step in the diagnostic
algorithm when CT shows negative or doubtful results. So the most effective
method for revealing pancreatic NET is a combined imaging protocol that
consists of both CT and EUS. The endosonographic pattern of these tumors
is mainly represented by small focal hypoechoic, omogeneous, round lesions,
with sharp margins, often hypervascular. Several studies have shown the high
sensitivity and specificity of EUS in localizing endocrine tumors of the
duodeno-pancreatic area. We demonstrated a correct localisation of
pancreatic tumors in 86.7% of 23 cases surgically confirmed. In conclusion
EUS is highly accurate in the detection of pancreatic neuroendocrine tumors
and is cost effective when used early in the preoperative localization
strategy. EUS decreased the need for additional invasive tests and avoided
unnecessary morbidity and resource consumption.
EUS should play a primary role in preoperative localization and staging of
these tumors.
GH and prolactin at their targets – S10
Cellular control mechanisms for GH sensitivity
Ger Strous, Peter van Kerkhof, Monique van den Eijnden & Joyce Putters
University Medical Center, Utrecht, Netherlands.
The growth hormone (GH) receptor is a key regulator of cellular metabolism.
Using model cell systems we have investigated how GH-induced signaling is
regulated, both in paracrine and autocrine conditions.
Three features render GHR unique: (a) an active ubiquitination system is
required for both endocytosis and degradation in lysosomes; (b) uptake of
receptor is a continuous process, independent of GH binding and Jak2 signal
transduction; (c) only cell surface expression of dimerised GHRs is
controlled by the ubiquitin system. Despite recent progress, molecular
mechanisms underlying GHR endocytosis and degradation are unknown.
Evidence from research on the interferon and prolactin receptors has
identified SCFTrCP as a positive factor for their degradation. This E3 is
known for its regulatory role in cell division and various signal transduction
pathways. Our results show that the ubiquitin ligase SCFTrCP is required for
GHR endocytosis: removal of its mRNA by small interference RNA results
in inhibition of GH uptake. In addition, we demonstrate that interaction
between GHR and beta-TrCP is independent of a canonical DSGxxS motif.
These results show the involvement of a SCF E3 ligase in endocytosis,
thereby regulating GH-sensitivity of cells. In cells that produce both GH and
GHR, the situation is basically the same. In these cells we investigated how
GH affects GHR receptor degradation, and how the Jak/Stat signaling
pathway is regulated. The consequences of these studies are important for
understanding autocrine-activated GHR in fetal and peri-natal, and cancer
GH receptor stimulation changes intracellular protein phosphorylation and activates
the JAK-STAT signalling pathway. The JAK2 - STAT5 components of this pathway
seem critical for growth. Factors of essence for cellular effects of GH include the
duration of GH receptor stimulation and in different species there are sex differences
in GH secretion where males have an episodic and females have a more continuous
mode of GH secretion. At the cellular level, these two types of GH secretion cause
different gene expression patterns to emerge and this is in particular the case for GH
effects on the liver. GH controls important aspects of liver metabolism and it is
interesting to note that some of these seem to depend on the secretory GH pattern.
Another aspect of GH signaling is that the duration of GH receptor signals is related
to changes in SOCS (suppression of cytokine signaling) expression. The SOCS
proteins seem to be part of an intracellular feed back loop that silence GH signals. In
our studies, SOCS2 appears to be a key intracellular regulator of GH sensitivity since
elimination of SOCS2 creates a situation of increased GH sensitivity. Our working
hypothesis is that SOCS2 ubiqitinates the GH receptor and thereby causes its
proteasomal degradation. The concept that SOCS2 is a part of an ubiquitin ligase
complex is substantiated by structural and biochemical findings. Furthermore, the
gene targets for GH induced signals include the SOCS2 gene. In this gene we have
characterized STAT 5 DNA binding elements in proximity to another transcription
factor binding site that is unique for SOCS2 the SOCS protein family. In summary
our data suggest that the liver is an important tissue for GH to exert metabolic
regulation and that SOCS2 is a component that determines GH sensitivity.
Gene expression profiling of the antiangiogenic factor 16K human
prolactin (hPRL) on endothelial cells underlines the key role of NF-kB
and reveals novel mechanisms of action
Sébastien Tabruyn1, Céline Sabatel1, Ngoc-Quynh-Nhu Nguyen1,
Catherine Verhaeghe1, Karolien Castermans2, Ludovic Malvaux1,
Arjan Griffioen2, Joseph Martial1 & Ingrid Struman1
University of Liège, GIGA-Research, B-4000 Sart Tilman, Liège,
Belgium; 2University and Hospital of Maastricht, P.O. Box 5800, NL-6202
Maastricht, The Netherlands.
The 16-kDa N-terminal fragment of human prolactin (16K hPRL) is a potent angiostatic
factor described to prevent tumor growth in mouse models. Using microarray
experiments, we have dissected how the endothelial-cell genome responds to 16K
hPRL treatment. Of the 23.000 transcripts present on the chips, 210 are regulated by
16K hPRL. Bio-informatic analysis and experiments performed on endothelial cells
with various chemical inhibitors clearly suggest that NF-kB is crucial for the direct
regulation of the majority of theses genes. In addition, our results reveal that the
angiogenesis inhibitor 16K hPRL regulates apoptosis and proliferation in endothelial
cells by numerous non-previously identified targets. Unexpectedly, a large proportion of
16K hPRL-regulated genes turned out to be associated with the process of immunity.
16K hPRL induces expression of various chemokines and endothelial adhesion
molecules. These expressions, under the control of NF-kB, result in an enhanced
leukocyte-endothelial cell interaction. Furthermore, analysis of B16-F10 tumor tissues
reveals a higher expression of adhesion molecules (ICAM-1, VCAM-1 or E-selectin) in
endothelial cells and a significantly higher number of infiltrated leukocytes within the
tumors treated with 16K hPRL than in the untreated ones. In conclusion, this study
describes a new anti-tumor mechanism of 16K hPRL. Since cellular immunity against
tumor cells is a crucial step in therapy, the discovery that treatment with 16K hPRL
overcomes tumor-induced anergy may become important for therapeutic perspectives.
Work supported by grants from the F.R.I.A. (“Fonds pour la formation à la
recherche dans l’industrie et l’agriculture”), Télévie, F.N.R.S. (“Fonds national pour
la recherche scientifique”), the Fédération Belge contre le Cancer and the Université
de Liège (Fonds Spéciaux).
Development of human prolactin receptor antagonists
Vincent Goffin1, Vincent Rouet1, Jean-Baptiste Jomain2, Estelle Tallet2,
Christine Kayser1 & Paul A. Kelly2
Inserm, Paris, France; 2University René Descartes Paris 5, Paris, France.
Experimental, clinical and/or epidemiological evidence points to a role for
prolactin (PRL) in the promotion of benign and malignant tumors of the breast
Endocrine Abstracts (2007) Vol 14
9th European Congress of Endocrinology, Budapest, Hungary, 2007
and the prostate. However, therapies reducing PRL levels (dopamine agonists) are
currently not considered for the treatment of these pathologies. Dopamine
agonists only target PRL secretion from the pituitary, while recent observations
suggest that the involvement of autocrine PRL is perhaps even more relevant than
circulating PRL in the growth of breast/prostate tumors. Therefore, alternative
strategies targeting locally-produced PRL warrant investigation.
For many years, we have been working on the development of PRL receptor
antagonists, by introducing mutations into appropriate regions of human PRL.
Ideal antagonists should be high-affinity ligands that bind but do not activate the
PRL receptor, leading to competitive inhibition of endogenous PRL actions. This
presentation will describe the most representative antagonists we have designed,
including their structure-function relationships based on cell and animal studies.
We will also discuss the pros/cons of our lead compound, the pure antagonist
del1-9-G129R-hPRL. Finally, we will address the potential therapeutic
indications of this novel class of molecules.
Polycystic ovary syndrome – S11
The CAG repeat polymorphism of the androgen receptor gene is an
independent risk factor for polycystic ovary syndrome (PCOS)
Andreas Schuering1, Andrea Jurgens1, Jorg Gromoll2, Michael Zitzmann2,
Barbara Sonntag1, Eberhard Nieschlag2, Robert Greb1 & Ludwig Kiesel1
Department of Obsterics and Gynecology Muenster University Hospital,
Muenster, Germany; 2Institute of Reproductive Medicine, Muenster
University Hospital, Muenster, Germany.
Polycystic ovary syndrome (PCOS) is a frequent disorder with a variable
phenotype and a suspected genetic background. Androgenic effects constitute the
central mechanism for the clinical, biochemical and sonographic features of
PCOS. Androgenic effects are transported by the androgen receptor, whose
activity can be modulated by a genetic polymorphism. We investigated the role of
the CAG repeat polymorphism of the androgen receptor in PCOS.
Patients and methods
In the infertility unit of a university clinic 126 patients fulfilling the Rotterdam
criteria of PCOS were compared with 184 controls undergoing a standardized
diagnostic work-up prior to infertility treatment. Individuals were assessed
regarding clinical, endocrine and sonographic parameters indicating the presence
of PCOS. The number of CAG repeats was determined by PCR, labelling with IR800 and PAGE. X-chromosome inactivation was assessed by a methylationsensitive assay. CAG repeat length was compared between groups and correlated
with the extent of oligomenorrhoea. In a regression analysis CAG repeat length
was tested including established risk factors of PCOS.
PCOS patients displayed a shorter mean CAG repeat length compared to
controls (PZ0.001). CAG repeat length correlated inversely with the extent
of oligomenorrhea, a central androgen dependent feature of PCOS (PZ0.007).
In a binomial regression analysis including BMI, LH and testosterone, CAG
repeat length was identified as a novel independent risk factor for PCOS
The CAG repeat polymorphism was identified as a novel independent risk factor
for PCOS. It could constitute a factor in the familial background, convey the
phenotypic variability and transport metabolic consequences of the syndrome.
Genetic markers of polycystic ovary syndrome (PCOS)
Joop Laven
Div Reproductive Medicine, Rotterdam, Netherlands.
Polycystic ovary syndrome (PCOS) represents the most common cause of
anovulatory infertility and its etiology is still unknown. Gene expression
profiles from human PCOS ovaries have identified dysregulated expression of
genes encoding components of several biological pathways or systems
such as Wnt signaling, extracellular matrix components, immunological
factors and androgens which, seem to play a key role in the pathogenesis of
Candidate genes have been extensively studied using Single Nucleotide
Polymorphisms (SNP’s). The impact of functional SNP’s on Gonadotrophins,
Endocrine Abstracts (2007) Vol 14
growth factors and their receptors as well as the consecutive enzymes of the
steroid biosynthesis pathways have been assessed in PCOS. Up till now only
two functional SNP’s have been consistently associated with PCOS. An FSH
receptor and an aromatase polymorphism seem to be more prevalent in
PCOS and are both associated discrete changes in the endocrine environment
in PCOS.
Family studies and linkage analysis is hampered by the lack of large well
phenotyped family cohorts. Recently we have studied PCOS patients from an
isolated population aiming to map gene(s) involved in PCOS susceptibility.
The genome wide association analysis revealed only weak evidence of
association for some markers scattered over the genome. Taken these
findings into account it seems that PCOS constitutes a complex genetic
disease with multiple genetic contributors which, might in turn be modified
through different environmental factors. The individual contribution of these
genetic components to the phenotype of PCOS seems to be very limited and
hence, detection of genetic factors is far from easy.
Hyperandrogenism and metabolic syndrome (MBS) in polycystic ovary
syndrome (PCOS)
Andrea Dunaif
The Feinberg School of Medicine, Northwestern University, Chicago,
United States.
PCOS is a complex genetic disease resulting from the interplay between
susceptibility genes and environmental factors. The syndrome is characterized
by hyperandrogenism, disordered gonadotropin secretion, profound insulin
resistance and, frequently, obesity. It is a leading risk factor for type 2
diabetes mellitus and MBS in adolescent and young adult women. In PCOS,
MBS risk increases with increasing androgen levels, independent of insulin
resistance and obesity, and antagonizing androgen action ameliorates features
of MBS. Obese premenarchal girls have elevated androgen levels.
Hyperandrogenemia is the major reproductive phenotype in families of
women with PCOS, including mothers and brothers. First-degree relatives
also have metabolic phenotypes, including MBS. We have now mapped a
genetic variant conferring PCOS susceptibility to an allele of a dinucleotide
repeat in an intron of the fibrillin-3 gene on chromosome 19p13.2 that is
both linked and associated with the reproductive phenotype. Further, the
PCOS susceptibility allele is associated with metabolic phenotypes in women
with PCOS and their first-degree relatives. These observations suggest that
the cardinal reproductive defect in PCOS, hyperandrogenemia, itself
contributes to metabolic risk. In utero testosterone excess can reproduce
features of the PCOS reproductive and metabolic phenotypes in rodents,
sheep and non-human primates. We propose that hyperandrogenemia
resulting from variation in a gene(s) regulating steroidogenesis causes
many of reproductive and metabolic features of PCOS by programming
actions at critical periods of development as well as by ongoing actions in
the adult. Additional environmental factors, such as obesity, modify these
Individual pharmacological therapy for polycystic ovary syndrome:
lessons from the phenotype
Renato Pasquali
Division of Endocrinology, S. Orsola-Malpighi Hospital, University of
Bologna, Bologna, Italy.
Hyperandrogenism, hyperinsulinemia and insulin resistance are the cardinal
features of most women with the polycystic ovary syndrome (PCOS). They
contribute in different ways to its phenotypic expression, including hirsutism,
menses abnormalities, oligo-anovulation, metabolic disturbances, and susceptibility to develop type 2 diabetes. From the theoretical point of view,
individual pharmacotherapy of PCOS should be planned in order to
counteract the main pathophysiological mechanisms, with the aim of
producing an overall benefit on all clinical and biochemical aspects of the
disorders, after the major complaints of each individual have been
considered. Dietary-induced weight loss and life style modifications should
however represent the first line therapeutic advice for every obese woman
with PCOS. Whether this applies in otherwise normal weight PCOS women
has not yet been demonstrated, although the scientific basis for such an
9th European Congress of Endocrinology, Budapest, Hungary, 2007
approach is appealing, particularly in those with abdominal fatness and
insulin resistance.
Since almost all obese PCOS women and more than half of lean PCOS
women are insulin resistant, therefore presenting some degree of hyperinsulinemia, the use of insulin sensitizers should be suggested in most
patients with PCOS. Their use has been associated with a reduction in
androgen levels, improvement of insulin and insulin resistance, and reversal
of serum lipid abnormalities and PAI-1. This therapy has also been
associated with a decrease in hirsutism and acne, although the main benefit
should be expected on menses abnormalities, anovulation and infertility. In
our experience, at least one third of obese PCOS women improve menses
and ovulation after a short period of treatment with metformin and life style
changes. Antiandrogens have been used for a long-time in the treatment of
hirsutism and hyperandrogenemia, We have recently performed pilot studies
to investigate potential additional effects of long-term treatment with
antiandrogens, and we have found that they can selectively improve visceral
fatness, lipid abnormalities and even insulin resistance, although their main
effect was on hirsutism and hyperandrogenemia.
The dual approach with insulin sensitizers and/or antiandrogens may provide
a rationale for targeting different therapeutical options according to the
required outcomes.
compounds of peptidergic nature, it has recently become apparent that these
neurons also produce several classical neurotrans-mitters. The role of classical
transmitters in regulating energy ba-lance has received less attention in
comparison to neuropeptides. The arcuate nucleus-median eminence area, a
region with a weak blood-brain barrier (BBB), contains at least two neuronal
cell populations that exert oppo-sing actions on energy balance. The majority
of the neurons located in the ventromedial aspect of the arcuate nucleus,
which pro-duce the or-exigenic peptides neuropeptide Y (NPY) and agoutirelated peptide (AGRP), in addition contain the GABA-synthesizing enzyme
glutamic acid decarboxylase (GAD) and the vesicular GABA transporter
(VGAT), thereby supporting their GABAergic nature. Subpopulations of
anorexi-genic neurons producing proopiomelanocortin (POMC)- and cocaineand amphetamine-regulated transcript (CART), located in the ventro-lateral
division of the arcuate nucleus have recently been reported to contain the
vesicular acetylcholine (ACh) transporter (VAChT) and cho-line acetyltransferase (ChAT), markers for cholinergic neurons, or the vesicular glutamate
transporter 2 (VGLUT2), a marker for glutamatergic neurons. In addition, two
new neuropeptides in have been identified in arcuate POMC neurons. In the
lateral hypothalamic area, hypocretin-/orexin neurons express VGLUT1 or
VGLUT2, but not GAD, whereas some melanin-concentrating hormone
(MCH) cells contain GAD. These observations support the view that ACh,
GABA and glutamate, relatively neglected feeding transmitters, are present in
neurons that regulate body weight and consequently may represent important
orexigenic-/anorexigenic mediators that convey information from the hypothalamus to other brain regions that participate in regulation of energy
Hypothalamic network controlling food intake – S12
Processing of metabolic signals in the hypothalamus: the integrative
role of the paraventricular nucleus
Zsolt Liposits1, Ronald Lechan2 & Csaba Fekete1
Institute of Experimental Medicine, Budapest, Hungary; 2Tufts-New
England Medical Center, Boston, MA, United States.
The hypothalamic paraventricular nucleus (PVN) is a major regulatory centre
of energy homeostasis by possessing the unique capability of simultaneously
controlling endocrine axes, water balance and autonomic functions. It
receives neuronal information form orexigenic and anorexigenic cell groups
of the basal hypothalamus that monitor peripheral metabolic signals (leptin,
insulin, ghrelin, glucose, glucocorticoids) and also from brainstem centers
relaying sensory information from visceral organs. In the regulation of
energy homeostasis, the hypophysiotrophic corticotropin-releasing hormone
(CRH) and thyrotropin-releasing hormone (TRH) neuronal systems play a
key role and both neuron populations are wired to neuronal circuits of the
basal hypothalamus and the brainstem. The lecture provides information
about the structural organization, functional domains and major neuronal
connections of the PVN, introduces the novel glutamatergic phenotype of
hypophysiotrophic CRH and TRH systems, elucidates the diverse chemical
nature of their synaptic afferents and describes the structural correlates of
retrograde endocannabinoid signalling acting upon inhibitory and excitatory
presynaptic terminals in the nucleus. The presentation also reveals distinct
hypothalamic and extrahypothalamic sources of neuronal afferents carrying
orexigenic (NPY) and anorexigenic (CART) peptides to TRH and CRH
neurons and demonstrates the impact of the released neuropeptides on the
postsynaptic targets. In addition to rodent data, the interrelationship of NPY
and a-MSH neuronal systems and the features of their projections to CRH
and TRH neurons will be presented in post-mortem human hypothalamic
Supported by grants from the National Science Foundation of Hungary
(OTKA T046492, T046574), NKFP 1A/002/2004 and the Sixth EU Research
Framework Programme (LSHM-CT-2003-503041).
The picture of the hypothalamus is becoming clearer: new concept of
Tamas Horvath, Qian Gao & Sabrina Diano
Yale University School of Medicine, New Haven, CT, United States.
Significant advancements have been made in the last century regarding the
neuronal control of feeding behavior and energy expenditure. The effects and
mechanism of action of various peripheral metabolic signals on the brain have
become clearer. Molecular and genetic tools for visualizing and manipulating
individual components of brain homeostatic systems in combination with
neuroanatomical, electrophysiological, behavioral and pharmacological techniques have begun to elucidate the molecular and neuronal mechanisms of
complex feeding behavior and energy expenditure. This talk will attempt to
highlight some of these advancements that have lead to the current understanding
of the brain’s involvement in the acute and chronic regulation of energy
homeostasis. The case will also be made to suggest that the hypothalamic
circuitry, which governs feeding behavior, is an appropriate model to examine in
order to yield the experimental proof for the causal relationship between synaptic
plasticity and behavior.
Whom is insulin in the brain speaking to?
J Bruening
Abstract unavailable
Neurotransmitter content of orexigenic and anorexigenic neurones
Björn Meister, Katrin Dürr & Ebba Norsted
Karolinska Institutet, Stockholm, Sweden.
During the last two decades attention has been focused on the role of
different neuropeptides in hypothalamic control of feeding behavior. Se-veral
hypothalamic peptides that participate in the control of ingestive behavior are
produced in neuronal cell bodies of the arcuate nucleus and/or the lateral
hypothalamic area. Apart from producing orexigenic or anorexigenic
Glucocorticosteroids – S13
Recent developments in nuclear receptor action
JA Gustafsson
Abstract unavailable
Endocrine Abstracts (2007) Vol 14
9th European Congress of Endocrinology, Budapest, Hungary, 2007
Evaluation of steroid receptor function by gene targeting in mice
Gunther Schuetz
German Cancer Research Center, Dept. of Molecular Biology of the Cell I,
Heidelberg, Germany.
Germline and somatic gene targeting of genes for steroid hormone receptor allows
the characterization of their functions as well as their molecular modes of action. For
the glucocorticoid receptor (GR) multiple modes of action have been identified. The
receptor activates expression of genes, e.g. for gluconeogenic enzymes in
hepatocytes, by binding as a dimer to glucocorticoid response elements (GRE) as
well as by interaction with Stat5, functioning as a coactivator for DNA-bound Stat5.
This functional interdependence of GR and Stat5 is reflected by sharing one third of
their target genes. The receptor is able to repress AP-1/NF kB-dependent expression
of genes involved in inflammation by protein-protein interaction and inhibits
proopiomelanocortian and prolactin expression via binding to negative GREs.
Cre/loxP-mediated generation of somatic mutants of the mineralocorticoid receptor
(MR) circumvents the early lethality observed after germline inactivation.
Inactivation of MR in the forebrain leads to impaired hippocampal-dependent
learning as evidenced in Morris water- and radial maze analyses. Normal circadian
corticosterone levels indicate that the limbic MR is dispensable for the maintenance
of basal hypothalamic-pituitary-adrenal axis activity. The mechanisms underlying
the critical actions of estrogen in the secretion of the gonadotropin-releasing
hormone (GnRH) are unknown. A neuron-specific ERa mutation in the forebrain
leads to infertility and loss of the positive feedback effects of estrogen upon GnRH
neurons. As GnRH neurons do not express ERa, these results indicate that ERaexpressing neuronal afferents to GnRH neurons are critical for the preovulatory
GnRH/LH surge. These genetic approaches to evaluate steroid hormone receptor
activity not only reveal novel neural functions of these regulatory molecules in gene
expression, but also unprecedented modes of their activity.
The 11b-hydroxysteroid dehydrogenase story
Jeremy Tomlinson
University of Birmingham, Birmingham, United Kingdom.
The global epidemic of obesity has heightened the need to understand the
mechanisms that contribute to its pathogenesis and also to design and trial
novel treatments. Patients with glucocorticoid (GC) excess, ‘Cushing’s
syndrome’ share many phenotypic similarities to patients with simple obesity.
GC availability to bind and activate the glucocorticoid receptor (GR) is
controlled by the type 1 isoform of 11b-hydroxysteroid dehydrogenase (11bHSD1) that converts inactive cortisone to cortisol and therefore amplifies local
GC action. We have previously shown that expression of 11b-HSD1 is crucially
important in both adipocyte differentiation and proliferation; Furthermore, overexpression specifically within adipose tissue leads to obesity and insulin
resistance in rodent models. In addition, we have recently been able to show
that inhibition of 11b-HSD1 in human adipose tissue can limit GC induced
lipolysis. Selective 11b-HSD1 inhibitors (selective in that they block the
activity of 11b-HSD1 and not 11b-HSD2 which inactivates cortisone to cortisol
in mineralocorticoid target tissues) are currently in development although not
yet available for use in clinical studies. Rodent studies utilizing these
compounds have shown dramatic improvements in insulin sensitivity as well
as improvements in lipid profiles and atherogenesis. The most fundamental
question is whether these observations in rodents will translate to the clinical
setting. It is likely that within the very near future, data from the first human
studies will be available. If these compounds prove to be as efficacious in
humans, then they may well represent an entirely novel, additional therapeutic
strategy in the treatment of obesity, insulin resistance and type 2 diabetes.
Glucocorticoid sensitivity: consequences for the clinic?
Jan W Koper
Internal Medicine / Endocrinology, Erasmus MC, Rotterdam, Netherlands.
Glucocorticoids (GCs) exert a wide variety of functions throughout the human body,
including mediation of the stress response, regulation of lipid and glucose
metabolism, immunosuppressive and anti-inflammatory actions, vascular effects,
increase of bone resorption, as well as effects on the development and function of
numerous organs. The immuno-suppressive effects of GCs are routinely used in the
treatment of chronic inflammatory or immune diseases (e.g. inflammatory bowel
Endocrine Abstracts (2007) Vol 14
disease, asthma). However, severe side effects (including diabetes and osteoporosis)
are associated with GC-treatment, limiting its therapeutic usefulness.
Within the normal population, there exists a considerable inter-individual
variation in GC sensitivity. Whereas some patients develop side effects on relatively
low doses of topically administered GCs, others appear to be less sensitive to GCs, as
they do not show an adequate improvement in response to treatment even on high
doses. Some patients are even resistant to the anti-inflammatory effects of GCs while
at the same time showing side effects known to reflect normal sensitivity to GCs,
including suppression of the hypothalamic-pituitary-adrenal axis. Variability in GC
sensitivity can be divided into GC resistance and GC hypersensitivity.
The signaling pathway of GCs is a complex process, in which distinct pathways
are involved that can influence GC sensitivity. Also, other mechanisms such as the
transport, local conversion and degradation of GCs play a role in the intracellular
bioavailability of GCs.
Here we will discuss the possible consequences for the clinic of genetic variation
in genes involved in the GC signalling pathway, and resulting in inter-individual
differences in glucocorticoid sensitivity.
Trojan horses for hormones – S14
Alpha-fetoprotein protects the developing female brain from estrogens
Julie Bakker1, Christelle De Mees2, Jacques Balthazart1 & Claude Szpirer2
University of Liège, Liège, Belgium; 2Université Libre de Bruxelles,
Gosselies, Belgium.
The classic view of sexual differentiation in mammalian species holds that sex
differences in the brain and behavior develop under the influence of estrogens derived
from the neural aromatization of testosterone: the brain develops as male in the
presence of estrogens and as female in their absence. In agreement with this view, it has
been proposed that the female brain needs to be protected from estrogens produced by
the placenta and that alpha-fetoprotein (AFP) - a major fetal plasma protein present in
many developing vertebrate species and produced transiently in great quantities by the
hepatocytes of the fetal liver– is the most likely candidate to achieve this protection
because of its estrogen-binding capacity. However, the idea that the female brain
develops in the absence of estrogens and the role of AFP in protecting the brain against
the differentiating action of estrogens have been challenged. First, there is
accumulating evidence that the normal development of the female brain might
actually require the presence of estrogens. Second, the presence of AFP within neurons
in the absence of any evidence for local AFP synthesis suggests that AFP is transported
from the periphery into the brain. It was thus proposed as well that AFP acts as a carrier,
which actively transports estrogens into target brain cells and, by doing so, has an
active role in the development of the female brain. The availability of AFP mutant mice
(AFP-KO) now finally allowed us to resolve this longstanding controversy concerning
the role of AFP in brain sexual differentiation, and thus to determine whether prenatal
estrogens contribute to the development of the female brain. We showed that the brain
and behavior of female AFP-KO mice were masculinized and defeminized. However,
when estrogen production was blocked by fetal treatment with an aromatase inhibitor,
the feminine phenotype of these mice was rescued. These results clearly demonstrate
that the principal action of prenatal estrogen exposure is to defeminize the brain and
that AFP normally binds estradiol circulating in the female fetus and thereby protects
the developing brain from defeminization.
Role of endocytic receptors in cellular uptake of steroid hormones
Thomas Willnow1, Annette Hammes1, Thomas Andreassen2 &
Anders Nykjaer2
Max-Delbrueck-Center for Molecular Medicine, Berlin, Germany;
University of Aarhus, Aarhus, Denmark.
Androgens and estrogens are transported bound to the sex hormone binding globulin
(SHBG). SHBG is believed to keep sex steroids inactive and to control the amount of
free hormones that enter cells by passive diffusion. Contrary to the free hormone
hypothesis, we demonstrate that megalin, an endocytic receptor in reproductive
tissues acts as a pathway for cellular uptake of biologically active androgens and
estrogens bound to SHBG. In line with this function, lack of receptor expression in
megalin knockout mice results in impaired descent of the testes into the scrotum in
males and in blockade of vaginal opening in females. Both processes are critically
dependent on sex steroid signaling and similar defects are seen in animals treated with
androgen or estrogen receptor antagonists. Thus, our findings uncover the existence of
endocytic pathways for protein-bound androgens and estrogens, and their crucial role
in development of the reproductive organs.
9th European Congress of Endocrinology, Budapest, Hungary, 2007
Hepatic deiodinase activity is dispensable for the maintenance of
normal thyroid hormone levels in mice
Ulrich Schweizer
Charité Universitätsmedizin Berlin, Berlin, Germany.
The main product of the thyroid is thyroxine (T4). However, the physiological
ligand of nuclear thyroid hormone receptors is triiodothyronine, T3. Deiodination
of T4 to yield T3 is achieved by 5 0 -deiodinase activity. Type I-deiodinase (Dio1)
was the first deiodinase cloned and its strong expression in liver and kidny,
together with the size of these organs, suggested a role for Dio1 in peripheral
conversion of T4 to T3. Later, Dio2 and Dio3 were cloned, enzymes with a more
restricted pattern of expression that mediate 5 0 - and 5-deiodination, respectively.
A model emerged in which activation and inactivation of thyroid hormones is
governed by the concerted action of tissue-specific deiodinase expression. One
aspect of this familiar textbook model, a central role of hepatic Dio1 in T3
production, was recently challenged. Since all deiodinase enzymes are
selenoproteins, targeted removal of the gene encoding selenocysteine tRNA
(Trsp) allowed the liver-specific inactivation of Dio1 activity. Using AlbuminCre; Trsp fl/fl mice we showed that loss of hepatic deiodinase did not disturb
circulating thyroid hormone levels. Moreover, deiodinase activities in other
organs did not show compensatory up-regulation. Data derived from the
conventional Dio1 knockout mice suggest that hepatic Dio1 is involved in the
re-cycling of iodine from iodothyroines. Since the targeted inactivation of Dio2
perturbed pituitary feedback regulation, but did not reduce serum T3 levels, the
question remains which deiodinase provides circulating T3. We have taken these
investigations further and will present data regarding the effects of thyroidspecific Trsp inactivation in transgenic mice.
IGF-independent actions of IGFBPs
Jean-Marc Ricort
INSERM U515, Paris, France; 2ENS de CACHAN, Paris, France.
The discovery that IGF binding proteins (IGFBPs) are capable of action
independently of ligand binding opened up a broad scope of investigation into the
mechanisms by which the IGFBPs elicit their intrinsic cellular effects. Numerous
studies have demonstrated the special role of IGFBPs in as diverse processes as
cell proliferation, migration and survival/apoptosis. However, the pathways by
which these actions occur have not been completely defined but interactions of
IGFBPs with other proteins or biomolecules must be involved.
IGFBPs can bind to many partners other than IGFs, although the relationship
between most of these binding interactions and IGFBP actions remains uncertain.
Several studies have identified membrane proteins that bind IGFBPs with
relatively high affinity. These include proteins known to be involved in other
signalling pathways (such as integrin receptor and TGFb receptor) and putative
receptors, the precise nature of which remains to be determined. Moreover,
IGFBPs can also bind to intracellular (even nuclear) proteins.
Therefore, an exciting challenge in identifying the signalling pathways modulated
by such interactions between IGFBPs and their partners is currently open.
Novel bone hormones and regulators – S15
Sclerostin, an osteocyte-produced regulator of bone formation
Socrates Papapoulos
Leiden University Medical Center, Leiden, Netherlands.
Sclerosteosis and van Buchem disease are closely related, rare sclerosing
disorders characterized by substantial increase in bone mass of good quality
which is due to increased bone formation. Both diseases have been linked to
deficiency of the SOST gene product sclerostin, which in the adult is localized
exclusively in osteocytes, the most abundant bone cell. In particular sclerostin is
localized in mature osteocytes in mineralised cortical and cancellous bone, it
inhibits the activity of osteoblasts and prevents them from promoting excessive
bone formation. It is, thus, a negative regulator of bone formation. Sclerostin may
be transported by the canaliculi to the bone surface where it inhibits the boneforming activity of osteoblasts.. In this respect it serves the function of the
unknown inhibitory factor proposed by Marotti and Martin that is secreted by
mature osteocytes and communicates with osteoblasts at a forming surface
causing the adjacent osteoblast to slow osteoid formation.
Because of its structural similarity to the DAN family of glycoproteins, it was
originally thought that sclerostin is a BMP antagonist. Whilst sclerostin inhibits BMPstimulated bone formation, it does not affect BMP signaling and is distinct from
classical BMP antagonists. Instead it antagonizes Wnt signaling in osteoblastic cells.
The human high bone mass (HBM) phenotype is an autosomal dominant condition
that, like sclerosteosis and van Buchem disease, is characterized by increased bone
mass due to enhanced bone formation in the presence of normal bone resorption. It is
due to mutations of the LRP5 gene that make it resistant to the inhibitory action of
Dkk1, thereby increasing Wnt signalling. The observations that sclerostin antagonizes
Wnt signaling rather than BMP signaling raises the possibility that these skeletal
diseases are due to increased activity of the same signaling pathway: LRP5-mediated
canonical Wnt signaling.
The restricted expression pattern of sclerostin and the exclusive bone phenotype of
good quality of patients with sclerosteosis and van Buchem diseases provide a basis
for the design of therapeutics that specifically stimulate bone formation, an action of
primary importance for the management of patients with osteoporosis. As sclerostin
is a secreted protein, one approach to achieve this is to develop humanized
monoclonal antibodies capable of inhibiting the biological activity of sclerostin,
mimicking, thus, the absence of sclerostin in sclerosteosis. Preliminary results of
such approaches in animal models have been very encouraging.
Hormonal regulation of periosteal bone growth
Dirk Vanderschueren & Katrien Venken
Unversity Hospitals, Leuven, Belgium.
In light of the gender differences in bone geometry, sex steroids have been proposed as
key regulators of pubertal periosteal bone formation. Sex steroids may affect
periosteal bone apposition following activation of sex steroid receptors [androgen
receptor (AR), estrogen receptor alpha (ERa) or beta (ERb)]. Traditionally, it has
been assumed that AR-mediated androgen action stimulates periosteal bone
formation and thereby determines the larger bone size in males, whereas estrogens
suppress periosteal bone formation resulting in a smaller bone size in females.
However, optimal periosteal growth in the male is only obtained in the presence of
both AR and ER activation as demonstrated in mice with a disruption of the AR gene
and in an adolescent man with a mutation in the gene encoding the aromatase enzyme.
Moreover, the bone phenotypes of ERa, ERb and double knock-out mice indicate that
the presence of ERa and ERb increase and decrease periosteal bone expansion,
respectively (the former is observed in males and females, the latter only in females).
Furthermore, administration of an aromatase inhibitor that blocks the conversion of
androgens into estrogens also limits periosteal bone expansion in growing male mice
and rats. Beside sex steroids, growth hormone (GH) and insulin-like growth factor-I
(IGF-I) are also major determinants of radial skeletal growth. Moreover, sex steroids
and GH-IGF-I closely interact in pubertal life in order to obtain optimal stimulation of
periosteal bone formation. In this context, targeted disruption of ERa in mice or
pharmacological inhibition of aromatization of androgens in mice and rats reduce
serum IGF. Such finding raises the question to what extent sex steroids are able to
affect periosteal bone formation independently from the GH-IGF-I axis. We therefore
studied periosteal bone formation following androgen or estrogen administration in
orchidectomized male mice with disrupted growth hormone receptor (GHR). GHR
activation appears the main determinant of radial bone expansion, but both GHR
signaling and androgen action are independently and cooperatively needed for
optimal stimulation of periosteal growth in the male during puberty. Interestingly,
estrogen treatment rescued periosteal bone formation in mice with disrupted growth
hormone receptor which was explained by a stimulation of IGF-I synthesis in the liver
independently from GHR activation.
In conclusion, optimal periosteal bone formation in the male during puberty
primarily depends on a functional GH-IGF-I axis, followed by activation of the AR.
However, both GH/IGF-I and androgens are independently needed for optimal
stimulation of radial bone growth. Moreover, part of the androgen action on periosteal
bone may be explained by aromatization and subsequent ERa activation. The latter
may interact with GH/IGF-I and may influence periosteal growth by estrogen-related
changes in serum IGF-I.
Wnt signaling and LRP 5/6 regulation of bone mass
Peter Bodine
Wyeth Research, Collegeville, PA, United States.
Wnts are a large family of carbohydrate- and lipid-modified growth factors that
mediate essential biological processes such as embryogenesis, morphogenesis and
organogenesis. These proteins bind to a membrane receptor complex comprised of a
Endocrine Abstracts (2007) Vol 14
9th European Congress of Endocrinology, Budapest, Hungary, 2007
frizzled (FZD) G-protein-coupled receptor and a low-density lipoprotein (LDL)
receptor-related protein (LRP). The formation of this ligand-receptor complex initiates
a number of signaling cascades that includes the canonical/beta-catenin pathway as
well as several noncanonical pathways. In recent years, canonical Wnt signaling has
been reported to play a significant role in the control of bone formation and remodeling.
Clinical studies have found that mutations in LRP-5 are associated with bone mineral
density and fractures. Investigations of knockout and transgenic mouse models of Wnt
pathway components including Wnt-10b, LRP-5 and -6, secreted frizzled-related
protein-1 and -4, dickkopf-1 and -2, Sclerostin, axin-2, beta-catenin and T-cell factor-1
have shown that canonical signaling modulates almost all aspects of osteoblast
physiology including proliferation, differentiation, function, mineralization, apoptosis
and mechanosensory perception as well as coupling to osteoclasts. In addition,
preclinical studies with pharmacologic compounds such as those that inhibit glycogen
synthase kinase-3beta support the importance of the canonical pathway in modulation
bone formation. Moreover, well-established bone forming agents like bone
morphogenetic proteins and parathyroid hormone have been demonstrated to intersect
and utilize components of Wnt signaling pathways. Future research in this swiftly
expanding area of skeletal biology should focus on understanding Wnt/FZD specificity
in the control of bone cell physiology, the role of noncanonical pathways in bone
remodeling, the interplay between Wnt signaling and other bone metabolic pathways
and direct actions of Wnts on cells of the osteoclast lineage.
Thyroid hormones/TR and bone
Graham R Williams
Molecular Endocrinology Group, MRC CSC, Hammersmith Hospital,
Imperial College London, London, United Kingdom.
Childhood hypothyroidism results in severely delayed skeletal development
whereas adult thyrotoxicosis is associated with a 3–4 fold increase in osteoporotic
fracture. To investigate molecular mechanisms underlying these abnormalities we
characterized the skeletal phenotypes of mice harboring dominant negative
mutations (TRa1PV/C, TRa1R384C/C, TRbPV/PV) or deletions (TRa0/0,
TRbK/K) of the genes encoding TRa and TRb. Endochondral ossification,
linear growth and bone mineralization were retarded in TRa0/0 mice and more
severely delayed in TRa1 dominant-negative mutants. In contrast, these
parameters were all advanced in TRb knockout and PV-mutant mice. In adults,
3D bone micro-architecture and micro-mineralization densities were analyzed by
quantitative backscattered electron scanning electron microscopy. TRa mice
displayed increased cortical bone width, and an 8–9 fold increase in trabecular
bone volume with increased thickness of individual trabeculae and greater microarchitectural complexity. In contrast, analysis of all these parameters including
quantitation of bone micro-mineralization density revealed TRb mutants were
markedly osteoporotic. Studies of T3-target gene expression revealed phenotypes
of skeletal hypothyroidism in TRa mutant mice but skeletal thyrotoxicosis in TRb
mutants. We further demonstrated that TRa is expressed at 15-fold higher levels
in bone than TRb, whereas TRb is predominantly expressed in hypothalamus and
pituitary and controls negative feedback regulation of TRH and TSH.
Accordingly, TRa mutant mice were euthyroid whereas TRbPV/PV and
TRbK/K displayed pituitary resistance to thyroid hormone with elevated
circulating thyroid hormone levels. This analysis of a series of TR mutant mice
with differing genetic backgrounds unequivocally demonstrates that TRa is the
predominant TR isoform in bone, and shows that skeletal responses to disrupted
TRb signaling result from effects of the mutation on systemic thyroid status.
Immune-endocrine turmoil of pregnancy – S16
Endocrine diseases during pregnancy
Risto Kaaja
Helsinki University Hospital, Helsinki, Finland.
Successful pregnancy depends on the ability of the maternal immune system to
tolerate a genetically incompatible feto-placental unit. One of the important
adaptations leading to this immuno-tolerance is the shift, at implantation, of Th 1
dominance to Th 2 dominance. Successful pregnancy is a Th2 dominant immune
state, therefore, it is not surprising that women with a Th 1 dominant immune
disease such as rheumatoid arthritis, thyroiditis or multiple sclerosis improve
during pregnancy, while patients suffering from Th 2 dependent immune disease,
such as SLE, fare worse during pregnancy.
Interestingly, three autoimmune diseases, rheumatoid arthritis, multiple
sclerosis and thyroiditis, that are reported to ameliorate or stabilize during
pregnancy in the majority of women, are more likely to relapse during the year
Endocrine Abstracts (2007) Vol 14
after delivery. The postpartum period can be regarded as a time of ongoing
heightened inflammatory activity. The onset of rheumatoid arthritis is five times
more likely in the puerperal period than at any other time. Multiple sclerosis is
known to ameliorate during the last trimester of pregnancy. After delivery, the
relapse rate is higher than that before pregnancy. Importantly, the decrease in the
relapse rate during pregnancy was more marked than any drug mediated
therapeutic effect reported to date. Of the acute endocrine emergencies an acute
form of Sheehan’s may go unrecognized, leading to unnecessary maternal deaths.
Cushing’s syndrome has very bad consequences for the fetus and must be
diagnosed and treated urgently, if not emergently. Pheochromocytomas are
always endocrine emergencies requiring urgent and sometimes emergent
treatment. Hyperparathyroidism is usually mild, but severe hypercalcemia can
be a true endocrine emergency.
Recognition of the interactions of these endocrine conditions and their specific
treatments with the complicated maternal-fetal unit makes their diagnosis and
treatment simultaneously both difficult and extremely rewarding.
Estetrol (E4), the forgotten fetal steroid
Herjan Coelingh Bennink & Monique Visser
Pantarhei Bioscience B.V., Holland, Netherlands.
Estetrol (E4) is a natural human steroid, produced exclusively during pregnancy
by the fetal liver. Estetrol has been discovered in 1965 by Diczfalusy at the
Karolinska Institute in Stockholm.
The role of E4 in embryonic physiology and/or human pregnancy is not known.
During human pregnancy E4 is detectable from 9 weeks pregnancy onwards.
Estetrol reaches the maternal blood circulation via the placenta. Maternal and
fetal E4 concentrations increase exponentially during pregnancy and peak at high
levels at term with fetal levels about 10–20 times higher than maternal levels as
confirmed by data obtained by Pantarhei Bioscience. Based on low receptor
binding compared to estradiol (E2), E4 was thought to be a weak estrogen. Since
the early eighties the molecule has been neglected.
The pharmacological properties of oral E4 as investigated by Pantarhei
Bioscience can be summarised as follows. Estetrol is orally bioavailable in the rat
and acts as an estrogen on bone, brain, vagina and endometrium. Estetrol
suppresses hot flushes and inhibits ovulation. Surprisingly, E4 acts as an estrogen
antagonist on the breast since it was shown to prevent development of breast
tumors and to remove pre-existing breast tumors in the DMBA rat model.
In phase I studies in early postmenopausal women E4 showed high oral
absorption, full dose linearity, high bioavailability, low inter-subject variability and a
long elimination half-life with a mean of 28 hours. Estetrol appeared to be
efficacious, safe and without side-effects up to a dose of 20 mg per day for 28 days.
Estetrol will be developed further for the treatment of breast cancer, prostate
cancer, osteoporosis and for those Th2-mediated auto-immune diseases, that are
known to improve during pregnancy.
Regulatory T cells in pregnancy
Ana Claudia Zenclussen1, Juliane Rau1, Catharina Thuere1,
Anne Schumacher1, Gerolf Zimmermann2, Hans-Dieter Volk1 &
Henry Alexander2
Charite, Institute of Medical Immunology, Berlin, Germany; 2University of
Leipzig, Leipzig, Germany.
The survival of the semiallogeneic fetus within the mother is thought to be due to
mechanisms of immunological tolerance. Regulatory T cells (Treg) are believed
to have a crucial role in maintaining pregnancy by creating a transient tolerant
microenvironment within the maternal uterus as former studies confirmed. We
have evidences that Treg expand in lymph nodes from normal pregnant mice
already on day 2 of pregnancy. Abortion-prone mice present diminished numbers
of Treg in immune organs throughout pregnancy. As both pregnancy
combinations (normal pregnant and abortion-prone mice) present similar levels
of progesterone, estriol and estrone, hormones do not seem to be involved in Treg
expansion. However, they may be involved in their recruitment into the vaginal
An enormous augmentation in the number of TCRabCCD4KCD8Kfoxp3C
cells in vaginal mucus from normal pregnant animals already on day 0.5 after
conception, followed by an increase in Treg numbers in lymph nodes, suggest that
Treg need to be activated by male antigens for being protective. The antigen
presentation would take place in the periphery e.g. in vaginal mucus, the first site
9th European Congress of Endocrinology, Budapest, Hungary, 2007
of contact with paternal antigens, directly after insemination as we could confirm
by identifying paternal antigens and paternal APCs at this site. This explains
previous observations on Treg transfer being effective in preventing abortion if
done on days 0–2 of pregnancy but not later. Interestingly, mating CBA/J females
with vasectomized BALB/c males generated foxp3C cells in lymph nodes
draining the uterus, while pseudopregnancy induced by mechanical stimulation
did not. Treg-induced tolerance is transient, as Treg came back to the normal
levels after the disappearance of the paternal/fetal antigens, 14 days post-partum.
The molecules responsible for Treg recruitment immediately after copulation
are being currently studied in our laboratory. Besides, running clinical studies will
help us clarifying whether similar pathways are taking place in humans.
of the tumors SST2. The same is true for most endocrine pancreatic tumors,
except for benign insulin producing tumors that has a lower expression (50%).
Signaling through SST2 inhibit hormone release and causes antiproliferation,
whereas stimulation of SST2 and 3 causes apoptosis. 111Indium-DTPA-octreotide
(Octreoscanw) can be applied for localisation and staging of neuroendocrine
tumors. Labelling of octreotide with either 177Lutetium or 90Yttrium is used for
tumor targeted radioactive treatment (PRRT). The use of somatostatin analogues,
Octreotide and Lanreotide, has been a real break-through in the management of
functioning neuroendocrine tumors. Symptomatic and biochemical improvement
has been noticed in 50-60% of the patients and tumor reduction in 5–10%. A new
somatostatin analogue – SOM230 – has been applied in phase-2-trials. This
analogue is binding with high affinity to receptor 1, 2, 3 and 5, but not 4. It has
already demonstrated significant symptomatic effects in patients with functioning
neuroendocrine tumors, resistant to octreotide treatment. In the future analysis of
the expression pattern of different somatostatin receptors in neuroendocrine
tumors will be important, particularly if new somatostatin analogues will be
The effect of pregnancy on immune disease
M. Hazes
The Netherlands.
Abstract Unavailable
Peptide receptor therapy
DJ Kwekkeboom
The Netherlands.
Abstract unavailable
Somatostatin receptors in health and disease – S17
Pro and contra of SRIF analogue therapy in pituitary tumors
AJ van der Lely
Erasmus MC, Rotterdam, Netherlands.
Long-acting somatostatin analogues normalize serum IGF-I levels in about 65%
of acromegalic patients. Somatostatin analogs reduce GH secretion but also
induce GH resistance of the liver because of low portal insulin levels; i.e. patients
have a relative high GH level and a GH resistance of the liver which results in a
relative low IGF-I action because of high IGFBP1 levels, but the other tissues still
have normal GH sensitivity. One might predict that long-term follow-up of
treated acromegalic patients is mandatory for find out the potential differential
effects of the various medical treatment modalities. Especially as nowadays, the
combination of somatostatin analogues and GH-R antagonists will be used by
clinicians more frequently in order to decrease administration interval of the
GH-R antagonist, as well as reduce its dose that is necessary to control disease
activity in those acromegalic patients that do not respond to long-acting
somatostatin monotherapy. The novel multiligand analogue SOM230 might
increase the number of patients that can be biochemically controlled. SOM230
inhibits free IGF-I in a more sustained fashion compared to octreotide, implying
longer duration of action. The superior action of octreotide compared with
SOM230 in stimulating IGFBP-1 levels in acromegalic patients, suggests direct
regulation of IGFBP-1 by somatostatin analogues via the somatostatin subtype 2
receptor. In summary, somatostatin analogs are the only compounds of which, at
least in acromegaly, it has been shown that they reduce tumor size in those
subjects that express sst on their pituitary tumors. However, the expression of sst
on other tissues, involved in glucose metabolism, might have a negative influence
on glucose metabolism on some patients
Somatostatin receptors in neuroendocrine tumors
Kjell Oberg
Department of Endocrine Oncology, Uppsala University Hospital,
Upppsala, Sweden.
A unique feature of neuroendocrine tumors is that they express peptide hormone
receptors. All five subtypes of somatostatin receptors are expressed in
neuroendocrine tumors with dominance for receptor type 2 (SST2). Stimulation
of SST2 can not only inhibit hormone release from the tumor, but also tumor cell
growth. Both SST2 and 3 are involved in apoptosis of neuroendocrine tumor cells.
SST’s in intratumoral blood vessels might implicate a role of anti-angiogenesis of
somatostatin and somatostatin analogues. Midgut carcinoids express about 80%
Cortistatin, a multi-functional somatostatin receptor analog
Luis de Lecea
Stanford University, Palo Alto, CA, United States.
Cortistatin is a neuropeptide that belongs to the somatostatin family, and shares 11
of its 14 amino acid residues with somatostatin. Studies in the central nervous
system have shown that cortistatin has activities different from somatostatin,
including enhancing slow wave sleep and selective conductances. However, in
the periphery cortistatin appears to act as a somatostatin receptor analog. We have
generated cortistatin ko mice and have analyzed the molecular, behavioral and
immunological consequences of cortistatin deficiency. Our data suggest that
cortistatin is a parallel system to somatostatin in the central nervous system, and
may have specific and relevant functions in the immune system.
Puberty and hypogonadism – S18
Endocrine disorders of puberty
Marek Niedziela
Poznan University of Medical Sciences, Poznan, Poland.
Puberty is a process in humans that leads to the development of secondary
sexual characteristics and reproductive capabilities. The physical changes of
puberty result from two separate and independent but overlapping processes:
gonadarche and adrenarche. The activation of hypothalamic-pituitary-gonadal
(HPG) axis plays a key role in gonadarche whereas body weight and body
mass index are postulated as triggering the adrenarche. The impairment of
this cascade will result in temporary or permanent disorders of reproductive
endocrine function. This primarily endocrine process can be disrupted by
genetic and environmental factors. The timing of pubertal onset is defined as
normal if occurs between the ages of 8 and 13 years in girls and 9 and 14
years in boys. However the controversies concerning the age limit of onset of
puberty have been raised. Precocity can be central (GnRH-dependent) or
peripheral (GnRH-independent) in its etiology and iso- or heterosexual
(consistent or inconsistent with gender). Central precocious puberty in girls is
rather idiopathic whereas in boys has predominantly pathologic cause.
Peripheral precocious puberty occurs rarely. The most common cause of
delayed puberty is constitutional delay of growth and puberty, especially in
Endocrine Abstracts (2007) Vol 14
9th European Congress of Endocrinology, Budapest, Hungary, 2007
boys. However the other common etiologies should be considered: 1.
Functional hypogonadotropic hypogonadism; 2. Permanent hypogonadotrophic
hypogonadism and 3. Permanent hypergonadotrophic hypogonadism. The
treatment strategy is highly specific for each single disorder. Genetic studies
on newly detected factors regulating HPG axis (eg. KiSS-1 and GPR54 as
gatekeepers of gonadotropin-releasing hormone release neurons or FGFR1)
may improve understanding of normal variation in pubertal timing and
provide further directions for treatment.
Role of sex steroids and nitric oxide in male sexual function
Vincenzo Rochira
Department of Medicine, Endocrinology and Metabolism, Geriatrics,
University of Modena and Reggio Emilia, Modena, Italy.
Nitric oxide (NO) is the main final effector for penile erection achievement and
maintenance in men and it constitutes a crucial target for therapeutical
strategies addressed to the treatment of erectile dysfunction. The role of sex
steroids penile NO pathway is still unclear, but some data suggest a positive
role of androgens. In order to study the effects of sildenafil on human sleeprelated erections according to the state of androgenization, we recently
evaluated the effects of sildenafil (S) or placebo (P) on sleep-related erections
in hypogonadal (H) men with very low testosterone levels: !200 ng/dl
(6.93 nmol/L), before (HKT) and during (HCT) testosterone replacement
treatment (T) and in control (C) subjects. Sleep-related erections were impaired
in hypogonadal men before testosterone treatment (HKTCP) when compared
with control subjects taking placebo (CCP). Testosterone alone (HCTCP)
and sildenafil alone (HKTCS) restored normal sleep related erections,
however, the combined treatment (sildenafil C testosterone) resulted in the
maximum positive effect on sleep-related erections parameters. The effects of
testosterone plus sildenafil resulted higher than the sum of the effects of both
drugs used alone. Sildenafil administered at bedtime improves sleep-related
erections in hypogonadal men, suggesting that the nitric oxide pathway may be
pharmacologically enrolled and enhanced despite low serum testosterone.
Furthermore, these data strongly support the idea of a synergic effect of
sildenafil and testosterone on sleep-related erections. In clinical practice this
concept is supported by the evidence that testosterone treatment restores
sildenafil efficacy in subjects with erectile dysfunction and low to low-normal
serum testosterone, who were non-responder to sildenafil alone. The combined
treatment seems to be efficacious also in subjects with metabolic diseases such
as diabetes mellitus. Whether or not estrogens are able to modulate NO
pathway within the penile tissue remains to be ascertained in detail, but an
androgen-estrogen cross-talk seems to be involved in the pathophysiology of
male penile erection, but concerning estrogens dose-response and in vivo
studies are lacking.
Clinical management of premature ovarian failure
S Christin-Maitre
Abstract unavailable
Gonadal function in ageing men
Jean M Kaufman
Ghent University Hospital, Ghent, Belgium.
Involutional changes of gonadal function in healthy ageing men are
progressive and mostly of modest amplitude with considerable betweensubject variability. Albeit some men may remain relatively spared, the
occurrence of age-related changes are nevertheless well documented at the
Endocrine Abstracts (2007) Vol 14
population level in both cross-sectional and longitudinal observational studies.
These changes affect Sertoli cell function and spermatogenesis as well as
Leydig cell function and testosterone (T) production and they are the
consequence of both primary testicular changes and alterations in neuroendocrine regulation of gonadotropin secretion. Men retain fertility until old
age, but there are age-related reductions of testicular size, Sertoli cell mass
and spermatogenic activity with moderate decline in semen volume, sperm
motility and morphology with maintained sperm concentration. This is
reflected in a progressive increase of FSH levels and marked decrease of the
ratio of serum levels of inhibin over FSH. More than 20% healthy men over
60 yr present with serum T levels below the range for young men. This is the
consequence of decreased Leydig cell mass and altered hypothalamic
regulation of LH secretion. Together with a progressive age-related increase
in serum SHBG levels, this results in a 50% reduction of the serum
bioavailable fractions of serum T (i.e. free and non SHBG-bound T) between
age 20 and 75 yr. Although the clinical changes of ageing in men are
reminiscent of signs and symptoms of hypogonadism in young men, clinical
relevancy of the decline in sex steroid levels in ageing men has not been
unequivocally established and minimal androgen requirement for elderly men
remain poorly defined and are likely to vary between individuals. Therefore,
borderline androgen deficiency cannot be reliably diagnosed in the elderly and
differentiation between “substitutive” and “pharmacological” androgen
administration is not possible. Awaiting documentation of long-term riskbenefit ratio, a conservative approach to androgen treatment in elderly men
seems appropriate.
Pituitary cell biology – S19
Role of folliculo-stellate cells in the anterior pituitary: a historical
Wilfried Allaerts
Nijverdal, Netherlands.
Cell developmental studies have frequently used the hypophysis as a model for
complex differentiation pathways. Nevertheless, many of this work has been
focused on the hormone-producing cell types of the anterior pituitary (AP),
whereas the so-called folliculo-stellate cells (FS cells) have often been ignored in
these studies. FS cells form an enigmatic, non-hormone-secreting cell group.
Initially designated as supportive cells, they were soon found to be the putative
source of many, newly discovered peptides and growth factors. They were also
shown to be involved in paracrine communication with other pituitary cell types
and in communication through electrically coupled syncytia. Moreover, several
authors have provided evidence for their possible role in pituitary cell
regeneration and processes of cell transdifferentiation.
So far, little is known about the precise embryological origin of the mature FS
cells. Since the discovery of adult stem cell populations in various organs, several
authors have indicated a possible role of FS cells in this respect too. Also new
evidence relating FS cells to the production of cytokines, their involvement in
nitric oxide signaling and an in vitro immune accessory function were added to
the list of physiological roles of the FS cells. The question however is whether
these multiple functions can be ascribed to one, homogeneous but pluripotent cell
type, or whether the pituitary FS cells represent a heterogeneous cell group
consisting of various subtypes (unrelated or related to a common ancestor cell
We previously demonstrated the partial overlap between immunocompetent
MHC-class II-positive dendritic cells (DC) and S100 protein-positive FS cells. In
a transgenic mouse model for conditional DC ablation, we showed that early
macrophages could be prevented from colonizing the AP. Also, around
embryonic day 12 of chick development, early macrophages were detected in
the anterior pituitary before pituitary cell differentiation was completed and well
before FS cells obtained their mature phenotype.
The present historical review of FS cell research highlights the importance of
conceptual frameworks in cell lineage studies. Cell biological systems from the
past, like the reticulo-endothelial system or the more recent mononuclear
phagocyte system, nowadays are considered obsolete and incomplete. Still there
is a need for theoretical frameworks in new annotation studies and for the clinical
applications of contemporary research. The FS cell model not only is very
interesting for the study of development of organs with two or more embryonic
Anlagen. Also, questions related to the therapeutic usefulness of pituitary cell
regeneration are envisaged in cases of pituitary dysfunctioning or
9th European Congress of Endocrinology, Budapest, Hungary, 2007
Signalling in pituitary tumours: the roles of Akt, BRAF, AIP and other
novel agents
Márta Korbonits
Department of Endocrinology, Barts and the London Medical School,
London, United Kingdom.
Adipocytokines and pituitary function
Maria M. Malagon1, Francisca Rodrı́guez-Pacheco1, Antonio J. Martı́nezFuentes1, Rafael Vázquez-Martı́nez1, Manuel Tena-Sempere1,
Carlos Diéguez2 & Justo P. Castaño1
Dept. Cell Biology, Physiology and Immunology. Univ. Córdoba, Cordoba,
Spain; 2Dept. Physiology, Univ. Santiago de Compostela, Santiago de
Compostela, Spain.
Numerous growth factors, oncogenes, tumour suppressor genes and hormonal
influences have been implicated in pituitary tumorigenesis. We have demonstrated that the PI3K-Akt pathway is upregulated in pituitary tumours and since
Akt is a major downstream signalling molecule of growth factor-liganded
tyrosine kinase receptors it is possible that an abnormality at this level could be
the primary driver of pituitary tumorigenesis. The serine/threonine kinase B-Raf
functions as a downstream effector of Ras, interpolated between the tyrosine
kinase receptor and the mitogen-activated protein kinase (MAPK) pathway and
acting in parallel to the Akt pathway. We have found significant over-expression
of B-Raf mRNA in pituitary adenomas, specifically NFPAs and a positive
correlation between mRNA and protein expression. B-Raf overexpression could
lead to increased activation of the MAPK pathway. Using microarray we have
found that the Bcl-associated athanogene (BAG1) mRNA is overexpressed in
somatotroph adenomas and NFPAs; this oncogene binds to and activates Raf-1,
which can potentiate B-Raf activity by heterodimerisation. In a pituitary protein
array we have identified several over- and underexpressed proteins and one of the
prominent differentially expressed proteins with potential importance in
tumorigenesis was the heat shock protein 110 (HSP110). This showed significant
overexpression in NFPAs and prolactinomas. Interestingly, another molecular
chaperone, the aryl hydrocarbon receptor interactive protein (AIP) has been
recently identified as a cause for pituitary adenomas in families with isolated
pituitary tumours. We have identified 5 different mutations in 19 familial
acromegalic families causing autosomal dominant disease with incomplete
penetrance. We have also observed prominent differences in AIP mRNA and
protein expression between normal pituitary cells and sporadic pituitary tumours.
Previous data suggest that AIP acts as a tumour suppressor gene but the exact
mechanism leading to pituitary tumorigenesis when AIP is lacking remains to be
Oncogene gsp and Gsa overexpression in pituitary cell biology
Anne Barlier2, Corinne Gérard1 & Enjalbert Alain1
Laboratory ICNE UMR6544 CNRS Université de la Méditérranée,
Marseille, France; 2Laboratory of Biochemistry anf Molecular Biology,
CHU Conception, Marseille, France.
Somatic mutations of the as subunit of G proteins were initially reported by
Landis and collaborators in 1989 in somatotroph tumors characterized by
markedly high cAMP levels. These mutations are localized at two critical sites
concerning the intrinsic guanosine triphosphatase activity of the protein leading to
a constitutive activation of the adenylyl cyclase. The mutated protein has been
named the gsp oncogene. On the other hand, Gsa mRNA level varied among
human somatotroph adenomas, the highest expression being observed in gsptumors (not bearing the active Gsa mutant). We previously showed that gsp
oncogene impacted tumoral phenotype, gspC tumors being smaller and more
sensitive to octreotide treatment. We have recently showed that high Gsa
expression impacted also tumoral phenotype of gsp- tumors.
Gsa is coded from GNAS gene which is imprinted in a tissue-specific manner.
Gsa is paternally silenced in normal pituitary, but a Gsa imprinting relaxation is
found in some tumoral tissue. Unexpectedly, we found that the loss of Gsa
imprinting did not induce the expected Gsa overexpression and was not
associated with a modification of methylation status of exon1A DMR
(a differentially methylated region controling the Gsa imprinting) in human
pituitary tumors.
To explore the impact on transduction pathways of mutated or overexpressed
Gsa protein, we obtained somatolactotroph GH4C1 cell lines by performing
doxycycline-dependent conditional overexpression of the wild type Gsa protein
and expression of the gsp oncogene. Although the resulting adenylyl cyclase and
cAMP levels were ten-fold lower in the wild type Gsa overexpressing cell line, a
sustained MAPKinase ERK1/2 activation was observed in both cell lines.
Overexpression of the wild type Gsa protein as the gsp oncogene initiated chronic
activation of endogenous PRL synthesis and secretion, as well as chronic
activation of ERK1/2-sensitive human PRL and GH promoters.
It is widely accepted that, in addition to serving as a repository for energy
reserves, adipose tissue is an active endocrine organ that secretes a variety of
signalling molecules, the adipokines, which play important roles in the
regulation of metabolism, energy balance, feeding behaviour, vascular
homeostasis and immunity. In particular, leptin, resistin and adiponectin
have been implicated in energy and glucose homeostasis. Additional
neuroendocrine functions have also been recognized for leptin as it regulates
the secretion of pituitary GH and LH. In order to elucidate whether
adiponectin, as leptin, may be involved in the regulation of pituitary cell
function, we investigated the effect of this adipokine on somatotrophs and
gonadotrophs and analyzed its interaction with major stimulatory regulators of
these cells (ghrelin, GHRH, GnRH), as well as with their corresponding
receptors (GHS-R, GHRH-R, and GnRH-R, respectively). Results show that
adiponectin inhibits GH and LH secretion as well as both ghrelin-induced GH
release and GnRH-stimulated LH secretion in rat pituitary cell cultures,
wherein the adipokine also increases GHRH-R and GHS-R mRNA content
while decreasing that of GnRH-R. Additionally, we have demonstrated that
the pituitary expresses both adiponectin and the adiponectin receptors,
AdipoR1 and AdipoR2, under the regulation of the adipokine. Taken
together, these data indicate that adiponectin, either locally produced or
from other sources, may play a neuroendocrine role in the control of both
somatotrophs and gonadotrophs. These results will be further discussed on the
context of adiponectin expression in pituitary tumoral cells and its interaction
with other adipokines present in the pituitary.
Financial-support: CVI-139-J.Andalucia, BFU2004-03883-MEC/FEDER,
and CIBER Obesity&Nutrition-ISCIII. Spain.
Thyroid – S20
Updated guidelines for the follow-up of thyroid cancer.
Martin Schlumberger
Institut Gustave Roussy, 94805b Villejuif, France.
Follow-up of thyroid cancer patients is aimed at controlling the adequacy of
thyroid hormone treatment and at the early diagnosis of recurrent disease.
Long term thyroxine treatment is given at suppressive doses only in the few
patients with persistent or recurrent disease. When cure has been assessed, serum
TSH should be maintained in the normal range (around 1 mU/ml).
The absence of disease is first controlled by the total body scan (TBS)
performed 3 to 5 days after the post-operative administration of radioiodine.
When the TBS is informative and does not show any focus of uptake outside the
thyroid bed, a subsequent routine diagnostic TBS is usually not necessary.
Cure is assessed at 9–12 months with a neck ultrasonography and a serum Tg
determination obtained 3 days after rhTSH stimulation (0.9 mg im, on 2
consecutive days). The quality of life of thyroid cancer patients is improved with
the use of recombinant human TSH (rhTSH) that avoids hypothyroidism,
provides an effective stimulation of any thyroid tissue and does not increase the
global cost of follow-up.
Low risk patients with a normal neck US and an undetectable rhTSH
stimulated serum Tg are considered cured. This reliable assessment of cure
permits reassurance of patients, the subsequent use of replacement doses of
thyroxine and the simplicity of the subsequent yearly follow-up with serum
TSH and Tg determinations. There is a close relationship between basal and
TSH-stimulated serum Tg levels, and the benefits of TSH stimulation may
decrease with Tg methods with an improved functional sensitivity. At the
present time, there is however no firm evidence that TSH-stimulated Tg
determination can be obviated.
When serum Tg is detectable at a low level following TSH stimulation,
another TSH stimulation should be performed 1 or 2 years later, and the trend
will indicate either irradiated thyroid cells (with decreasing Tg level) or
neoplastic cells (with an increasing Tg level).
Endocrine Abstracts (2007) Vol 14
9th European Congress of Endocrinology, Budapest, Hungary, 2007
Congenital hypothyroidism with gland in situ
Luca Persani
Dept of Medical Sciences, University of Milan and IRCCS Ist Auxologico
Italiano, Milan, Italy.
Congenital hypothyroidism (CH) is the most frequent endocrine congenital defect
affecting about 1:3000 newborns. In economically/ socially advanced counties,
CH is routinely screened by means of TSH (and/or T4) measurement on dry blood
spot (dbs) since more than 20 years. Neonatal screening allows early recognition
and treatment of affected newborns. Upon data collected in years !2000 by the
Italian CH Registry, the newborns with confirmed CH and gland-in-situ
constituted about 20% of total CH cases. However, in more recent years the
technical improvements in TSH determination in the Center for Neonatal
Screening of Milan region have lead to a progressive lowering of dbs TSH cutoff
value for newborn recall down to 10 mU/l. This has resulted in a significant
increase of the recall rate for CH (CH incidence 2003: 80/91,948 newborns), with
gland-in-situ cases nowadays accounting for more than 55% of total CH cases.
This phenomenon has several important implications concerning the correct
diagnosis and adequate management of these babies. One of the most important
questions raised by this new picture concerns the necessity to treat babies with
mild TSH elevations. The possibility to give correct answers to these questions is
complicated by the extreme heterogeneity of this CH category, highlighted by the
variable thyroid phenotype as well as by the multiple possibilities of association
with non-thyroid malformations/disorders. Relevant advancements have been
done in recent years with the discovery of new genetic causes and the description
of their underlying molecular mechanisms and related phenotypic presentation.
Nevertheless, the cause of several gland-in-situ CH cases remains still unsolved
justifying further efforts in this research field. These efforts will contribute to
reach a more complete pathogenic classification of CH with gland-in-situ which
represents one of the major steps toward an improved and evidence-based clinical
management of CH patients.
Thyroid and ageing
Istvan Szabolcs
Semmelweis University, Budaoest, Hungary.
In the healthy elderly there seems to be an age dependent decrease of TSH and FT3
but not FT4. The prevalence of TPOAb positivity increases with age but surprisingly
it has been found to be decreased in centenarians. Antibody positivity is not
predictive for future thyroid dysfunction in old age. The upper range of normal TSH
for the healthy elderly living in sufficient iodine intake areas is higher than in case of
iodine deficiency. In iodine deficient areas there is a high prevalence of nodular goiter
and hyperthyroidism is mainly caused by toxic nodules. Radioiodine should be
prefered for therapy of Graves’ disease in old age, long term thyrostatic therapy is not
safe. TAO is more severe in old age and there is a less favourable outcome of the
therapeutical options. In an elderly subject subclinical hyperthyroidism with
suppressed TSH is a risk factor for progression to overt disease, for atrial fibrillation,
osteoporosis and may be associated with increased cardiovascular and all-cause
mortality, thus we believe that it should be treated. The clinical significance of
subnormal but measurable TSH is less clear, but in old age treatment may be
considered in case of heart disease or osteoporosis. Subclinical hypothyroidism is a
risk factor for atherosclerosis but slightly elevated TSH in old age should not be
treated: it may even be favourable to have a longer life. In any case, TSH levels
outside the reference intervals should first be controlled before considering
treatment. The cancer risk in cold thyroid nodules increases with advanced age.
According to most but not all studies, in older differentiated thyroid cancer-patients
poor prognostic features are more frequent, total thyroidectomy and radioablation are
recommended and additional treatment of progressive disease should not be denied
because of advanced age.
Thyroid autoimmunity: genes and environment
Pia Skov Hansen
Odense University Hospital, Odense, Denmark; 2University of Southern
Denmark, Odense, Denmark.
Autoimmune thyroid diseases (AITD) comprise two clinical phenotypes, Graves’
disease and Hashimoto’s thyroiditis. These conditions share distinct
Endocrine Abstracts (2007) Vol 14
immunological features such as autoreactivity against the key thyroid
autoantigens thyroglobulin and thyroid peroxidase. Considering Graves’ disease
as well as Hashimoto’s thyroiditis, twin studies have revealed a higher
concordance rate among monozygotic (MZ) as compared to dizygotic (DZ)
twins, suggesting a relative strong genetic influence in the aetiology. According to
the endophenotypic approach, it might be useful to subdivide a clinical phenotype
into a set of variables thought to represent more basic processes. The presence of
thyroid autoantibodies in euthyroid individuals can be regarded as a central
phenotypic anchor point and, using the twin design, the relative contributions of
genetic as well as environmental effects in the aetiology of AITD, at this early
stage of the disease process, has been clarified as well.
The genetic contribution to autoimmune disease (AID) has been intensely
investigated, and a slow progress towards identification of AITD susceptibility
genes is seen. There is evidence of association and, in some cases, even linkage
between AITD and several genetic loci. However, one problem is often the very
pronounced discrepancy between the initial and subsequent reports. On the other
hand, epidemiological studies aim at identifying specific measurable environmental exposures of importance for the development of AITD. So far only a few
environmental factors (e.g. iodine intake and smoking habits), with a clear
detectable effect on the disease, have been characterized. The underlying
challenges in trying to understand a complex phenotype, such as AITD, will be
Pheromones, odorant and taste receptors – S21
Odorant receptors and reproduction
Hanns Hatt
Ruhr-University Bochum, Bochum, Germany.
Fertilization is still one of the nature’s best-kept secrets. Despite a century of
research we still lack a comprehensive understanding how mammalian sperm
cells navigate inside the female body, locate, and finally fertilize the egg. More
than a decade ago, the unexpected finding of olfactory receptor expression in
human testicular tissue led to speculation about a potential role of these
chemoreceptors in various aspects of mature sperm behavior, especially sperm
chemotaxis. We could obtain first evidence in favor of this hypothesis by the
identification of hOR17-4, a testicular olfactory receptor that mediates human
sperm chemotaxis. We showed that in vitro activation of the receptor hOR17-4 by
a variety of floral odorants (e.g. bourgeonal, cyclamal) mediates both chemotaxis
and chemokinesis in human sperm cells. A detailed characterization of the
receptor’s molecular receptive range as well as the first description of a potent
receptor antagonist could provide the basis for future applications in fertility
treatment with important consequences in contraception. Very recently we
reported cloning, recombinant expression and functional characterization of
another human testicular olfactory receptor (hOR17-2). Using a combination of
imaging behavioral assays, we showed activation of sperm by cognate receptor
ligands and described a specific receptor-mediated motility pattern. Comparative
analysis of different OR-induced signaling pathways as well as cell-specific
receptor expression profiles are subject of current research. Given an estimated
number of up to 40 different testiculary expressed odorant receptors, an
identification of the stimulatory ligands of further members of this “unconventional” group of ORs is critical to gain new insight in their role in reproduction.
Molecular architecture of pheromone sensing in mammals
Catherine Dulac
HHMI, Cambridge, MA, United States, Harvard University, Cambridge,
MA, United States.
The neuronal processing of pheromone signals within distinctive brain structures
leads to marked changes in animal behaviour and endocrine status. The highly
reproducible and species-specific character of the response to pheromones offers a
unique opportunity to uncover the neural basis of genetically pre-programmed
behaviours. Molecular and genetic investigation of the mechanisms underlying
pheromone pheromone-evoked responses in the mouse nose and brain have
revealed a neural strategy that is strikingly different from that used in other
chemosensory modalities such as taste and olfaction. Our studies have provided
novel insights into the sensory coding of pheromone signals leading to gender
identification and aggressive behaviour, and into the developmental mechanisms
leading to the emergence of distinct olfactory pathways. Our most recent
9th European Congress of Endocrinology, Budapest, Hungary, 2007
experiments using conditional and GFP-expressing viral vectors are aimed at
visualizing entire brain circuits responsible for innate behaviours.
together, our data strongly suggest that genetics and peripheral taste receptor
mechanisms govern gustatory perception and perceptual variability in the
population with a probable impact on nutrition and health.
Endocrine and behavioural responses to pheromones
Peter Brennan
University of Bristol, Bristol, United Kingdom.
According to the original definition, pheromones are substances released by an
individual that have definite behavioural or physiological effects on another
individual of the same species. For example, male mouse urine contains a
complex mixture of chemosignals, some of which, such as brevicomin and
thiazole are testosterone-dependent and signal the presence of a reproductively
active male. These have powerful effects as releaser pheromones to elicit
aggression from other males, as well as having effects as primer pheromones on
female reproductive state, such as puberty acceleration and induction of oestrus.
However, as the complexities of vertebrate chemosensory communication have
become evident, the original definition of pheromones has begun to appear too
restrictive. For instance, peptide chemosignals related to the major histocompatibility complex convey information about individual identity, which as
signaller pheromones can influence behaviour or physiology without eliciting a
definite response.
In addition to mediating individual recognition in social contexts, these
individuality chemosignals enable female mice to recognise the urinary
pheromones of their mate, to which they are exposed at mating. This
chemosensory memory is vital for their reproductive success, as it prevents the
pre-implantation pregnancy failure that is induced by exposure to urinary
pheromones from an unfamiliar male. This pregnancy block effect (Bruce effect)
is mediated by the vomeronasal system, via the dopaminergic suppression of
prolactin production by the pituitary. A range of evidence suggests that memory
formation to the mating male’s pheromones involves synaptic changes in the
accessory olfactory bulb at the first stage of the vomeronasal pathway. This results
in a selective inhibition of the mate’s pheromonal signal, preventing it from
activating neural circuits in the corticomedial amygdala and hypothalamus that
mediate the endocrine changes responsible for pregnancy block. This is just one
example of the way that learning can reinforce or inhibit innate pheromonal
Bone – S22
Bisphosphonates: molecular mode of action and adverse effects
Michael J Rogers
University of Aberdeen, Aberdeen, United Kingdom.
Bisphosphonates are the mainstay of treatment for metabolic bone diseases such
as post-menopausal osteoporosis and Paget’s disease. Enormous progress has
been made over the last few years in understanding how these drugs act at the
molecular level. After targeting bone and selective internalisation by osteoclasts,
simple bisphosphonates are incorporated into cytotoxic, non-hydrolysable
analogues of ATP. By contrast, the more potent nitrogen-containing bisphosphonates inhibit FPP synthase (an enzyme of the mevalonate pathway), which
disrupts the synthesis of the isoprenoid lipids FPP and GGPP. These lipids are
required for the carboxy-terminal modification (prenylation) of small GTPbinding proteins such as Ras, Rho, Rac and Rabs. Prenylated small GTPases act as
molecular switches, regulating processes fundamental to osteoclast function,
including membrane ruffling, vesicular trafficking, cytoskeletal organisation and
cell survival. Inhibition of FPP synthase by bisphosphonates prevents the
prenylation of small GTPases and causes the accumulation of the unprenylated
(and, in some cases, inappropriately activated) forms of the proteins, thus
disrupting osteoclast function and causing osteoclast apoptosis.
The most common adverse effect of intravenous bisphosphonate therapy is a
brief, ‘flu-like acute-phase reaction. We have recently demonstrated that this
effect appears to be due to inhibition of FPP synthase in peripheral blood
mononuclear cells, which causes an accumulation of the upstream isoprenoid
lipid IPP. The latter is known to stimulate the Vgamma9Vdelta2 subset of
gamma,delta-T cells, causing the release of TNFalpha and IFNgamma and hence
the rapid onset of ‘flu-like symptoms. Esophageal irritation by oral bisphosphonates may also be caused by inhibition of FPP synthase in GI epithelial cells,
however the exact cause of recently-described, rare cases of osteonecrosis of the
jaw remains unclear.
Thus, the ability of nitrogen-containing bisphosphonates to inhibit the
mevalonate pathway explains their well-known, potent inhibitory effects on
bone-destroying osteoclasts as well some of their adverse effects.
Bitter taste receptors and food intake
Wolfgang Meyerhof, Maik Behrens, Bernd Bufe, Anne Brockhoff,
Susann Förster, Claudia Reichling, Christina Kuhn & Marcel Winnig
German Institute of Human Nutrition, Potsdam-Rehbruecke, Germany.
Taste is an overriding determinant of food choice and leads to the development of
preferences impacting on nutrition and eventually health. To investigate the
molecular basis of gustation and its link to nutritional behaviour, we isolated all
25 members of the human bitter taste receptor gene family, TAS2Rs, and
established their expression profile on the tongue. Using functional assays we
identified the cognate bitter compounds for whalf of the encoded receptors. Our
data suggest that TAS2Rs appear to be broadly tuned to detect compounds with
common structural motifs, explaining how humans are capable of perceiving
thousands of bitter substances with a small set of receptors. This broad tuning is
likely caused by the presence of multiple binding sites for various bitter
compounds on the TAS2Rs. Our experiments also revealed that the biochemical
properties of the receptors define perceptual sensitivity of individuals. Moreover,
frequently occurring polymorphisms in TAS2R genes determine numerous
receptor variants, which can differ in the sensitivities for their cognate bitter
compounds up to 1000 fold, thereby generating perceptual variability in the
population. How far receptor mechanisms determine tasting is shown for
saccharin, a compound that taste sweet through activation of the sweet taste
receptor at low and moderate concentration, with an off-taste caused by its ability
to activate two TAS2R bitter taste receptors simultaneously and to block the
sweet taste receptor at higher concentrations.
To date direct evidence is still missing that convincingly proves or disproves the
impact of gustation on intake behaviour. However, strong circumstantial evidence
comes from the phylogenetic analysis of human TAS2R genes and from the
analysis of TAS2R polymorphisms and taster phenotypes that evolved
independently in chimanzees and humans as well as from an association study
identifying a TAS2R16 allele as a risk factor of alcohol dependence. Taken
Calcimimetics in the management of hyperparathyroidism
Munro Peacock
Indiana Universtity, Indianapolis, United States.
The cell surface calcium receptor (CaR) in the parathyroid gland plays a central
role in the regulation of serum calcium homeostasis. Activation and inactivation
mutations in the CaR lead to chronic hypocalcemia and hypercalcemia states
(Brown, EM. Mutations in the calcium-sensing receptor and their clinical
implications. Horm Res 1997 48 199–208). Type 11 calcimimetics are a novel
class of compounds that directly reduce PTH secretion from the parathyroid cell
by binding to the CaR and increasing its sensitivity to extracellular ionized
calcium, thus causing a left-shift in the Ca-PTH setpoint (Nemeth, EF et al.
Calcimimetics with potent and selective activity on the parathyroid calcium
receptor. PNAS USA 1998 95 4040–4045). Cinacalcet is an oral calcimimetic that
has been shown to reduce serum PTH and calcium in secondary hyperparathyroidism of renal failure (Block, GA et al. Cinacalcet for secondary hyperparathyroidism in patients receiving hemodialysis. N Engl J Med 2004 350
1516–1525), in primary hyperparathyroidism (Peacock et al. Cinacalcet
Hydrochloride maintains long-term normocalcemia in patients with hyperparathyroidism. J Clin Endocrinol 2005), and in parathyroid cancer (Silverberg, SJ
et al. Cinacalcet reduces hypercalcemia in patients with parathyroid carcinoma.
J Bone Min Res 2006 21 Suppl. 1 S440).
Cinacalcet therapy is well tolerated long-term, and current studies indicate that
it may play a valuable role in the medical management of diseases of
Endocrine Abstracts (2007) Vol 14
9th European Congress of Endocrinology, Budapest, Hungary, 2007
Primary hyperparathyroidism: surgical approach and benefits
Svatopluk Adamek
3rd Dpt of Surgery, First Fac of Medicine, Charles University, Prague, and
Teaching Hospital Motol, Czech Republic, Prague, Czech Republic.
Surgical therapy of the primary hyperparathyroidism (PHP) offers a definite and
curative treatment. The cooperation with an experienced endocrinologist is
necessary, because the confidence that the patient has a PHP, is the primary
presumption for the proper surgical therapy of the PHP. The result of a
parathyroidectomy depends mainly on preoperative localization of hyperfunctional
tissue and the experience of the surgeon. The parathyroidectomy remains curative
approach in 97% of patients if provided by an experienced surgeon. The neck
ultrasonography and MIBI scintigraphy of parathyroid glands remain the gold
standards in preoperative imaging. The surgeon must but be able to perform a
parathyroidectomy in case where preoperative localizing methods are not successful.
In addition, we require an indication to surgical approach in patient with concomitant
thyreopathy. The basic technique of a parathyroidectomy is the bilateral exploration
of the neck with the examination of all locations of the parathyroid glands, including
ectopic ones, usually from the collar skin incision above the jugulum.
In terms of a minimalization of surgical approach, unilateral, radionavigated and
miniinvasive approaches were developed. In case of intrathoracic-mediastinal
localization of parathyroid glands, the partial median sternotomy is the basic
approach. In 3.5% of 680 our patients, the neck approach was not sufficient. The
complications of parathyroidectomy are not common. They include the hypoparathyroidism and the recurrent laryngeal nerve injury with following vocal cord
paralysis. Benefits To date, the parathyroidectomy is a short, one-day surgery
operation in surgical centers. The improvement of surgical technique offers a surgical
treatment to ”asymptomatic“ patients. In case of a clear localization of parathyroid
adenoma by sonography or MIBI scintigraphy, the operation is short, safe and does
not stress the patient. In these patients, the so-called small symptoms (fatigue,
musculoskeletal pain, weakness, dyspepsia, polydypsia, constipation, polyuria,
pruritus, depression) are ameliorated.
Supported by IGA MZ ČR č. 8308-5/2005
Absolute risk prediction for fracture
H Pols
was reduced as was expression of proteins involved in formation of junctional
complexes. Leydig cell function was altered even though expression of Ar was
maintained in these cells confirming the existence of paracrine interactions
between the seminiferous and interstitial compartments. In conclusion, testicular
function and male fertility are androgen dependent; expression of AR in Sertoli
cells is essential for normal germ cell maturation and fertility.
The experimental mouse model for men with Klinefelter syndrome
YanHe Lue, Christina Wang, David Jentsch, Krista Erkkila, Peter Liu,
Monica Schwarcz & Ronald Swerdloff
Dept of Medicine, Division of Endocrinology, LABiomed at Harbor-UCLA
Med Ctr, Torrance, CA, USA.
Klinefelter syndrome (XXY males) is the most common sex chromosome
aneuploidy, occurring in about 1 per 500 men. To study the underlying molecular
mechanisms caused by the extra X chromosome, we have developed an experimental
mouse model for men with Klinefelter’s syndrome. We have demonstrated that adult
XXY mice have absence of germ cells, decreased serum testosterone levels, and
elevated gonadotropin levels. Testicular failure begins early as a result of massive
germ cell loss that precedes the initiation of meiosis. Loss of germ cells is mediated
through apoptosis. Gene microarray with testicular RNA samples from 1-day-old
mice showed inactive X specific transcripts (Xist) expression increased 4.14-fold,
indicating the extra X chromosome is inactivated in XXY testes. Proapoptotic Bcl2interacting killer-like and caspase 7 have 1.59- and 1.68-fold increase, and
antiapoptotic transcripts IAP and Bcl2-like-10 have 3.73- and 2.08-fold decrease
respectively in XXY mice. By immunohistochemistry, we found c-kit expression in
gonocytes occurred earlier in XXY than XY siblings, suggesting early differentiation
of gonocytes may contribute to germ cell loss in XXY mice. In addition to germ cell
defect, androgen receptor expression in Sertoli cells is nearly depleted in adult XXY
mice, suggestive of Sertoli cell dysfunction. By transplantation of XY germ cells into
adult XXY testes, we found a few donor XY spermatogonia were able to survive for
10 weeks without further differentiation. Leydig cells in adult XXY mouse testes are
both hypertrophic and hyperplastic. Testosterone production from XXY Leydig cells
is impaired. Besides reproductive dysfunction, we have demonstrated that XXY
mice have impaired learning, memory, and social interaction. By giving testosterone
implants to adult XXY mice, we demonstrated that testosterone treatment
significantly improves the learning ability of adult XXY mice.
Abstract unavailable
Reproductive endocrinology/andrology – S23
Androgen regulation of spermatogenesis
Philippa Saunders1, Lee Smtih1, Robert Hooley1, Karel De Gendt2,
Evi Denolet2, Guido Verhoeven2 & Richard Sharpe1
MRC Human Reproductive Sciences Unit, Edinburgh, United Kingdom;
Catholic University of Leuven, Leuven, Belgium.
Spermatogenesis is a complex process involving interactions between the somatic
cells (Sertoli, Leydig, peritubular) and germ cells within the adult testis.
Androgens are key regulators of spermatogenesis and intra-testicular concentrations of testosterone (T), produced by the Leydig cells, are higher than that in
blood. Androgen action is mediated by the androgen receptor (AR), an
X-chromosome-encoded, ligand-activated, transcription factor. The mechanisms
by which androgens regulate testis function have been explored by determining
the pattern of expression of AR, by manipulating androgen concentrations, by
performing studies in vitro on isolated tubules/cells and most recently by studying
mice with cell-specific deletion of the Ar gene.
In adult testes AR have been immunolocalised to the nuclei of Sertoli, Leydig
and peritubular myoid cells as well as the cells lining blood vessels. Expression in
adult Sertoli cells is stage-dependent and in vitro studies have demonstrated that it
is T-regulated. In rats, ablation of Leydig cells with ethane dimethane sulphonate
results in an acute reduction in intra-testicular T and germ cell loss; germ cell
demise is first observed in the stages of spermatogenesis in which AR expression
in Sc is highest. The impact of Sertoli cell-specific ablation of Ar on testicular
function has been investigated in three independent laboratories. In all cases Ar
ablation resulted in a reduction in testicular size, germ cell loss and infertility.
Expression of rHox5, a Sertoli cell protein previously shown to be T-regulated,
Endocrine Abstracts (2007) Vol 14
Genes involved in male infertility: sorting facts from fiction
Ewa Rajpert-De Meyts
Copenhagen University Hospital (Rigshospitalet), Copenhagen, Denmark.
Male infertility is a common disorder and a growing health problem. A large
proportion of unexplained cases have been summarily categorised as idiopathic
infertility. The majority of idiopathic cases, especially those with severely
impaired spermatogenesis incl. azoospermia, are presumably caused by genetic
defects. Genetics of male infertility has been a largely unexplored area, until quite
recently, when new molecular tools unabled discovery of a growing number of
genes involved in spermatogenesis and gamete maturation, e.g. genes mapped to
the AZF region of the Y-chromosome and some genes on the X-chromosome. In
addition, several pathways related to hormonal regulation of reproductive
function contain polymorphic genes, which may affect the function of a given
gene in a discrete manner, such as the CAG and GGN repeats on androgen
receptor, or polymorphisms in CYP, INSL3 genes. Finally, polymorphisms of
genes seemingly unrelated to the reproductive function, have been associated with
male infertility, e.g. mitochondrial gene polymerase, POLG. A rush to analyse
polymorphic genes in various populations, often with poorly characterised cases
and controls, created a lot of confusion in the literature as to the real
pathogenetical involvement of the studied genes in male infertility. There is a
need for large and well-controlled studies, underpinned by basic functional
studies of the investigated genes. A great care must be taken to use proper control
groups, which must be selected with fertility, ethnicity, and age of the subjects in
mind. A very important point is having in mind that environmental exposures
and/or lifestyle factors frequently exert their influence primarily in genetically
predisposed individuals. A good description of the reproductive parameters
(outcomes), preferably with the analysis of the reproductive function on children,
is also essential for the analysis of the consequences of studied polymorphism/
gene aberration, and for an early prognosis as to the future fertility problems.
9th European Congress of Endocrinology, Budapest, Hungary, 2007
Genetic basis of testicular tumors
Leendert Looijenga
Erasmus MC, Rotterdam, Netherlands.
Various types of human germ cell tumors (GCTs) can be found, referred to as
type I, II and III. The type I are the teratomas and yolk sac tumors of
neonates and infants. No genomic aberrations have been identified in
teratomas, while yolk sac tumors show chromosomal imbalances related to
chromosomes 1, 6 and 20. Type II GCTs are the seminomas and
nonseminomas, derived from carcinoma in situ (CIS)/intratubular germ cell
neoplasia unclassified (ITGCNU). CIS/ITGCNU and seminoma cells mimic
primordial germ cells/gonocytes, amongst others characterized by expression
of the diagnostic marker OCT3/4-POU5F1. All invasive tumors show gain of
the short arm of chromosome 12. The type III GCTs, i.e. spermatocytic
seminomas, occur predominantly in elderly, and only in the testis. They
originate from primary spermatocytes, and show consistent gain of
chromosome 9, of which DMRT1 is a candidate. GCTs show specific
patterns of mRNA and microRNA expression, of possible diagnostic and
prognostic value. Besides familial predisposition and infertility, disorders of
sex differentiation (DSD) is a risk factor for type II GCTs. This specifically
forms of hypovirilization and gonadal dysgenesis, in the presence of part of
the GBY region. Besides CIS/ITGCNU, gonadoblastoma can be the precursor
in DSD patients. Gonadoblastoma is the earliest developmental stage in the
genesis of GCTs. TSPY (testis specific protein on the Y chromosome) is a
likely candidate to explain the requirement of the GBY region for malignant
transformation of germ cells. A significant limiting diagnostic factor in DSD
is lack of specific markers for CIS/ITGCNU in case of maturation delay of
germ cells. The type II GCTs are in fact an embryonic cancer in adult
patients. This explains a number of specific characteristics, like their histology
(totipotency), overall sensitivity to DNA-damaging agents, as well as their
chromosomal and genetic constitution.
Obesity – S24
Altering adipocyte metabolism as a way to counteract obesity and
insulin Resistance
Sven Enerbäck
Medical Genetics, Dept of Medical Biochemistry, Göteborg University,
Medicinareg, 9A, Box 440, SE 405 30 Göteborg, Sweden.
Advances over the last two decades in our understanding of the adipocyte have
clarified its role as a key regulator of both energy balance and intermediary
metabolism. It is now known that in addition to being an insulator and energy
depot, the adipocyte is a highly active cell, secreting a wealth of factors,
including leptin, that play a part in CNS and appetite regulation. There is also a
much greater understanding of how fat cells themselves develop from precursor
cells FOXC2, pRb, PGC-1and RIP140 has been discussed as genes influencing
adipocyte cell fate. By increasing the already existing pool of brown adipocyte
in human adipose tissue, as a way to dissipate excess energy through
uncoupling, this would help conserve ample triglyceridestorage capacity in
white adipocyte and hence counteract ectopic lipid depositions in tissues like
liver and muscles. Since ectopic lipid deposition is intimately connected to the
development of insulin resistance and the metabolic syndrome, factors affecting
white versus brown fat partitioning constitutes an interesting approach to this
health problem.
Triglyceride-lowering effect of metabolic switch in white adipose tissue
Jan Kopecky
Institute of Physiology, Academy of Sciences of the Czech Republic,
Prague, Czech Republic.
High level of triglycerides (TG) in plasma is a risk factor for cardiovascular
disease. Various treatment strategies aimed at decreasing plasma TG concentrations affect synthesis of lipoproteins in the liver and/or increase clearance of
TG by peripheral tissues. Lipid-lowering effects of fibrates reflects modulation of
the liver metabolism. Antidiabetic agents thiazolidinediones (TZD) lower plasma
TG by enhancing lipoprotein lipase activity in white adipose tissue (WAT). Longchain polyunsaturated fatty acids of n-3 series, namely eicosapentaenoic (EPA;
20:5 n-3) and docosahexaenoic (DHA; 22:6 n-3) acids, that are abundant in sea
fish, act as hypolipidemics, while decreasing the production of lipoproteins. EPA
and DHA may also affect the TG clearance. Most of the above mentioned
treatments induce expression of mitochondrial uncoupling proteins (UCPs) in
WAT. The aims of our studies were to characterize: (i) the potency of WAT to
decrease plasma TG levels; and (ii) the involvement of WAT in the hypolipidemic
effects of EPA and DHA. A large potency of WAT to decrease plasma TG was
demonstrated using transgenic mice with ectopic expression of UCP1 in WAT
(aP2-Ucp1 mice). The ectopic UCP1 induces respiratory uncoupling in WAT,
hence stimulating in situ lipid oxidation and mitochondrial biogenesis, and
clearance of plasma TG. Moreover, aP2-Ucp1 mice were resistant to high-fat diet
induced obesity and showed higher whole body lipid oxidation. The obesity in
wild type mice was also prevented by replacing only 9% of the dietary lipids by
EPA and DHA. This dietary treatment lowered plasma TG, while inducing lipid
oxidation and mitochondrial biogenesis in WAT. These results supported a
possibility to induce a metabolic switch in WAT, which may change whole body
phenotype, including the lowering of plasma TG. Further studies are required to
assess the importance of this switch for the effectiveness of the lipid-lowering
Adipokines and insulin sensitivity in humans
José Manuel Fernández-Real
Hospital of Girona, Girona, Spain.
Decreased insulin action has been proposed as the common factor that is in the
background of the different components of the metabolic syndrome. Insulin
resistance is also associated with a chronic activation of the innate immune
system. The innate immune system constitutes the first line of body’s defence and
it is constituted by different barriers (epithelia, adipose tissue), and different blood
and tissue components as macrophages, and neutrophils. Once activated, the acute
phase response is activated, with generation of different acute phase proteins and
cytokines that are produced in order to struggle against different aggresions, as
infections and traumatisms. The aim of this response is to eradicate these agents,
to repair the harmed tissues, and, through increased insulin resistance, to optimize
the energetic substrates, which will be drained to vital tissues and organs (i.e.
brain and the immune system). Evolution pressures have led to survival of the
fittest individuals, those with genetics that allows the best defence against
infection and periods of famine. The initial evolutive advantages of increased
inflammatory responses, hypersecretion of proinflammatory cytokines (TNF-a,
interleukin 6, interleukin 18), counterbalanced by antiinflammatory molecules
(adiponectin, sCD14, BPI, MBL), turn into chronic inflammation conditions, such
as obesity and type 2 diabetes. Increasing evidence is reported according to which
chronic inflammation precedes these conditions. The knowledge of how these
metabolic pathways interact with the inflammatory cascade will facilitate new
therapeutic approaches.
Lipodistrophy and abdominal fat accumulation: new therapeutic
LF Van Gaal
Department of Diabetology, Metabolism and Clinical Nutrition, University
Hospital Antwerp, Antwerp, Belgium.
Lipodystrophy (LD) is a well-recognised clinical syndrome of peripheral fat
atrophy and central adiposity, often associated with laboratory abnormalities such
as dyslipidemia and glucose intolerance, and probably linked to insulin resistance.
The long-term consequences of LD and its potential association with
cardiovascular disease remain unknown. The visceral fat accumulation is
characterised by the increased, abundant secretion of a number of peptides
such as leptin, insulin-like growth factor (IGF), adiponectin and the recently
reported resistin and visfatin hormones. Elevated resistin and tumour necrosis
factor (TNF-alpha) levels and low levels of adiponectin secretion may have
implications for the risk of development of type 2 diabetes and cardiovascular
disease. LD is observed not only in rare autosomal syndromes, but also in patients
positive for the human immunodeficiency virus (HIV) who have been treated with
protease inhibitors. Both the origin of LD and its treatment deserve more attention
and further research in clinical settings.
Potential treatment options with leptin and human growth hormone can be
considered to reduce the burden and cardiovascular risk of lipodystrophy.
Endocrine Abstracts (2007) Vol 14
9th European Congress of Endocrinology, Budapest, Hungary, 2007
Novel hormones – S25
Hormones help you live longer - the threat of Klotho
M Kuro-o
The University of Texas Southwestern Medical Center, Dallas, Texas, USA.
A defect in klotho gene expression in mice leads to a syndrome resembling aging,
including a shortened life span, hypogonadism, growth arrest, hypoactivity, skin
atrophy, muscle atrophy, hearing loss, premature thymic involution, cognition
impairment, motor neuron degeneration, arteriosclerosis, osteopenia, soft tissue
calcification, and pulmonary emphysema among others. In contrast, overexpression of the klotho gene extends life span in the mouse. Thus, the klotho
gene functions as an aging suppressor gene. The klotho gene encodes a singlepass transmembrane protein and is expressed in limited tissues, notably in the
kidney and brain. The extracellular domain of Klotho is shed and secreted in the
blood, raising the possibility that Klotho protein itself may function as a humoral
Extended life span in transgenic mice that overexpress Klotho is associated
with increased resistance to insulin/IGF1 and oxidative stress, mechanisms for the
suppression of aging evolutionarily conserved from worms to mammals. Klotho
may affect aging processes partly through its ability to inhibit insulin/IGF1
signaling and to reduce oxidative stress.
Mice defective in fibroblast growth factor-23 (FGF23) exhibit aging-like
phenotypes similar to those observed in Klotho-deficient mice, suggesting that
Klotho and FGF23 may function in a common signal transduction pathway(s). My
laboratory has shown that Klotho binds to multiple FGF receptors (FGFRs) and
enhances the ability of FGF23 to activate FGF signaling. FGF23 was originally
identified as a hormone that inhibited phosphate reabsorption in the kidney. In
fact, both Klotho-deficient mice and FGF23-deficient mice exhibit elevated serum
phosphate levels. In addition, many aging-like phenotypes in these mice are
rescued by restriction of dietary phosphate or ablation of vitamin D activity.
These findings imply a novel concept that FGF signaling and phosphate
metabolism may participate in the regulation of aging in mammals.
which is discharged by bone resorption and is totally excreted urinary. A
further marker of collagen resorption is the c-terminal telopeptide of
collagen type I, which is liberated to blood circulation within the bone’s
degradation and undergoes renal elimination. The aim of our investigation
was to look after a correlation of these parameters in healthy subjects (nZ
28), patients with type 1 diabetes mellitus (DM) (nZ65), and female
patients with diagnosed postmenopausal osteoporosis (PMO). For the
labaratory analysis of DPD we used a solid phase chemiluminescence
enzymimmunoassay and for assessment of c-terminal telopeptide of type I –
collagen a quantitative ELISA was used. We found correlations of both
parameters within the main group (nZ181), and all the other subgroups.
The strongest correlation could be found in the group with DM type 1 (rZ
0.79, P!0.05) followed by the group of healthy subjects (rZ0.75, P!
0.05). In the group of female patients (PMO) a weaker, but significant
positive correlation could be verified (rZ0.58, P!0.05). The arithmatic
average of DPD was in the group of healthy subjects about 15,4 nM
DPD/mM Krea (95%KI: 11.1–19.72), in the group of type 1 DM patients
21.02 (11.23–30.82) and about 38.51 (28.32–48.7) nM DPD/mM Krea in the
group of the female patients (PMO). Both parameters reflect the diverse
amount of bone turnover and correlated significantly positive to each other.
In comparison to the healthy subjects an enhanced bone turnover could be
measured consistently in the group of type 1 DM patients. The hihgest
values but concurrent the widest statistic spread with weaker correlation was
measured in the group of female patients (PMO). This may indicate, that the
results found before therapy are of limited diagnostic value, unlike in the
course of antiresorptive therapy the observed significant alterations of bone
resorption parameters are of specific diagnostic value.
Hormonal regulation of iron homeostasis by hepcidin
Sophie Vaulont
Institut Cochin, Paris, France.
Phosphatonins and the regulation of renal phosphate transport
P Kumar
Abstract unavailable
Correlation of desoxypyridinolin and c– terminal telopeptide of
collagen type I within different patient collectives
Walter Fassbender, M Goedde, Vincent Brandenburg,
Klaus-Henning Usadel & Ulla Stumpf
Hospital z. Hl. Geist, Kempen, Germany; University Hospital, Frankfurt/
Main, Germany; University Hospital, Aachen, Germany;
Endokrinologikum, Frankfurt/Main, Germany; University Hospital,
Duesseldorf, Germany.
Bone metabolism can be measured indirectly with specific biochemical
markers. Desoxypyridinolin (DPD) is a derivate of hydroxypyridinium,
Endocrine Abstracts (2007) Vol 14
Hepcidin is a small circulating 25-amino-acid cysteine-rich peptide first identified
in human blood and urine. The hepcidin gene is expressed mainly in the
hepatocytes, secreted in the circulation and cleared by the kidney. In mammals,
convincing evidence indicates that hepcidin constitutes the master regulator of
iron homeostasis; the circulating peptide acts to limit gastrointestinal iron
absorption and serum iron by inhibiting dietary intestinal iron absorption and iron
recycling by the macrophages. To limit iron egress, hepcidin binds to ferroportin,
a transmembrane iron exporter, thereby inducing its internalization and
subsequent degradation, leading to decreased export of cellular iron.
As befits an iron-regulatory hormone, hepcidin synthesis is induced by iron
stores and inflammation and inhibited by anemia and hypoxia. The mechanisms
regulating hepcidin expression are only beginning to be understood. Recent
studies have highlighted two regulatory cascades: BMP/Smad signaling of
hemojuvelin (a transmembrane protein whose mutation is leading to juvenile
hemochromatosis) and IL-6/STAT3 signaling of inflammation.
Dysregulation of hepcidin is involved in the pathogenesis of a spectrum of iron
disorders. Most of the iron overload syndromes known to date (Hereditary
Hemochromatosis and secondary iron overloads) imply a reduction of hepcidin
secretion. In contrast, excessive cytokine-induced hepcidin expression causes
hypoferremia and contributes to the anemia of inflammation.
The emergence of hepcidin as the pathogenic factor in most systemic iron
disorders should provide important opportunities for improving their diagnosis
and treatment.
9th European Congress of Endocrinology, Budapest, Hungary, 2007
Oral Communications
Endocrine Abstracts (2007) Vol 14
9th European Congress of Endocrinology, Budapest, Hungary, 2007
Thyroid clinical - OC1
OC1.1 – ESE Young Investigator Award
Prevalence of inactivating TSH receptor (TSHR) mutations in a large
series of pediatric subjects with non-autoimmune mild hyper-thyrotropinemia (hyperTSH)
Daniela Cordella1, Alessandro De Marco2, Davide Calebiro1, Tiziana
de Filippis2, Giorgio Radetti3, Giovanna Weber5, Maria Cristina Vigone5,
Marco Cappa4, Alessandro Sartorio2, Marta Busnelli2, Marco Bonomi2,
Bice Chini6, Paolo Beck-Peccoz7 & Luca Persani1
Dept of Medical Sciences, University of Milan and Ist. Auxologico
Italiano, Milan, Italy; 2Lab of Experimental Endocrinology, IRCCS Ist
Auxologico Italiano, Milan, Italy; 3Pediatric Unit, Bolzano, Italy; 4Pediatric
Unit, Bambin Gesù Hosp, Rome, Italy; 5Pediatric Unit, HSR, Milan, Italy;
CNR, Milan, Italy; 7Endocrine Unit, Fondazione Policlinico IRCCS,
Milan, Italy.
Mild hypothyroidism is a heterogeneous and frequent disorder in the general
population that is due to autoimmune disease in most of the cases. TSH
resistance is considered a rare genetic disease due to germline loss-of-function
TSHR mutations. However, TSHR mutations have been mainly searched in
patients with large TSH elevations and their actual prevalence among patients
with mild TSH elevations (as those found in mild hypothyroidism) is so far
unknown. In this study, we evaluated the involvement of TSHR mutations in
a large pediatric series of unrelated cases of hyperTSH (nZ48, 26 W and 22
M; age 0–12 yrs) selected in various collaborating centers. All subjects had
high TSH (4–15 mU/ml), normal freeT4 concentrations, no antithyroid
antibodies and normal thyroid volume and structure at ultrasound. Through
dHPLC (WAVE apparatus, Transgenomic) and direct sequencing of abnormal
PCR products (ABI Prism), we analyzed TSHR coding sequence, proximal
promoter and intron-exon boundaries. These investigations lead to the
disclosure of 11 carriers of heterozygous TSHR mutations among the 48
patients with hyperTSH (frequency: 22.9%). Seven of these 11 carriers had at
least another first-degree relative with known hyperTSH and 4/11 were
positive at neonatal TSH screening. Three TSHR mutations are novel (P162L,
T607I, R609Q), never found in other patients with TSH resistance and in 150
internal control alleles, and 4 mutations had been previously reported (C41S,
P162A, L467P, 655delAC). The mutations C41S, P162A, T607I, 655delAC
have been found in 2 unrelated cases. In conclusion, the prevalence of
heterozygous TSHR mutations in a pediatric series of hyperTSH is
surprisingly elevated. The diagnosis of TSH resistance by means of TSHR
gene analysis retains a primary role for appropriate clinical management of
subjects with hyperTSH and genetic counseling of their families.
Expression gene profile may be useful for the diagnosis of thyroid
Pamela Piampiani1, Cristina Romei1, Barbara Cosci1, Agnese Vivaldi1,
Raffaele Ciampi1, David Viola1, Valeria Bottici1, Riccardo Giannini2,
Fulvio Basolo2, Aldo Pinchera1 & Rossella Elisei1
Department of Endocrinology, University of Pisa, Pisa, Italy; 2Department
of Oncology, University of Pisa, Pisa, Italy.
Although 20% of follicular neoplasms are papillary thyroid carcinoma (PTC),
their cytological diagnosis is not diagnostic. A different profile of gene
expression between malignant and benign thyroid tumors has been reported.
Aim of this study was to identify a gene expression profile to be used in
distinguishing malignant from benign thyroid neoplasms. By real-time RT-PCR
we analyzed mRNA expression of 6 thyroid differentiation genes (TTF-1,
PAX8, TPO, TSHr, NIS and Tg) and 5 genes known to be involved in thyroid
tumorigenesis [PPARg, Gal3, EGFR, MET and oncofibronectin (onfFN)] in
174 human thyroid tissues (87 tumor samples and 87 corresponding normal
tissues) belonging to 72 patients affected with PTC and 15 patients affected
with benign nodular disease (BND). Our results indicate that thyroid
differentiation genes and PPARg were significantly less expressed in PTC
samples than in normal tissue (TPO, 61/72 cases, P!0.0001; NIS, 64/72 cases,
P!0.0001; Tg, 59/72 cases, PZ0.0002; TSHr, 57/72 cases, PZ0.0169; TTF1,
47/72 cases, PZ0.002; PAX8, 55/72 cases, PZ0.0001; PPARg, 57/72 case,
P!0.0001). On the contrary, 3 genes were more expressed in the tumor than
in normal tissue (onfFN, 64/72 cases, P!0.0001; MET, 55/72 cases, PZ
0.0018; Gal3, 53/72, P!0.0001). No statistically significant difference was
observed for the mRNA expression of EGFR between tumoral and normal
tissues. In BND a statistically significant difference between mRNA expression
in tumoral and normal tissue was observed only for PPARg as observed in
Endocrine Abstracts (2007) Vol 14
PTC specimen. Summarising, our data show that 10/11 selected genes are
differentially expressed in the tumor tissue with respect to normal. On the
contrary only 1/11 was differentially expressed in BND with respect to its
normal tissue. In conclusion, 9/11 of these genes are characterized by a gene
expression profile that was specific for the malignant neoplasms. The analysis
of the levels of expression of these genes in Fine Needle Aspiration material
might represent a helpful and innovative method for the presurgical diagnosis
of citologically indeterminate thyroid nodules.
Persistence of decreased peripheral B-lymphocytes after Rituximab
treatment is associated to inactive disease in patients with thyroidassociated ophthalmopathy
Irene Campi1, Guia Vannucchi1, Danila Covelli1, Paola Bonara2,
Nicola Currò3, Davide Dazzi4, Giacinta Pirola3, Stefania Rossi5,
Claudio Guastella6, Paolo Beck-Peccoz1 & Mario Salvi1
Endocrine Unit Department of Medical Science; 2Internal Medicine;
Ophthalmology; Fondazione Policlinico IRCC, University of Milan, Milan,
Italy; 4Internal Medicine, Ospedale di Fidenza, Fidenza, Italy; 5Pathology
Unit, Department of Medicine, Surgery and Dentistry, University of Milan,
Ospedale S. Paolo and Fondazione Policlinico IRCCS, Milan, Italy;
Otolaryngology, Fondazione Policlinico IRCC, University of Milan, Milan,
The anti-CD20 antibody Rituximab (RTX) induces peripheral B cells
depletion. Aim of the present study was to evaluate changes of lymphocytes
after RTX therapy, administered at the dosage of 1000 mg twice at 2-week
interval, in 10 patients with Graves’ disease, 8 of whom had associated
ophthalmopathy (TAO). In all patients, we studied the standard immunophenotypic panel before therapy and monthly for up to 2 years. Total CD20C
(and CD19C) cell depletion was observed after the first infusion in 9 patients
while one patient had persistence of !5% CD19CCD5C lymphocytes. 8/10
patients were depleted for 4–6 months after RTX, while 1 and 1 patients after
2 and 10 months respectively. A reduction of CD20C cells of about 50% from
baseline was observed in 6 patients at 18 months and in 3 at 26 months. While
after RTX there was no significant change of serum thyroid autoantibodies
levels, nor correlation with CD20C depletion, we observed a stable
improvement of TAO with a significant decrease of the clinical activity
score. Although progression to inactive TAO did not correlate with CD20C
cells, since at 5 months they began repopulating, we did not observe relapse of
active TAO even after B cell return. In contrast, in the patient with persistence
of CD19C5C, severe TAO relapsed at the time of CD20C cells return.
Another cycle of RTX (1000 mg) was then administered but again we observed
persistence of !7% CD19C5C with no definite improvement of the clinical
signs of TAO. At subsequent orbital decompression we were able to detect
CD19C5C in the orbital tissues. In conclusion, in patients with TAO a
reduction of CD20C of about 50% from the baseline is still present at 18–24
months after RTX treatment. This may explain the consistent improvement of
TAO and the lack of relapse, in patients after total B-cells depletion.
Persistence of CD19C5C lymphocytes in the peripheral blood and, perhaps,
in the orbit, may associate to a not completely satisfactory therapeutic
A novel tyrosine-kinases selective inhibitor with anti-tumoral efficacy
(Sunitinib) induces a block in iodine uptake and transient
Deborah Mannavola1, Guia Vannucchi1, Marco Carletto2, Virgilio Longari2,
Rossella Bertuelli3, Paola Coco3, Paolo Casali3, Paolo Beck-Peccoz1 &
Laura Fugazzola1
Endocrine Unit, Dept. of Medical Sciences, University of Milan,
Fondazione Policlinico IRCCS, Milan, Italy; 2Nuclear Medicine Unit,
Fondazione Policlinico IRCCS, Milan, Italy; 3Dept. of Oncology, Istituto
Nazionale dei Tumori, Milan, Italy.
Sunitinib (SU11248) is a multitarget inhibitor of tyrosine-kinases (RTK)
recently tested in clinical trials for the treatment of some human cancers. Side
effects are mostly represented by asthenia and appear in a dose and time
9th European Congress of Endocrinology, Budapest, Hungary, 2007
correlated manner. After the unexpected observation of a myxedematous coma
in a patient affected with GIST and treated with Sunitinib, we evaluated the
effect of this drug on thyroid function in 24 patients treated for GISTs Imatinib
resistant. Patients received the following cycles of therapy: 4 weeks of daily
treatment at the dose of 50 mg/day orally (ON) and 2 weeks of withdrawal
(OFF). On days 1 and 28 of each cycle TSH, FT3, FT4, thyroglobulin, anti-Tg
and anti-TPO autoantibodies were measured. Eleven patients (46%) treated
with SU11248 developed a transient hypothyroidism between the 1st and the
6th cycle of treatment (median 3rd cycle). Hypothyroidism was subclinical in
10 cases and overt in 1 patient. During the OFF periods TSH normalized, but a
progressive increase of TSH levels was observed. After a variable number of
cycles, the lack of normalization during the OFF periods was observed. In
order to elucidate the possible mechanism underlying Sunitinib-induced
hypothyroidism, in vivo morpho-functional examinations were performed.
Neither ultra-sonographic alterations (in particular destructive-like), nor
variations in thyroglobulin and anti-thyroid autoantibodies, were observed
during the ON and OFF phases even after several cycles. On the contrary, 123I
uptake was normal in basal conditions and largely reduced after the 4 weeks of
treatment, with partial or total normalization after the 2 weeks of withdrawal.
In conclusion, SU11248 determines hypothyroidism in the 46% of patients.
The absence of anti-thyroid autoantibodies and the normal echographic pattern
allow to exclude autoimmune and/or destructive mechanisms. Interestingly,
hypothyroidism seems to be correlated with a defect in the uptake of iodine.
The possibility to perform a selective and temporary block of thyroid function
could be useful in the treatment of some thyroid diseases.
Meta-analyses of individual-level data from 10 (nZ4.906 subjects) and 5 (nZ
2.386) collaborating teams for GD and HT, respectively, using haplotypes of both
polymorphisms were also performed. Group-level data suggested significant
associations with GD and HT for both A49G (odds ratio 1.49, PZ6!10K14 and
1.29 [PZ0.001] per G allele, respectively) and CT60 (OR 1.45, [PZ2!10K9]
and 1.64 [PZ0.003] per G allele, respectively). Results were consistent between
Asian and Caucasian descent subjects. Individual-level data showed that
compared with the AA haplotype the risk conferred by the GG haplotype was
1.49 (95% CI: 1.31–1.70) and 1.36 (95% CI: 1.16–1.59) for GD and HT,
respectively. The AG haplotype also increased the risk of GD (1.35, 95% CI:
1.16–1.55) but not of HT (1.02, 95% CI: 0.71–1.47). The results for the GA
haplotype were inconclusive. Data were consistent with a dose-response effect for
the G-allele of CT60.
The CT60 polymorphism of CTLA-4 maps an important genetic determinant for
the risk of both GD and HT across diverse populations.
Sensitization against Soybean may induce an increase in the levels of
anti-thyroid peroxidase antibodies in thyroid autoimmunity
Ildikó Molnár
Kenézy County and Teaching Hospital, Debrecen, Hungary.
CTLA- 4 gene polymorphisms and autoimmune thyroid diseases: metaanalyses of published and individual-level data
Fotini Kavvoura1, Takashi Akamizu2, Takuya Awata3, Yoshiyuki Ban4,
Dimitry Chistiakov5, Irena Frydecka6, Abbas Ghaderi7, Stephen Gough8,
Yuji Hiromatsu9, Rafal Ploski10, Pei-Wen Wang11, Yoshio Ban4,
Tomasz Bednarczuk12, Emma Chistiakova13, Marcin Chojm10,
Joanne Heward8, Hitomi Hiratani2, Suh-Hang Hank Juo14, Lidia Karabon18,
Shigehiro Katayama3, Susumu Kurihara3, Rue-Tsuan Liu11, Ikuyo Miyake9,
Gholam-Hossein Omrani15, Edyta Pawlak18, Matsuo Taniyama16,
Teruaki Tozaki17 & John PA Ioannidis1
Department of Hygiene and Epidemiology, University of Ioannina School
of Medicine, Ioannina, Greece; 2Translational Research Center, Kyoto
University Hospital, Kyoto University School of Medicine, Kyoto, Japan;
Department of Medicine, Saitama Medical University, Saitama, Japan;
Third Department of Internal Medicine, Showa University School of
Medicine, Tokyo, Japan; 5Department of Pathology, University of
Pittsburgh Medical Center, Pittsburgh, PA, United States; 6Department of
Hematology, Medical Academy, Wroclaw, Poland; 7Shiraz Institute for
Cancer Research, Medical School, Shiraz University of Medical Sciences,
Shiraz, Iran; 8Institute of Biomedical Research, The Medical School,
University of Birmingham, Birmingham, United Kingdom; 9Kurume
University School of Medicine, Kurume, Fukuoka, Japan; 10Human
Molecular Genetics Laboratory of the Department of Forensic Medicine,
Department of Medical Genetics, Medical University of War, Warsaw,
Poland; 11Chang Gung Memorial Hospital-Kaohsiung Medical Center,
Chang Gung University College of Medicine, Kaohsiung, Taiwan;
Department of Endocrinology, Medical Research Center, Polish Academy
of Science, Warsaw, Poland; 13Department of Molecular Diagnostics,
National Research Center GosNIIgenetika, Moscow, Russia; 14Graduate
Institute of Medical Genetics, Kaohsiung Medical University Hospital,
Kaohsiung, Taiwan; 15Endocrine and Metabolism Research Center,
Namazee Hospital, Shiraz, Iran; 16Division of Endocrinology and
Metabolism, Showa University Fujigaoka Hospital, Yokohama, Kanagawaken, Japan; 17Department of Medical Information, Showa University School
of Pharmaceutical Science, Showa, Japan; 18Institute of Immunology and
Experimental Therapy, Polish Academy of Sciences, Wroclaw, Poland.
CTLA-4 polymorphisms have been widely examined for their associations with
autoimmune thyroid diseases (Graves’ disease [GD] and Hashimoto thyroiditis
[HT]) but their relative population effect remains unclear.
Methodology/Principal findings
Meta-analyses of group-level data from 32 (nZ11.019 subjects) and 12 (nZ
4.479) published and unpublished studies were performed for the association of
the A49G polymorphism with GD and HT, respectively. Fifteen (nZ7.246) and 6
(nZ3.086) studies were available for the CT60 polymorphism, respectively.
Soybean diet could involve in the development of goitre according to antithyroid
effects of isoflavones. Isoflavones from Soybean could induce not only inhibition
of thyroid peroxidase (TPO) catalyzed reactions but they are allergens for patients
suffering from atopic or autoimmune diseases. Two hundred-sixty patients with
thyroid autoimmunity (150 with Graves’ disease, 110 with Hashimoto’s
thyroiditis) were investigated for the sensitization against Soybean. Allergenspecific IgE levels were measured by Western blot Allergy Screen panels and the
levels of thyroid hormones (TSH, FT 4 , FT 3 ) and anti-TPO, anti-Htg
(thyroglobulin), TSH receptor (TRAK) antibodies were detected by immunoassay. The data were presented as meanGSE.
Allergic sensitization against Soybean was as follows: 24 cases in Graves’
disease and 16 cases in Hashimoto’s thyroiditis. Graves’ patients with Soybean
allergy showed increased anti-TPO levels compared to patients who were
negative for allergen (567.33G82.88 IU/ml vs 264.88G30.77 IU/ml, P!0.001).
However, in patients with Soybean allergy, the elevation in anti-TPO levels was
higher in hyperthyroid cases than in those without allergy (736.6G138.87 IU/ml
(nZ7) vs 296.15G50.81 IU/ml (nZ41), P!0.011). Surprisingly, higher FT3
(and FT4) levels were demonstrated in sensitized hyperthyroid cases compared to
nonsensitized ones (15.92G4.7 pg/ml vs 5.44G0.56 pg/ml, P!0.001 for FT3
(and P!0.049 for FT4)). The increase in anti-TPO levels for sensitized euthyroid
Graves’ patients strongly associated with ophthalmopathy in comparison
with nonsenzitized ones (669.98G162.38 IU/ml (nZ6) vs 156.81G
48.46 IU/ml (nZ29), P!0.003).
In conclusion, the presence of Soybean allergen-specific IgE levels in
thyroid autoimmunity could contribute to the elevation in anti-TPO levels for
Th2 dominant Graves’ disease. The sensitization against Soybean may induce
thyroid autoimmunity due to increased anti-TPO levels in disease susceptible
Pregnant women on thyroxine substitution are often dysregulated in
early pregnancy
Bengt Hallengren1, Mikael Lantz1, Bengt Andreasson2 & Lars Grennert3
Department of Endocrinology, Malmö University Hospital, Malmö,
Sweden; 2Department of Pediatrics, Malmö University Hospital, Malmö,
Sweden; 3Department of Obstetrics and Gynecology, Malmö University
Hospital, Malmö, Sweden.
Thyroid hormones are important for normal fetal development. The aim of this
prospective study was to explore whether thyroxine treated pregnant women with
hypothyroidism are adequately thyroxine substituted during pregnancy.
Endocrine Abstracts (2007) Vol 14
9th European Congress of Endocrinology, Budapest, Hungary, 2007
Material and method
During the years 1997–2002 119 pregnancies in 101 females with thyroid
diseases were followed at the Department of Endocrinology. The diagnoses were
autoimmune thyroiditis (AIT) with or without hypothyroidism nZ46, hypothyroidism (non AIT) nZ9, status post Graves’ thyrotoxicosis (GD) nZ33, active
GD nZ8, multinodular toxic goitre (MNTG) nZ2, atoxic goitre with or without
autonomous function nZ20, operated thyroid cancer nZ1 (C1 in the group
status post GD).
64 patients were on thyroxine due to hypothyroidism at the first visit: 50%
(32/64) had serum TSH values within the reference range (0.4–4.0 mIE/l) at
first laboratory control. 20% (13/64) had TSH!0.40 mIE/l, 14% (9/64)
%0.1 mIE/l, 30% (19/64) had TSHO4.0 mIE/l, 14% (9/64)O10 mIE/l. 67%
(44/66) had to increase the dose during pregnancy, 2/66 could stop thyroxine
medication when finishing antithyroid drugs, 30% (20/66) did not have to
change the dose.16 miscarriages, 1 late miscarriage, 1 intrauterine fetal death
occurred. Of these 18/119 (15%) patients 78% (14/18) had TSH outside the
reference range at first control. 44% (8/18) had TSH!0.40 mIE/l, 33% (6/18)
had TSHO4.0 mIE/l.
In 50% of pregnant women on thyroxine substitution the serum TSH values were
outside the reference range at first control. A majority had to increase the
thyroxine substitution during pregnancy. In pregnant women with miscarriage a
great majority had TSH values outside the reference range at first control. The
study demonstrates that pregnant women with thyroxine substitution should be
carefully checked and the thyroxine dose increased early in pregnancy to avoid
OC2.1 Bone and calcium – OC2
Effect of once-yearly infusion of zoledronic acid 5 mg in postmenopausal women with osteoporosis
Richard Eastell1, Peter Lakatos2, Dennis Black3, Steven Boonen4,
Felicia Cosman5, Steven Cumings3, Pierre Delmas6, Erik Fink Eriksen7,
Ping Chung Leung8, Zulema Man9, Peter Mesenbrink10, Ian Reid11 &
Jane Cauley12
University of Sheffield, Sheffield, United Kingdom; 2Semmelweis
University, Budapest, Hungary; 3University of California, San Francisco,
San Francisco, CA, United States; 4Leuven University Center for Metabolic
Bone Diseases, Leuven, Belgium; 5Helen Hayes Hospital, West Haverstraw,
NY, United States; 6INSERM Unit 403, Hopital Edouard Herriot, Lyon,
France; 7Novartis Pharma AG, Basel, Switzerland; 8The Chinese University
of Hong Kong, Hong Kong, China; 9Centro TIEMPO, Buenos Aires,
Argentina; 10Novartis Pharmaceuticals Corporation, East Hanover, NJ,
United States; 11University of Auckland, Auckland, New Zealand;
University of Pittsburgh, Pittsburgh, PA, United States.
Background and methods
The HORIZON-PFT is a multinational, 3-year, randomized, double-blind,
placebo-controlled trial evaluating the potential of once-yearly zoledronic acid
(ZOL) 5 mg, infused over 15 minutes, to decrease risk of fracture in 7736
postmenopausal osteoporotic women 65–89 years of age.
Treatment with ZOL 5 mg resulted in significant relative risk reductions in
morphometric vertebral fracture of 70% vs PBO (3.8% vs 12.8%; 95% CI [62%,
76%]) and in hip fracture of 41% vs PBO (1.4% vs 2.5%; 95% CI [17%, 58%]).
Secondary endpoints, non-vertebral (excluding finger, toe, and facial), clinical
vertebral, and any clinical fracture (including non-vertebral, hip, and clinical
vertebral), were significantly reduced by 25%, 77%, and 33% (all P!.0001),
respectively. Bone mineral density increased significantly in ZOL vs PBO at total
hip (6.0%), lumbar spine (6.9%), and femoral neck (5.0%) (P!.0001). While
transient increases in serum creatinineR0.5 mg/dl over pre-infusion levels were
seen in a small fraction (1.3%) of patients in the ZOL 5 mg group, no cumulative
impact on renal function was demonstrable. Hypocalcemia (serum calcium!
2.075 mmol/l) was observed in 2.3% of patients. Virtually all events occurred after
the first infusion of ZOL and all were asymptomatic and transient. Adverse events
occurring%3 days after infusion were more frequent after first infusion (44.7%
ZOL vs 14.7% PBO) but declined markedly on subsequent infusions. There were
more atrial fibrillation serious adverse events in ZOL vs PBO (1.3% vs 0.5%). Two
cases of osteonecrosis of the jaw (1 in PBO, 1 in ZOL) were identified on
adjudication; both resolved with antibiotic therapy and limited debridement.
Endocrine Abstracts (2007) Vol 14
Once-yearly infusion of ZOL 5 mg over 3 years achieves a highly significant
decrease in vertebral, hip, and other fracture risk and is generally safe and well
Role of IGF system on the regulation of osteoblast aromatase activity
in vitro
Claudia Palermo, Marica Arvigo & Francesco Minuto
Department of Endocrinological & Metabolic Sciences and Center of
Excellence for Biomedical Research, University of Genoa, Genoa, Italy.
Several studies demonstrated that IGFs stimulate aromatase activity in ovary
but no data on bone are available. In the present study the role of IGF system
components on aromatase action has been characterized during osteogenic
differentiation in a model of rat tibial osteoblasts. At confluence (day 0) cells
have been transferred to differentiating medium supplemented with 1% FCS
and delta4androstenedion with or without IGF-II 3 nM, IGFBP-2 1 nM and
IGFBP-3 1 nM. Cells have been treated with test substances continuously for
9 days or at intervals corresponding to the stages of osteogenesis: Stage 1Z
proliferation; Stage 2Zextracellular matrix deposition; Stage 3Zmineralization of extracellular matrix. The aromatase activity has been evaluated by
measuring in the conditioned medium the concentration of estradiol by a
competitive chemiluminescent enzyme immunoassay. The differentiating effect
has been evaluated by the measurement of alkaline phosphatase, which is an
early marker of osteogenesis and of calcium incorporation, which is a late
marker of osteogenesis. The secretion of the metalloproteinases by means of
zymogram has been evaluated in different stages. The results showed that the
continous treatment for 9 days with IGF-II and IGFBP-2 alone or in
combination, inhibits the physiologic decrease of aromatase and stimulates the
differentiation markers, including the metalloproteinase activation. Conversely,
treatment with IGFBP-3 inhibits both aromatase activity and cellular
differentiation. IGF-II, IGFBP-2 and IGFBP-3 exerted their action on
aromatase activity and cellular differentiation also when added in S1 stage.
IGF-II resulted ineffective when added alone in S2 or S3 but in S2 addition of
IGFBP-2 restored the effect. IGFBP-3 and IGFBP-2 exerted their action also
in S2 but not in S3.
In conclusion, these preliminary data suggest that in our cell system the
aromatase activity is related to the osteogenic differentiation stages. Moreover,
the IGF system plays an important role in the regulation of both bone
aromatase activity and osteogenesis.
Clinical and biochemical differences in patients affected with sporadic
and type 1 multiple endocrine neoplasia (MEN) related primary
Cristina Eller-Vainicher1, Sara Massironi2, Maddalena Peracchi2,
Luca Persani3, Paolo Beck-Peccoz1, Anna Spada1 & Sabrina Corbetta4
Endocrine Unit, Medical Sciences Department, University of Milan,
Fondazione Ospedale Maggiore, Mangiagalli, Regina Elena IRCCS, Milan,
Italy; 2Gastroenterology Unit, Department of Medical Sciences, University
of Milan, Fondazione Ospedale Maggiore, Mangiagalli, Regina Elena
IRCCS, Milan, Italy; 3Lab of experimental endocrinology, Department of
Medical Sciences, University of Milan, Istituto Auxologico Italiano IRCCS,
Cusano Milanino, Milan, Italy; 4Endocrinology and Diabetology Unit,
Department of Medical-Surgical Sciences, University of Milan, Policlinico
San Donato IRCCS, San Donato, Milan, Italy.
Primary hyperparathyroidism (PHPT) may occur sporadically or within MEN
syndromes. It is classically thought that PHPT in MEN occurs at earlier ages than
sporadic PHPT without significant differences in clinical and biochemical
presentation. The aim of the study was to compare clinical and biochemical
parameters between sporadic PHPT and MEN1 patients. The study included 41
genetically diagnosed MEN1 patients (14M, 27F) and 88 sporadic PHPT patients
(24M, 64F) matched for age at diagnosis. All PHPT patients were studied for
calcium metabolism parameters and renal and bone complications and evaluated
9th European Congress of Endocrinology, Budapest, Hungary, 2007
for familial history and the presence of signs or symptoms possibly related to
MEN1. Young (!50 ys) MEN1 patients showed significantly lower serum PTH
(71.23G50.89 vs 224.42G220.20 mg/dl, meanGSD, PZ0.019), total (11.05G
0.56 vs 12.02G1.22 mg/dl, PZ0.015) and ionized calcium levels (1.48G0.07 vs
1.62G0.19 mmol/l, PZ0.021) compared with age-matched sporadic PHPT
patients, while such differences were not detected in old (51–70 ys) MEN1 vs
sporadic PHPT patients. Despite the low PTH and calcium levels in MEN1, the
prevalence of nephrolithiasis and osteoporosis was similar in the two PHPT
forms. A female to male ratio of 1:1 was observed both in MEN1, as expected,
and young sporadic PHPT patients. Moreover, young sporadic PHPT patients
showed significantly higher serum calcium levels than the old patients (12.0G1.2
vs 11.2G0.9 mg/dl, PZ0.008), in contrast to the pattern observed in MEN1. Our
data suggested that milder hypercalcemia and PTH levels within the normal range
were not uncommon in young MEN1 with respect to young sporadic PHPT
patients, though both groups of patients did not differ for renal and bone
complications. In conclusion, young symptomatic hyperparathyroid patients with
slightly elevated serum calcium and PTH levels should be carefully screened for
MEN1 diagnosis.
Assessment of prevalent vertebral deformities in morphometric X-ray
Elzbieta Skowronska-Jozwiak1, Pawel Pludowski2,
Elzbieta Karczmarewicz2, Andrzej Lewinski1 & Roman Lorenc2
Department of Endocrinology & Metabolic Diseases, The Medical
University of Lodz, Lodz, Poland; 2Department of Biochemistry and
Experimental Medicine, The Children’s Memorial Health Institute, Warsaw,
Vertebral morphometric X-ray absorptiometry (MXA) is a new tool developed to
evaluate the presence of vertebral deformities. Low dose of radiation, fan-beam
and the centerline scan technique are believes more advantageous than the classic
morphometry using conventional lateral radiograms. We assessed the prevalence
of vertebral fractures by MXA in adult population of Łódź region as a part of
Polish population studied in EPOLOS epidemiological study.
Patients and methods
362 subjects without history of osteoporosis in anamnesis were examined [244
women, mean age 53G16 years (xGSD) and 97 men, mean age 53G14 years]. MXA
lateral scans were performed using DXA system Expert-XL. Six point digitization
were used to calculate the anterior (Ha), central (Hc), and posterior (Hp) height of the
vertebral bodies Th4-L4. Vertebra were defined as having prevalent deformities when
at least one ratio value (Ha/Hp, Hc/Hp, Hp/Hp up, or Hp/Hp low) fell 3 SD below or
even more than the reference mean of that ratio at any vertebral level.
3969 vertebrae were analyzed. 126 (3.17%) vertebrae in 863 subjects (22.7% of
examined individuals) were classified as deformed. In 56 subjects (69.13%) one
deformity and in 25 subjects multiple deformities were detected. In 89% of fractures,
mild deformities (grade 1) were observed. The prevalence of vertebral fractures was
higher in women and increased with age. Th8 and Th12 were the most frequently
Bone studies indicated that, as in other regions of Poland, also in Łódź region
vertebral osteoporotic fractures are common. Thus, the morphometric X-ray
absorptiometry (MXA) seems to be a useful and safe tool in the diagnostics of
vertebral fractures.
Effect of gonadal status on baseline and after rhGH treatment
prevalence of spinal deformities in adult patients with growth hormone
deficiency (GHD)
Gherardo Mazziotti1, Antonio Bianchi2, Stefania Bonadonna1,
Monica Nuzzo1, Vincenzo Cimino2, Alessandra Fusco2, Laura De Marinis2
& Andrea Giustina1
Department of Internal Medicine, University of Brescia, Brescia, Italy;
Department of Endocrinology, Catholic University, Rome, Italy.
Adult GHD patients may have reduced BMD, which is thought to be reverted by
long-term rhGH replacement therapy. We have recently reported high prevalence
of vertebral osteoporotic deformities in untreated adult GHD patients. Gonadal
status is the main determinant of bone loss in patients with primary form of
In this cross-sectional study, we investigated whether the prevalence and
degree of spinal deformities in adults with treated or untreated GHD was in
relation to the gonadal status of the patients. Seventy-six adult hypopituitary
patients (46 males and 30 females; mean age 46.8 years, range: 16–81) with
severe GHD were evaluated for BMD (dual-energy X-ray absorptiometry) and
vertebral deformities (T4-L5 quantitative morphometric analysis according to
Genant score). At the study entry, 41 patients were eugonadic (21 patients with
preserved gonadal function and 20 patients in adequate replacement therapy),
whereas 35 patients were hypogonadic.
Vertebral deformities (O20%) were found in 48 patients (63.2%), with higher
prevalence in untreated (42 cases) vs. treated patients (24 cases) [76.9% vs.
33.3%; P!0.001]. Eugonadic and hypogonadic patients with untreated GHD
showed comparable fracture rate (78.6% vs. 75.0%; PZ0.8). rhGH replacement
therapy was accompanied by a significant decrease in fracture rate as compared to
untreated patients [eugonadic: 35.3% vs. 75.0%, PZ0.01; hypogonadic: 28.6%
vs. 78.6%, PZ0.01]. Eugonadic patients had slightly but significantly higher
BMD than hypogonadic patients. Multivariate logistic regression analysis
demonstrated that no treatment with rhGH was the only factor significantly
influencing the occurrence of spinal deformities in adult GHD patients (odds
ratio: 5.8, CI 95% 1.9–18.1) whereas no significant correlation was found with
gonadal status, BMD, sex and age.
Gonadal status of adult patients with GHD may be not critical for the
prevalence of vertebral radiological deformities which is instead mainly affected
by the replacement treatment with rhGH.
Sunlight exposure and vitamin D supplementation at the institutionalized elderly – effects on calcium and bone metabolism
Peter Bottermann2, Dumitru Branisteanu1, Voichita Mogos1 &
Eusebie Zbranca1
University of Medicine and Pharmacy “Gr.T.Popa”, Iasi, Romania;
Technical University, Munchen, Germany.
We investigated calcium and bone metabolism in a group of 123
institutionalized volunteers between 60 and 98 years old, 73 females and
50 males. 25OH-D 3 was measured by an indoor RIA technique.
1.25(OH)2D3 was measured by HPLC, serum calcium by photocolorimetry,
bone alkaline phosphatase by immunoenzymatic technique, whereas serum
PTH and urinary deoxypyridinoline (DPD) were measured by IRMA.
Almost all volunteers (92.6%) had low 25OH-D3 values, but normal or even
increased levels of the active hormone, 1.25(OH)2D3. High PTH was found
in 40 cases (32.5%), of which three were primary hyperparathyroidism,
whereas the others had low or low-normal calcium levels (secondary
hyperparathyroidism). PTH-induced 1a hydroxylation in the elderly with
undamaged kidney function seems to compensate the paucity of vitamin D
substrate. More than half of the cases had high DPD levels, suggesting high
bone turnover. Bone turnover parameters were higher in females than in
males (P!0.05). A positive correlation between PTH and urinary DPD was
noticed (R2Z0.351), suggesting the role of secondary hyperparathyroidism
in high turnover bone loss. We further supplemented the vitamin D intake in
42 volunteers with a daily dose of 2000 IU of 25-OHD3 for three months in
the summer period, whereas other 42 volunteers received placebo (vitamin
B). Normalization of 25-OHD3 levels was seen in both groups, suggesting
that even mild sun exposure increases skin resources of vitamin D. A more
significant increase in both 25OH-D3 and 1.25(OH)2D3 was however
observed in the vitamin D-treated group. Normalization of serum PTH,
but not of turnover parameters was observed in both groups. Mild
hypercalcemia and increase in serum creatinine were noticed in the vitamin
D-treated group. Vitamin D supplementation might therefore be accompanied by hypercalcemic and nephrotoxic effects at doses higher than 2000
IU/day. Sunlight exposure seems efficient to replenish vitamin D reserves at
institutionalized patients.
Endocrine Abstracts (2007) Vol 14
9th European Congress of Endocrinology, Budapest, Hungary, 2007
OC3.2 – ESE Young Investigator Award
Vitamin K2 induces phosphorylation of protein kinase A and expression
of novel target genes in osteoblastic cells
Kuniko Horie-Inoue1, Tomoe Ichikawa1 & Satoshi Inoue2
Research Center for Genomic Medicine, Saitama Medical University,
Hidaka-shi, Saitama, Japan; 2Graduate School of Medicine, the University
of Tokyo, Bunkyo-ku, Tokyo, Japan.
Adrenal lesions in multiple endocrine neoplasia type 1: data from the
French Group for the Study of Endocrine Tumors (GTE)
Blandine Gatta1, Maud Monsaingeon1, Pierre Goudet2, Arnaud Murat3,
Patricia Niccoli-Sire7, Alain Calender5, Vincent Rohmer6, Olivier Chabre4
& Antoine Tabarin1
Dpt Endocrinology, Bordeaux, France; 2Dpt Surgery, Dijon, France; 3Dpt
Endocrinology, Nantes, France; 4Dpt Endocrinology, Grenoble, France;
Lab Genetics, Lyon, France; 6Dpt Endocrinology, Angers, France; 7Dpt
Endocrinology, Marseille, France.
Vitamin K is known as a critical cofactor in blood coagulation and bone
homeostasis by helping the function of vitamin K-dependent gammacarboxylase. We have recently shown that vitamin K2, one of the natural
vitamin Ks, has a novel function to regulate the transcription of extracellular
matrix-related genes in osteoblastic cells and increase collagen accumulation by
activating the steroid and xenobiotic receptor, SXR. In the present study, we
searched for novel vitamin K target genes up-regulated specifically by
menaquinone-4 (MK-4), a potent vitamin K2 isoform, using oligonucleotide
microarray analysis in human osteoblastic MG63 cells. Among these genes,
growth differentiation factor (GDF15) and stanniocalcin 2 (STC2) were
characterized as MK-4-specific targets, as their mRNA expression was not
induced by vitamin K1, another vitamin K2 isoform MK-7, or the MK-4 side
chain structure geranylgeraniol. The MK-4-specific induction of GDF15 and
STC2 was also observed in murine MC3T3-E1 cells and shown to be
independent of either gamma-carboxylation or SXR signaling. As a possible
mechanism for MK-4-specific gene regulation, we investigated the contribution
of protein kinase A (PKA), one of the key regulators of transcription in
osteoblasts. We found that MK-4 enhanced PKA phosphorylation, and the
MK-4-specific induction of GDF15 and STC2 genes was reduced by treatment
with the PKA inhibitor H89 or siRNA against PKA alpha-catalytic subunit. In
conclusion, vitamin K2 has novel functions beside its activity as a coenzyme and
plays a significant role in regulating various gene expression and modulating
collagen production in osteoblastic cells.
The characteristics of adrenal involvement in Multiple Endocrine Neoplasia
type 1 (MEN1) have been defined from studies involving a limited number of
patients. We have assessed retrospectively the prevalence, characteristics and
evolution of adrenal involvement from the French group for the study of
endocrine tumours (GTE) registry, involving 688 patients with MEN1. In our
series, adrenal tumours identified at abdominal imaging occurred in 130
patients (18.9%). The mean age of patients at the discovery of the adrenal
lesion was 46.1 yr (range, 2–78 yr). Adrenal lesions were bilateral in 32% of
cases and the mean tumor diameter was 27.6 mm (range, 7–70 mm). Hormonal
hypersecretion was found in 16% of patients with adrenal involvement (10
cases of Cushing’s syndrome, 7 cases of primary hyperaldosteronism, 2 cases
of hyperandrogenism and 1 pheochromocytoma). Among adrenal lesions that
were removed, histopathologic examination revealed benign lesions (adenoma
and hyperplasia) in 87.5% of cases, adrenal carcinoma in 7.5% and adrenal
metastasis in 5%. Overall, malignancy of adrenal lesions was documented in
3.8% of the whole series. Adrenal lesions were associated with enteropancreatic tumors in 66.4% of cases. In patients in whom follow-up imaging was
available (mean 6.6 years), 15% demonstrated significant tumoral progression
and 13% developed controlateral lesions. No case of adrenal malignancy was
found during the follow-up. No correlation was found between genotypic
lesions of the menin gene and the presence or the type of adrenal lesion. In our
series, adrenal tumours are a less frequent than previously reported. Most of
adrenal lesions are small in size benign and not responsible for hormonal
hypersecretion. Our series do not support the hypothesis of a physiopathologic
link between pancreatic tumours and adrenal lesions in MEN1.
Endocrine tumors and neoplasia – OC3
Multiple somatostatin receptor subtypes activation reduces cell viability
in non-functioning pituitary adenomas by inhibiting Vascular
Endothelial Growth Factor secretion
Maria Chiara Zatelli1, Daniela Piccin1, Federico Tagliati1, Maria
Rosaria Ambrosio1, Antonio Bianchi2, Marta Bondanelli1, Herbert
A Schmid3, Massimo Scanarini4, Laura De Marinis2, Giulio Maira5 & Ettore
C degli Uberti1
Section of Endocrinology, Department of Biomedical Sciences and
Advanced Therapies – University of Ferrara, Ferrara, Italy; 2Institute of
Endocrinology, Catholic University of Rome, Rome, Italy; 3Novartis
Institutes for Biomedical Research, Oncology, Basel, Switzerland;
Division of Neurosurgery – Hospital of Padova, Padova, Italy; 5Department
of Neurosurgery, Catholic University of Rome, Rome, Italy.
Somatostatin (SRIF) analogs have been employed in medical therapy of nonfunctioning pituitary adenomas (NFA), with contrasting results. Previous
evidence showed that SRIF can exert its antiproliferative effects by reducing
Vascular Endothelial Growth Factor (VEGF) secretion and action, and that
VEGF expression may be related to pituitary tumor growth. The aim of our
study was to clarify the possible effects of a multireceptor SRIF ligand on VEGF
secretion and cell proliferation in human NFA primary cultures, we assessed
SRIF receptors (SSTR1-5) expression and the in vitro effects on VEGF secretion
and on cell viability of SRIF and of the stable SRIF analogue pasireotide
(SOM230) which activates SSTR1, 2, 3 and 5. Twenty-five NFA were examined
by RT-PCR for expression of a-subunit, SSTR, VEGF, and VEGF receptors 1
(VEGF-R1) and 2 (VEGF-R2). Primary cultures were tested with SRIF and with
pasidreotide. All NFA samples expressed a-sub, VEGF and VEGFR-1 and 2,
while SSTR expression pattern was highly variable. Two different groups were
identified according to VEGF secretion inhibition by SRIF. VEGF secretion and
cell viability were reduced by SRIF and pasireotide in the “responder” group,
but not in the “non responder” group, including NFA expressing SSTR5. SRIF
and pasireotide completely blocked Forskolin-induced VEGF secretion. In
addition, SRIF and pasireotide completely abrogated the promoting effects of
VEGF on NFA cell viability. Our data demonstrate that pasireotide can inhibit
NFA cell viability by inhibiting VEGF secretion, and suggest that the
multireceptor-SSTR agonist pasireotide might be useful in medical therapy of
selected NFA.
Endocrine Abstracts (2007) Vol 14
BMP dependent effects on adrenal tumorigenesis and function
Inga Johnsen1, Sarah Kaufmann1, Lilia Spady1 & Felix Beuschlein2
Institute of Molecular Medicine and Cell Research, Albert-LudwigsUniversity Freiburg, Freiburg, Germany; 2Medical Clinic, University
Hospital Innenstadt, Ludwig Maximilians University, Munich, Germany.
Members of the TGFb family of ligands - including bone morphogenic proteins
(BMPs) - have been demonstrated to profoundly impact tumorigenesis in a
variety of tumor entities. As for the adrenal cortex, BMP6 has been implicated
as an important modulator of aldosterone secretion. To screen for alterations of
TGFß dependent pathways in adrenal tumorigenesis we performed gene
profiling experiments. By comparing human adrenal carcinoma (ACC) against
normal adrenal tissue samples (Co) we detected a down-regulation of various
BMPs (e.g. BMP2 and BMP5) which was further validated by Real Time
analysis (BMP5, ACC vs. Co 6.1G1.4% vs. 100G29.7%, P!0.01; BMP2,
ACC vs. Co 35.1G1.2% vs. 100G17%, P!0.01). As similar expression
pattern with loss of BMP5 expression was evident in NCIh295 cells, this cell
line was used as an in vitro model to assess potential impact of BMP
dependent pathways. Incubation with recombinant hBMP5 induced phosphorylation of SMAD 1/5/8 and subsequent increase of ID protein expression
levels in a dose dependent manner, while co-incubation with the physiological
BMP antagonist Noggin neutralized these effects. Thus, these findings
demonstrated the integrity of the pathway in NCIh295 cells. Notably, BMP5
treatment resulted in a decrease in cellular viability (68.3G1.1% vs. 100G
2.7%, P!0.01) but increase in the expression levels of steroidogenic enzymes
such as StAR (225G9.6% vs. 100G2.3%, P!0.01) and SCC (460.3G58.8%
vs. 100G0.53%, P!0.01). The BMP5 dependent reduced viability was
accompanied by concomitant changes in the cell cycle possibly through an
increased rate in apoptosis. Taken together, we demonstrate that loss of BMP
expression is a common finding in ACC. Moreover, we provide first evidence
that BMP dependent pathways might be involved in modulation of the
malignant phenotype of adrenocortical cancer.
9th European Congress of Endocrinology, Budapest, Hungary, 2007
RET mutation – Tyr791Phe – the genetic cause of different diseases
derived from neural crest
Eliska Vaclavikova1, Sarka Dvorakova1, Petr Vlcek2, Richard Skaba3,
Radovan Bilek1 & Bela Bendlova1
Dept. of Molecular Endocrinology, Institute of Endocrinology, Prague,
Czech Republic; 2Dept. of Nuclear Medicine and Endocrinology, 2nd
Faculty of Medicine, Charles University and Hospital Motol, Prague, Czech
Republic; 3Dept. of Pediatric Surgery, 2nd Faculty of Medicine, Charles
University and Hospital Motol, Prague, Czech Republic.
Familial medullary thyroid carcinoma (MTC), multiple endocrine neoplasia
types 2A and 2B (MEN2A, 2B) and Hirschsprung disease (HSCR) are
inherited neurocristopathies linked to germline mutations in the RET protooncogene. Activating germline RET mutations are presented in patients with
FMTC, MEN2A and MEN2B, on the other hand, inactivating germline
mutations in patients with HSCR. Nevertheless, there is an overlay in specific
mutations in the exon 10 of the RET proto-oncogene. The aim of this study
was to screen 6 exons (10,11,13,14,15 and 16) of the RET proto-oncogene by
fluorescent sequencing method in three different groups of patients - 174
families with MTC (including MEN2A, 2B), 73 families with HSCR and 20
patients with only pheochromocytoma. In this report, we show that the point
mutation Tyr791Phe in exon 13 of the RET proto-oncogene can cause
different diseases derived from neural crest. We found Tyr791Phe mutation in
5 families with MTC (3%), 2 families with HSCR (3%) and 1 family with
pheochromocytoma (5%). All these patients with the mutation have also
a silent polymorphism Leu769 (T/G) in exon 13. In addition, in 2 families
with MEN2 double germline mutations were detected: MEN2A family
Tyr791Phe C Cys620Phe (exon 10) and MEN2B family Tyr791Phe C
Met918Thr (exon 16). Tyr791Phe mutation had not been previously observed
in HSCR patients. Detection of Tyr791Phe mutation in MEN2/MTC and
HSCR families leads to a question whether this mutation has dual “Janus”
character (gain-of-function as well as loss-of-function) as mutations described
in exon 10 in HSCR/MEN2A patients. This study shows other character of
this strange and frequently discussed Tyr791Phe mutation. On the basis of our
genetic finding total thyroidectomy was recommended for all patients with
Tyr791Phe mutation.
The work was supported by IGA MZ CR NR/7806-3, GACR 301/06/P425
and IGA MH CR NR/8519-3 and was approved by local Ethical committee.
OC3.5 – ESE Young Investigator Award
[123I]Iodometomidate as a radiotracer for adrenal scintigraphy – first
clinical experience
Stefanie Hahner1, Andrea Stuermer1, Martin Fassnacht1, Michael Kreissl2,
Christoph Reiners2, Felix Beuschlein3, Martina Zink1, Ilse Zolle4,
Andreas Schirbel2 & Bruno Allolio1
University of Wuerzburg, Dept. of Endocrinology and Diabetology,
Wuerzburg, Germany; 2University of Wuerzburg, Dept. of Nuclear
Medicine, Wuerzburg, Germany; 3University of Munich, LMU, Division of
Endocrine Research, Munich, Germany; 4University of Vienna, LudwigBoltzmann-Institute of Nuclear Medicine, Vienna, Austria.
Adrenal masses are highly prevalent tumours comprising of a variety of
entities. Therefore, therapeutic consequences also vary considerably. The
CYP11B-specific PET-tracer [11C]metomidate has been shown to be suitable
to characterize adrenal lesions. However, its availability is restricted to
PET-centers with an on-site cyclotron. Also imaging is hindered by the short
tracer half-life (20 min). Therefore, we have developed [123I]iodometomidate
as a tracer for adrenal imaging. Pharmakokinetics and biodistribution after
i.v.-injection of 40 MBq of [123I]iodometomidate were analyzed in mice using
small animal single photon emission computed tomography (SPECT). A 49
year old woman with bilateral adrenal tumors (hounsfield units O10
suggesting a non-adenoma lesion) and borderline urinary catecholamines
(patient 1) and a 22 year old man after adrenalectomy for adrenocortical
carcinoma with a lesion suspicious for metastasis in the os sacrum (patient 2)
were investigated with [123I]iodometomidate-SPECT. Adrenals were excellently visualized in mice with high tracer uptake and little background
activity. In patients, adrenals were first detected 60 min p.i. with a maximum
uptake in the adrenals after 5–6 hours indicating slow pharmacokinetics of the
tracer. At 24 h.p.i. high uptake was detected exclusively in the adrenals. In
patient 1 both tumours exhibited high tracer uptake confirming the
adrenocortical origin of the lesions. In patient 2 the remaining hyperplastic
adrenal was clearly visible. However, no uptake was detected in the os
sacrum lesion. Subsequent biopsy revealed a periostal chondroma. For both
patients calculated whole body radiation exposure was 3.2 mSv. This is the
first description of [123I]Iodometomidate as a radiotracer in patients.
Iodometomidate is a highly suitable tracer combining specific uptake in
adrenocortical tissue with far lower radiation exposure compared to
norcholesterol scintigraphy. Availability and pharmacokinetics are superior
to [11C]metomidate-PET. Furthermore, radiotherapy of adrenocortical carcinoma using [131I]iodometomidate appears to be feasible.
ERß-specific transcriptional profile in colon cancer
Valentina Martineti1, Massimiliano Mascherini4, Carmelo Mavilia1, Silvia
Carbonell Sala1, Isabella Tognarini1, Chiara Azzari3, Federico
Mattia Stefanini4, Francesco Tonelli2 & Maria Luisa Brandi1
Department of Internal Medicine, School of Medicine, University of
Florence, Florence, Italy; 2Department of Clinical Physiopathology, School
of Medicine, University of Florence, Florence, Italy; 3Department of
Pediatrics, School of Medicine, University of Florence, Florence, Italy;
Department of Statistics, University of Florence, Florence, Italy.
Epidemiological data clearly evidence a protective role of estrogens against
the development of colon cancer and ERb has been identified as the
predominant ER subtype in human colon. More recently it has been identified
as a favourable prognostic marker in this disease, possibly explaining the
protective effect of estrogens against colon cancer development. To
understand the specific role and mechanism of action of ERb in colon
tumorigenesis we developed an in vitro engineered cell model through
transfection and cloning of HCT8 human colon cancer cell line for stable
over-expression of wild type human ERb (HCT8b8), providing the first direct
evidence that ERb plays an important role in colon cancer as a regulator of
cell proliferation through induction of G1-S phase transition arrest. To
investigate the molecular events underlying growth arrest we analyzed specific
ERb-regulated genes by comparing expression profile of HCT8b8 cells versus
its non-engineered counterpart using Agilent’s Human 1A Oligo Microarray
(V2) chips harbouring over 22,000 human genes and ESTs. A list of 189
reproducibly ERb-regulated targets, comprising 64 up-regulated and 125
down-regulated genes, emerged indicating that ERb over-expression heavily
affects different aspects of HCT8 cell function regarding both its intracellular
metabolism and relationship with the extracellular milieu. According to their
function, ERb-modulated genes have been grouped into 16 categories, our
interest for further validation (by quantitative real time RT-PCR and Western
blotting) focused on cell cycle and mitosis genes category and this technique
confirmed 50% of gene modulations. On the whole a trend to the slowing
down of the cell cycle is demonstrated and one of the up-regulated genes is
E4F transcription factor 1 (E4F1), which is already known to be an estrogenmodulated transcription factor. Two of their downstream targets are p21waf1
and cyclin E whose altered expression has already been documented in our
cell model. We hypothesize that E4F1- p21WAF1-cyclin E is an ERb specific
pathway in colon cancer cells.
Fasting insulin levels are predictors of colonic lesions in patients with
acromegaly: an observational, open, prospective study in 189 patients
Annamaria Colao1, Rosario Pivonello1, Mariano Galdiero1, Renata
S. Auriemma1, Diego Ferone2, Paolo Marzullo3 & Gaetano Lombardi1
Department of Molecular and Clinical Endocrinology and Oncology,
section of Endocrinology, University “Federico II” of Naples, Naples, Italy;
Department of Endocrine and Metabolic Diseases, University of Genova,
Genova, Italy; 3Section of Endocrinology, Auxologic Institute of Verbania,
Verbania, Italy.
Elevated insulin levels are correlated with colonic adenomas and carcinomas in the
general population. Patients with acromegaly are considered at high risk to develop
colonic lesions and have a high insulin levels. To evaluate the role of insulin levels
on colonic polyps (hyperplastic, adenomatous, single or synchronous) or
adenocarcinoma in acromegaly we designed this analytical, observational, open,
prospective, study enrolling 189 patients (100 women, 89 men, age 20–82 yrs)
undergoing pan-colonoscopy at diagnosis. Age, gender, estimated disease
duration, body mass index, GH and IGF-I levels, fasting glucose and insulin
Endocrine Abstracts (2007) Vol 14
9th European Congress of Endocrinology, Budapest, Hungary, 2007
levels, HOMA-index [R (resistance) and b (b-cell function)] were considered as
predictors. Colonic lesions were found in 74 patients (39.1%): hyperplastic polyps
in 31 (16.4%), adenomatous polyps in 24 (12.7%), both hyperplastic and
adenomatous polyps in 14 (7.4%) and adenocarcinoma in 6 patients (3.2%);
polyps were single in 22 patients (29.8%) and synchronous in 52 (70.3%). Colonic
lesions were positively correlated with patients’ age, insulin levels, HOMA-R and
HOMA-b (P!0.0001), negatively with GH levels (PZ0.006) but not with
estimated disease duration, IGF-I levels, BMI or glucose levels. Compared to
patients with normal glucose tolerance, patients with impaired glucose tolerance
had a prospective risk (RR) to develop colonic lesions 2 times higher (95% CI 1.2–
3.3) while those with diabetes 2.9 times higher (95% CI 1.8–4.6). Serum fasting
insulin levels were the strongest predictor of the presence of colonic lesions. The
best cut-off of insulin levels to predict the presence of colonic lesions was 20.6
mUI/liter [sensitivityZ73.8% (61.5–84%); specificityZ81.1% (72.5–87.9%);
positive predictive valueZ69.6%, negative predictive valueZ84.1]. The patients
with fasting insulin levels O20.6 mU/liter at the diagnosis of acromegaly had a RR
to develop colonic lesions 5.1 times higher than those with levels %20.6 mU/liter
(95% CI 3.1–8.5). In conclusion, high fasting insulin levels predict the presence of
adenomas and adenocarcinomas.
synthesis and release of growth hormone (GH) from the pituitary via the
activation of specific receptors. New data indicate that GHRH is also
produced in both extrahypothalamic brain areas and in peripheral tissues.
GHRH-receptor splice variants (SVs) have been found in several peripheral
normal and neoplastic human tissues and mediate effects on cell
proliferation and differentiation. At present, central non-endocrine effects
of GHRH in extra-pituitary brain tissues have not yet been characterised.
The aim of the present study was to investigate the effects of GHRH on cell
survival in rat adult hippocampal progenitor cells (AHP) and to study the
intracellular pathway involved. Cell viability was assessed by the Alamar
blue assay. RT-PCR was performed to detect the presence of GHRH
receptor mRNA. The results showed that GHRH receptor is expressed in
AHP cells. GHRH dose dependently increased cell survival on AHP cells
compared to control. After GHRH administration a significant increase of
cAMP levels analyzed by ELISA was observed, suggesting a GHRHinduced activation of cAMP pathway. Consistently, western blot analysis
showed a significant activation of Akt and ERK 1/2 survival pathway after
GHRH administration. Activation of these signalling pathways preceded
CREB phosphorylation, which plays an important role in the differentiation
and maturation of newborn neurons in hippocampus. In conclusion, this
study shows that GHRH has a protective effect on AHP cells. Moreover, in
these cells GHRH is able to activate the cAMP-CREB pathway. Akt and
ERK1/2 seem to be involved in this survival signalling. Thus, GHRH and its
receptor may play an important role for hippocampal progenitor cells
Neuroendocrinology basic – OC4
Organismal, cellular and molecular evolution of water balance
regulation in vertebrates: the amphibian hinge
Roger Acher, Jacqueline Chauvet & Yves Rouillé
University Paris VI, Paris, France.
Amphibia, through metamophosis, recapitulate the evolution of water homeostasis
from aquatic life to terrestrial one. Whereas the tadpole has the status of a freshwater
fish, the adult has developed a three osmoregulatory organ system, including kidney,
bladder and skin, for facing terrestrial dehydration. Amphibia have differentiated
epithelial hydroosmotic cells in each organ: principal cells in nephron collecting
duct, granular cells in urinary bladder, principal cells in ventral skin. These cells,
equipped with hormone receptors and effectors (aquaporins, ion channels, urea
transporter) are largely controled by neurohypophysial hormones. Each vertebrate
possesses two similar neurohypophysial nonapeptides. From the 13 peptides
chemically characterized in the laboratory, we have traced two main evolutionary
paralog lines: vasotocin (nonmammalian vertebrates) – vasopressin (mammals)
involved in osmoregulation, and isotocin (bony fish) – mesotocin (nonmammalian
tetrapods) – oxytocin (mammals) possibly implicated in reproduction.
Twelve amphibian species originating from Europa, North- and South-America,
Africa and Asia have been investigated. Neurohypophysial secretory granules have
been isolated from the neurointermediate pituitary by sucrose gradient centrifugation
and their components, purified by HPLC, identified by aminoacid sequencing and/or
coelution with synthetic peptides. Along with vasotocin ([Ile3]-vasopressin) and
mesotocin (([Ile8]-oxytocin), vasotocinyl-Gly (hydrin2) has been identified in all
species. This peptide results from a limited processing of the 141-residue
provasotocin. A 4-enzyme cascade operating in secretory granules on vasotocinylGly-Lys-Arg sequence leads usually to the alpha-amidated vasotocin but downregulation of the last amidating enzyme gives, in amphibians only, vasotocinyl-Gly.
Vasotocin and hydrin2 have different conformations and act on distinct receptors.
Whereas vasotocin shows a water (re)absorption activity in kidney, bladder and skin,
hydrin2 is devoid of antidiuretic activity and is more active than vasotocin on the
skin. Hydrin2 is twice more abundant in species living in arid countries. Evolution
has synchronized a new osmoregulatory organ (skin) with a new specific hormone,
making two hormones from a single precursor.
Growth Hormone-Releasing Hormone (GHRH) exerts protective effects
on adult rat hippocampal progenitor cells
Silvia Destefanis1, Inger Johansson2, David Aberg2, Riccarda Granata1,
Ezio Ghigo1 & Jorgen Isgaard2
University of Turin, Turin, Italy; 2Sahlgrenska University, Goteborg,
Growth hormone releasing hormone (GHRH) is a neuropeptide mainly
synthesised in the hypothalamus, known to exert a stimulatory effect on the
Endocrine Abstracts (2007) Vol 14
Absence of germline AIP mutations in early onset sporadic
Leonor Gomes1, Hugo Prazeres2, Isabel Paiva1, Cristina Ribeiro1,
Olinda Rebelo3, Teresa Martins2, Manuela Lacerda2 &
Manuela Carvalheiro1
Serviço de Endocrinologia, Diabetes e Metabolismo dos Hospitais da
Universidade de Coimbra, Coimbra, Portugal; 2Laboratório de Patologia
Molecular do Serviço de Anatomia Patológica do Centro Regional de
Oncologia de Coimbra do Instituto Português de Oncologia, EPE, Coimbra,
Portugal; 3Serviço de Anatomia Patológica dos Hospitais da Universidade
de Coimbra, Coimbra, Portugal.
The pathogenesis of pituitary tumours is still incompletely understood.
Somatotropinomas occur both sporadically and in the context of familial
syndromes, such as multiple endocrine neoplasia type 1 (MEN1), Carney
complex (CNC) and isolated familial somatotropinoma (IFS). Recently,
germline mutations were reported in AIP (aryl hydrocarbon receptor
interacting protein) gene in Finish and Italian families and in Finish
patients with apparently sporadic pituitary tumours. The aim of this study
was to determine if AIP gene mutations influence individual susceptibility to
develop sporadic pituitary somatotropinomas in a group of young patients
originating from the central region of Portugal.
Blood samples were obtained from 20 patients (8 males and 12 females)
with sporadic somatotrophinomas, including 6 plurihormonal for GH and
PRL, who were diagnosed when they were younger than 35 years of age
(mean age 25.7G4.97, 16-33 years). Detection of the AIP germline
mutations was carried out by PCR amplification of genomic DNA, followed
by direct sequencing of the entire gene coding sequence and intron-exon
boundaries as previously described.
In this series of patients, with early onset sporadic oversecreting-GH pituitary
adenomas, no AIP germline mutations were found. A heterozygous synonymous
C/T polymorphism (Asp45Asp) was found in a single patient.
Our results provide evidence that AIP germline mutations are not associated
with sporadic pituitary tumours. We studied patients diagnosed at young
ages, with a hypothetically higher probability of harbouring occult germline
mutations. The absence of germline mutations in this group of patients
suggests that AIP germline mutations probably do not play an important role
in the pathogenesis of sporadic pituitary somatotropinomas. Similar
observations have been made by other groups. Further studies are needed
in order to identify other genetic factors underlying early onset sporadic
pituitary tumours.
9th European Congress of Endocrinology, Budapest, Hungary, 2007
Is there a role for dopamine D2 receptor gene polymorphisms in
determining cabergoline sensitivity in prolactin-secreting pituitary
Marcello Filopanti, Anna Maria Barbieri, Rita Angioni, Andrea Lania,
Giovanna Mantovani, Anna Spada & Paolo Beck-Peccoz
Endocrine Unit, Dept. Medical Sciences, University of Milan; Fondazione
Ospedale Maggiore Policlinico IRCCS, Milano, Italy.
Metabolic abnormalities in patients with adrenal adenomas may be
associated with BclI polymorphism in the glucocorticoid receptor (GR)
gene and expression of tumor-specific hsp70 isoforms
Svetozar Damjanovic, Jadranka Antic, Bojana Beleslin, Sanja Ognjanovic,
Jovana Vignjevic, Milan Petakov, Djuro Macut, Ivan Paunovic,
Tatjana Isailovic, Bojana Popovic & Ivana Bozic
Institute for Endocrinology, Diabetes and Metabolic Diseases, Belgrade,
Dopamine agonist cabergoline (CB) is the first-choice treatment in prolactinsecreting adenomas (PRL-omas). It is effective in reducing PRL secretion and
tumour size in about 90% of patients by binding dopamine D2 receptor (DRD2).
Although no mutations in DRD2 were found, it has been reported that several
polymorphisms of this locus associate with alcoholism and schizophrenia,
diseases in which dopaminergic system plays an important role. To assess the
possible association of DRD2 gene polymorphisms (i.e. TaqIB, HphIG/T,
NcoIC/T and TaqIA) with the sensitivity to CB, a multicentric retrospective study
was carried out including 252 patients with PRL-oma and 211 healthy controls.
Genotyping was carried out by restriction fragment length polymorphism analysis
(RFLP) on blood DNA. Pituitary MRI and PRL assay were performed at
diagnosis and during CB therapy follow-up (median 17 months, range 5–49).
Patients were defined as resistant when they failed to normalize PRL levels and/or
to reduce tumor size with a CB dosage higher than 3 mg/week. According to this
definition, in our series the overall prevalence of resistant patients was 8% and
3.4%, respectively. As far as DRD2 genotypes were concerned, no differences in
allele frequencies between patients and normal subjects were observed.
Moreover, any polymorphism correlated with clinical presentation, biochemical
data and tumor size. Conversely, we observed an higher frequency of NcoITC
allele in subjects defined as resistant to CB in term of both normalization of PRL
levels [(c2)PZ0.038] and tumor size reduction [(c2)PZ0.006]. Finally,
[A1-/B1-/T-/T-] haplotype was found to be associated with a greater sensitivity
to CB in term of PRL normalization. In fact, this haplotype was found in 34% of
patients taking less of 3 mg/week of CB vs 11% of resistant patients [(c2)PZ
0.021]. In conclusion, further studies are required to assess the mechanisms
underlying the involvement of DRD2 gene polymorphisms in determining the CB
Lack of nuclear Hes1 expression coincides with transformation of
endocrine pancreatic cells in Men1 knock out mice
Térèse Johansson, Margareta Halin Lejonklou & Britt Skogseid
Institution of Medical Sciences, Uppsala, Sweden.
Homozygous inactivation of the MEN1 tumor suppressor gene frequently occurs
in endocrine pancreatic tumors (EPT); however, a heterozygous germ line
inactivation of the gene seems to lead to development of an increase amount of
endocrine pancreatic cells. The Notch signaling cascade plays a vital role in
sustaining the balance between cell proliferation, differentiation and apoptosis
during pancreatic development. Whether Notch signaling is MEN1 dependent is
To explore the Notch pathway by means of the transcription factors Hes1, Hey1
and Mash1 expression pattern and their role in endocrine tumour progression by
in Men1C/K mice.
Notch1, Hes1, Hey1, Mash1, and Men1 mRNA expression were investigated by
qPCR. Fifteen mice (10 Men1C/K, five Wt, 12 or 18 month,) were used; the
endocrine tissue was divided according to size: small islets, islets, small tumors
and larger tumors. Protein expression were assessed by immunohistochemistry
(13 Men1C/K and 12 Wt, 9–22 month)
Men1, Notch1, Hes1, and Hey1 mRNA expression was found in endocrine tissue
of all sizes; Mash1 was found in 28/55 samples. Variable degree of loss of menin
(the Men1 protein) expression was observed in tumors of Men1C/K mice age
14–22 month. Men1C/K and Wt mice showed no difference in Notch1, Hey1, and
Mash1 immunoreactivity. Wild type mice of all ages expressed nuclear Hes1,
whereas only the younger Men1C/K mice displayed nuclear Hes1 immunoreactivity. The tumors of the heterozygous mice age 14–22 month had lost nuclear
Hes1 expression.
Mash1 immunoreactivity was invariably and abundantly displayed. The lack of
Hes1 in tumor cell nuclei in elderly Men1C/K mice indicates that Hes1 might be
of importance in endocrine pancreatic tumorigenesis.
Intronic BclI polymorphism of glucocorticoid receptor (GR) gene and adrenal
adenomas of incidental discovery are frequently associated with metabolic
syndrome. We studied in these patients metabolic and hormonal parameters, the
sequence alteration in BclI polymorphism of the GR gene from constitutive DNA
and the expression of Hsp70 within the tumor and in tissue adjacently to tumor.
Patients and methods
We assessed 114 healthy subjects (79 men; age range 21–68 years) and 30
patients operated due to non-functioning adrenal mass (5 men; age range 36–76
years). Besides clininical and anthropometrical assessment, morning cortisol and
fasting insulin levels were determined. DNA was obtained from leucocytes and
after amplification, PCR fragments were digested with BclI enzyme.
Subsequently, the sequence of the fragments was analyzed. Equal amounts of
protein obtained from total cell lysates of adenomatous and adjacent normal
adrenal tissue was resolved by 9% SDS-PAGE and transferred to nitrocellulose
membranes (Western blot analysis).
We found a G-to-C transition in the second intron of GR gene in 24 of 26 (92%)
patients that is significantly higher frequency of the larger allele within patients
than in normal population (42% vs 4.2%; P!0.001). Patients and controls had
similar BMI and morning cortisol levels. However, the frequency of diabetes type
2, and hypertension were significantly higher in patients with adrenal tumor (PZ
0.002 for both) and these patients had significantly higher HOMA index than
controls (6.8G1.9 vs 2.9G0.1; P!0.001). In all tumor tissues two isoforms of
Hsp70 co-expressed while only higher molecular weight isoform was detected in
adjacent normal tissue.
Increased sensitivity to glucocorticoids associated with specific BclI polymorphism of GR gene and altered trafficking of GR by the Hsp90/Hsp70-based
chaperone machinery within adrenal adenoma seems to play role in the
development of insulin resistance in these patients.
Function and evolution of GHRH, PACAP and PRP in vertebrates
Billy KC Chow, Francis KY Siu, Janice KV Tam & Leo TO Lee
University of Hong Kong, Pokfulam, HK, SAR, China.
In mammals, GHRH is the most important neuroendocrine factor that stimulates
the release of GH from the anterior pituitary. In non-mammalian vertebrates,
however, the previously named GHRH-like peptides were unable to demonstrate
robust GH-releasing activities. In this report, we provide evidence that these
GHRH-like peptides are homologues of mammalian PACAP-related peptides
(PRP). Instead, GHRH peptides encoded in cDNAs isolated from goldfish,
zebrafish and African clawed frog were identified. Moreover, receptors specific
for these GHRHs were characterized from goldfish and zebrafish. These GHRHs
and GHRH-Rs are phylogenetically and structurally more similar to their
mammalian counterparts than the previously named GHRH-like peptides and
GHRH-like receptors. Information regarding their chromosomal locations and
organization of neighbouring genes confirmed also that they share the same
origins as the mammalian genes. Functionally, the goldfish GHRH activates
cAMP production in receptor-transfected CHO cells as well as GH release from
goldfish pituitary cells. Tissue distribution studies by real-time PCR showed that
the goldfish GHRH is expressed almost exclusively in the brain, while the
goldfish GHRH-R is actively expressed in brain and pituitary. In addition, specific
receptors for PRPs (formerly GHRH-like peptides) were cloned from goldfish,
zebrafish and Xenopus, clearly suggesting a function of PRP in these species. By
phylogenetic and chromosomal syntenic studies, we found PRP receptors only in
non-mammalian vertebrates but not in mammals, indicating that the receptor was
lost in the mammalian lineage. Based on these data, a comprehensive
evolutionary scheme for GHRH, PRP-PACAP, PHI-VIP genes in relation to 3
rounds of genome duplication early on in vertebrate evolution is proposed.
Finally, the newly discovered GHRHs, also found in flounder, Fugu, medaka,
stickleback, Tetraodon and rainbow trout, provide new research directions
regarding the neuroendocrine control of growth in vertebrates.
Endocrine Abstracts (2007) Vol 14
9th European Congress of Endocrinology, Budapest, Hungary, 2007
Thyroid basic – OC5
Structure-function of glycoprotein hormones using site-directed
mutagenesis and gene transfer: designing new agonists and antagonists
Fuad Fares, Naiel Azam, Rinat Bar-Shalom & Zaki Kraiem
Carmel Medical Center and the Faculty of Medicine, Technion-israel
Institute of Trechnology, Haifa, Israel.
The main goal of the present study is to investigate the role of N-linked
oligosaccharides on the structure and function of human thyrotropin (hTSH). A
second aim of the present study is to design new analogs of hTSH.
Overlapping PCR technique was used to convert hTSH heterodimer to a
biologically active single chain by fusing the a subunit to the carboxyl terminal
end of hTSHb subunit in the absence (hTSHba) or presence of a w30 aminoacid
peptide from hCGb (CTP) as linker (hTSHbCTPa). hTSH mutants lacking the
sequence site of N-linked oligosaccharides were prepared using site-directed
mutagenesis. hTSH variants were expressed in CHO cells. The TSH receptor
binding activities of the variants were determined by radioligand receptor assay
using CHO cells stably transfected with hTSH receptor. In vitro bioactivity was
tested using cultured human thyroid follicle cells and in vivo longevity and
bioactivity were tested in mice animal model.
The single-peptide variants of hTSH were biologic active in vitro and in vivo
with a longer half-life. Variants lacking the N-linked oligosaccharides were
expressed and secreted from CHO cells. Interestingly, the deglycoselated
variants were significantly less potent than TSH wild type. Moreover, the
deglycoselated variants blocked cAMP formation and T3 secretion stimulated
by hTSH or by hTSI in the receptor level. The variants were found to bind
the hTSH receptor with high affinity. In addition, deglycoselated hTSH
variants had a partial activity in vivo and significantly inhibited TSH
Human TSH single peptides are biologically active. Deglycosylated variants
inhibit the activity of hTSH and hTSI. These variants may offer novel therapeutic
strategies in the treatment of Thyroid diseases.
Tyroglobulin (Tg) depletion in receptor associated protein (RAP) KO
mice is due to a reduction of Tg aggregates
Simonetta Lisi, Roberta Botta, Aldo Pinchera, Claudio Marcocci &
Michele Marinò
Department of Endocrinology, University of Pisa, Pisa, Italy.
RAP KO mice have a reduction of colloidal Tg resulting in subclinical
hypothyroidism and histological signs of goiter. The difference in colloidal Tg
between RAP KO and WT mice was striking by immunohistochemistry, but
could not be detected in thyroid extracts. To explain this discrepancy, we
hypothesized that the reduction of Tg reflected a reduction of Tg aggregates
discarded during tissue extraction. To investigate this possibility, pellets
obtained by thyroid homogenization were solubilized with 6M guanidine and
analyzed by Western blotting. Tg resolved into two bands at 660 and
330 kDa, which were found in WT, but not in RAP KO mice, supporting a
reduction of Tg aggregates in the latter. We then investigated the effects of
detergents, denaturation and pH on homogenates separated into membraneassociated and cytoplasmic fractions. The Tg bands were detected in all
samples from RAP KO and WT mice. Detergents and high pH increased the
intensity of the bands in the cytoplasmic fractions from WT mice, suggesting
the presence of Tg aggregates of high molecular mass. Under denaturing
conditions the Tg bands were less intense, probably due to Tg degradation. In
RAP KO mice, cytoplasmic Tg was less sensitive to detergents and pH,
possibly because of a reduced number of Tg aggregates compared with WT
mice. Higher amounts of Tg were found in the membrane-associated than in
the cytoplasmic fractions, regardless of the extraction procedure and the
genotype, representing Tg-containing vesicles within the colloid, Tg within
intracellular organelles, and cell membrane-bound Tg. In RAP KO mice the
amounts of membrane-associated Tg were greater than in WT mice, in
agreement with immunohistochemical findings. In conclusion, the absence
of RAP in the thyroid gland results in a reduction of colloidal Tg aggregates,
which are known to represent the major storage form of thyroid hormones.
Endocrine Abstracts (2007) Vol 14
Polarized plasma membrane targeting of the NaC/IK symporter (NIS)
is regulated by its carboxy terminus
Orsolya Dohan2, Carla Portulano1, Chris Ginter1 & Nancy Carrasco1
Albert Einstein College of Medicine, Bronx, New York, United States;
Institute of Experimental Medicine Hungarian Academy of Sciences and
Szent Rokus Hospital and Institutions, Budapest, Hungary.
The NaC/IK symporter (NIS), a glycoprotein expressed at the basolateral
plasma membrane of thyroid epithelial cells, mediates active IK uptake for
the biosynthesis of thyroid hormones and radioiodide transport for diagnosis
and treatment in thyroid cancer. Our cloning of the NIS cDNA and generation
of anti-NIS antibodies provided the basis to investigate the decrease in IK
transport in thyroid cancer relative to healthy thyroid cells. Instead of finding
only the expected lower NIS expression, we have reported that in the
majority of thyroid cancers, NIS is surprisingly overexpressed as compared to
the surrounding tissue but retained intracellularly. Therefore, it is of
considerable interest to elucidate the mechanisms underlying NIS plasma
membrane targeting, a pursuit that could lead to new therapeutic interventions
to increase the sensitivity of radioiodide diagnostic imaging and the
effectiveness of radioiodide therapy. We report that the NIS carboxy terminus
contains crucial information for NIS trafficking and that the length of the
carboxy terminus correlates linearly with functional cell surface expression of
the transporter. We also demonstrate that whereas the last four amino acids
(E615TNL618) are not necessary for NIS trafficking, even though they
comprise a PDZ binding motif, the 602–614 sequence carries essential
determinants for NIS basolateral targeting.
BRAFV600E mutations but not RET/PTC rearrangements are correlated
with a lower expression of NIS mRNA expression in papillary thyroid
cancer (PTC)
Cristina Romei1, Pamela Piampiani1, Pinuccia Faviana3, Fulvio Basolo3,
Valeria Bottici1, Mariangela Sculli1, Piero Berti2, Gabriele Materazzi2,
Aldo Pinchera1 & Rossella Elisei1
Department of Endocrinology, University of Pisa, Pisa, Italy; 2Department
of Surgery, University of Pisa, Pisa, Italy; 3Department of Oncology,
University of Pisa, Pisa, Italy.
Several studies have identified a relationship between oncogene activation and
dedifferentiation of PTC. Mutations of RAS, RET/PTC and BRAF modulate
the expression of thyroid genes. An impaired NIS expression has been
demonstrated in PTCs harboring the BRAFV600E mutation.Aim of this study
was to analyze BRAF and RET/PTC1-3 alterations and their influence on the
expression of thyroid differentiation genes. Seventy-one PTC samples were
studied. Quantitative analysis of TPO, Tg, TSH-R, TTF1 and NIS were
performed by real time RT-PCR. Our results indicate that 44/71 cases (62%)
were positive for one genetic alteration and 7/71 (9.8%) showed the
simultaneous presence of 2 gene mutations. In particular BRAFV600E and
RET/PTC rearrangements were present in 32.2% and 19.7% of cases
respectively. BRAFV600E was more frequently found in the classical than in
the follicular variant (PZ0.02). At variance no correlation was identified
between RET/PTC rearrangement and clinico-pathological features of PTCs.
Genetic alterations were correlated with mRNA expression (DCt) of Tg, TPO,
TSH-R, TTF-1, NIS. mRNA expression of NIS gene was significantly lower
(PZ0.0001) in PTCs harbouring the BRAF mutation with respect to not
mutated samples. By immunohistochemistry we did not find any relationship
between BRAFV600E and NIS protein. No difference in NIS mRNA expression
was found in PTC with or without RET/PTC rearrangements. We did not
observe any significant difference in the expression of thyroid differentiation
genes neither when compared with BRAF mutation or RET/PTC rearrangements. Furthermore no relationship was found between serum TSH and the
expression of NIS mRNA in thyroid tumors. In conclusion our data indicate
that (a) the frequency of BRAFV600E mutations and RET/PTC rearrangements
was 35% and 20% respectively; (b) in our series 10% of PTC cases harbored
2 different genetic alterations; (c) NIS mRNA expression was significantly
lower in PTCs harboring a BRAF mutation but not a RET/PTC
rearrangement; (d) the expression levels of other thyroid differentiation
genes were not correlated with the presence of gene alterations.
9th European Congress of Endocrinology, Budapest, Hungary, 2007
Transcriptional regulation of human type 2 deiodinase and chorionic
gonadotropin genes in human placenta: emerging evidence of a common
promoter code
Gianluca Canettieri, Maria Giulia Santaguida, Antonella Franchi, Michele
Della Guardia, Alberto Gulino & Marco Centanni
University of Rome “La Sapienza”- Polo Pontino, Latina, Italy.
This work was supported by AMB Grant 3-50693L (to JM) and KBN Grant
2P05B01826 (to KK).
Human type 2 deiodinase (hD2) regulates T3 production in placenta during
trophoblast development. hD2 mRNA and protein levels are elevated only during the
first trimester of gestation then becoming barely detectable. These variations are
similar to those of chorionic gonadotropin (hCG), a well-known marker of early
gestation secreted by the cytotrophoblast. A peculiar promoter architecture of the
gene encoding the alpha subunit of hCG allows a CRE-mediated synergism between
cAMP and EGF, leading to elevated levels of hCG-mRNA only during early
pregnancy. In addition, hCG promoter contains several CCAAT boxes, that are likely
to confer tissue specificity to this gene. Similarly, in our previous studies we have
demonstrated that Dio2 promoter is synergistically stimulated by cAMP and
mitogens. These signals are integrated and converge to the Dio2 CRE, which recruits
a transcription factor complex including CREB, c-Jun and c-Fos. Here we show that
CCAAT enhancer binding proteins (C/EBPs), are master regulators of Dio2
expression in JEG3 cells, a cell line similar to early trophoblast. RT-PCR studies
have demonstrated that C/EBPs significantly increases hD2 mRNA levels. With
functional assays of micro-deletion mutant constructs we have shown that C/EBPs
robustly enhanced the transcriptional activity of hD2 gene through a highly
conserved CCAAT element, located nearby the TATA box. Biochemical evidence
confirmed the binding of C/EBPs to this regulatory site. Remarkably, the inducibility
was dramatically increased in promoter constructs lacking the CRE or when
CREB/CRE interaction was prevented by an acidic dominant negative inhibitor. This
latter observation suggested that CREB and C/EBP regulates transcription of Dio2
gene in an antagonistic fashion. In conclusion we have found that aCG and Dio2
genes seem to share a common promoter code, represented by CCAAT, CREs,
TATA/TSS units, that imparts tissue specificity and inducibility to both genes in
early trophoblast.
A crucial role of interleukin-6 in the pathogenisis of thyrotoxicosisrelated disturbances of bone turnover in mice
Janusz Mysliwiec1, Robert Zbucki2, Maria Malgorzata Winnicka2,
Boguslaw Sawicki3, Agnieszka Nikolajuk1, Karol Kaminski4,
Wlodzimierz Musial4, Piotr Mysliwiec5, Zofia Bondyra6, Jerzy Walecki6 &
Maria Gorska1
Dept. of Endocrinology, Diabetology and Internal Diseases, Bialystok,
Poland; 2Dept. of General and Experimental Pathology, Bialystok, Poland;
Dept. of Histology and Embryology, Bialystok, Poland; 4Dept. of
Cardiology, Bialystok, Poland; 5II Dept. of General Surgery, Bialystok,
Poland; 6Dept. of Radiology, Bialystok, Poland.
Interleukin-6 (IL-6) has been shown to be involved in the pathogenesis of several
bone diseases characterized by a negative balance between bone resorption and
The aim of the study was to estimate serum markers of bone turnover:
osteoclast-derived tartrate-resistant acid phosphatase form 5a (TRACP 5b) and
osteocalcin in IL-6 knock-out mice to assess the role of IL-6 in the pathogenesis
of thyrotoxicosis-related disturbances of bone metabolism.
Material and methods
C57BL/6J (wild-type; WT) and C57BL/6JIL6K/KKopf (IL-6 knock-out; IL6KO)
mice randomly divided into 4 groups with 10 in each one: 1/WT mice in
thyrotoxicosis (WT-thx), 2/WT controls (WT-ctrl), 3/IL6KO mice with
thyrotoxicosis (IL6KO-thx) and 4/ IL6KO controls. Experimental model of
hyperthyroidism was induced by intraperitoneal injection of levothyroxine. The
serum levels of TRACP 5b and osteocalcin were determined by ELISA.
Serum concentration of TRACP 5b (median and interquartile ranges) were
significantly increased in both groups of mice with thyrotoxicosis: WT (28.2
(18.8–41.6) U/l) and IL6KO (26.4 (23.0–31.2) U/l) as compared to the respective
controls. Osteocalcin serum levels in IL6KO-thx mice (111.9 (103.1–175.6)
ng/ml) were significantly elevated in comparison to WT-thx animals (46.1 (32.5–
58.9) ng/ml).
The results of the present study suggest that IL-6 plays a crucial role in
thyrotoxicosis-related disturbances of bone turnover in mice, determining the
imbalance between bone resorption and bone formation caused by excess of
thyroid hormones predominantly by inhibition of bone formation.
The 1188A/C polymorphism of IL-12 gene in Graves’ disease
Natalia Wawrusiewicz-Kurylonek, Maria Gorska, Janusz Mysliwiec &
Adam Jacek Kretowski
Department of Endocrinology, Diabetology and Internal Medicine, Medical
University of Bialystok, Bialystok, Poland.
Background and aims
Interleukin-12 (IL-12) is a pro inflammatory cytokine, which was suggested to
play a key role in the pathogenesis of Th1-cell-mediated autoimmune diseases.
The aim of our study was to estimate the association of 1188A/C polymorphism
of IL12B gene with the predisposition to Graves’ disease (GD) in Polish
Materials and methods
The study was performed in the group consisting of 245 individuals with GD
sequentially recruited from the endocrinology outpatient clinic. GD was
confirmed on the basis of clinical observation, biochemical criteria of
thyrotoxicosis and the presence of TSH receptor antibodies. Two hundred and
one healthy volunteers served as the control group. In all subjects A1188C
polymorphism in the 3 0 -UTR region of the IL-12B gene was determined by direct
sequencing of the appropriate fragment of IL-12B gene.
In our study the frequencies of 1188C allele and 1188CC genotype were significantly
higher in patients with GD in comparison to healthy subject (respectively, 22.1% vs.
16.2%, PZ0.027 and 7.7% vs. 1.5%, PZ0.003). There were no differences in the
distribution of 1188AA and 1188AC genotype IL-12B gene between the studied
groups. Furthermore we also observed that frequency of 1188CC genotype was
higher in patient with ophtalmopathy in comparison to subject without
ophtalmopathy and healthy controls. The frequency of 1188CC IL-12 genotype
was also higher among patients, who developed GD before the age of 40 years, when
compared to subjects with Graves’ disease onset before age of 40.
We observed that the frequency of 1188CC genotype of IL-12B gene is higher in
patients with GD and with ophtalmopathy in comparison to subject without
ophtalmopathy and healthy controls. This suggests that 1188A/C polymorphism in
IL-12B gene could have a role in predisposition to Graves’ ophthalmopathy.
Cardiovascular endocrinology – OC6
Growth hormone-releasing hormone prevents cardiomyocyte apoptosis
and activated PI3K/AKT, ERK1/2 and CREB signaling pathways
Riccarda Granata, Letizia Trovato, Silvia Destefanis, Fabio Settanni,
Marta Annunziata, Davide Gallo & Ezio Ghigo
Dept. Internal Medicine, Div. Endcocrinology and Metabolism, University
of Turin, Turin, Italy.
The hypothalamic hormone growth hormone-releasing hormone (GHRH), has
been shown to function via its receptor splice variants as an autocrine/paracrine
growth factor in normal and malignant cell lines and tissues, besides positively
regulating growth hormone (GH) synthesis and secretion from the pituitary.
Moreover, GHRH antagonists are known to suppress the proliferation of a wide
variety of cancer cells through mechanisms yet to be fully elucidated. Aim of this
study was to investigate the effect of GHRH on cell death and apoptosis induced
by either serum deprivation or by the b adrenergic agonist isoproterenol (ISO) in
rat H9c2 cardiomyocytes and in isolated adult rat cardiac myocytes. H9c2 cells
and cardiac myocytes were cultured in serum-deprived medium for 48 h in the
presence or absence of either ISO (100 mM) or GHRH (0.5 mM). RT-PCR
analysis revealed the presence of GHRH receptor (GHRH-R) mRNA in both
H9c2 cells and rat cardiac myocytes. GHRH (0.5 mM) significantly counteracted
serum starvation- and ISO-induced cell death and apoptosis in both cell models.
Further, either GHRH or isoproterenol induced ERK1/2 phosphorylation,
whereas only GHRH activated Akt survival signaling pathway. Interestingly,
both GHRH and ISO induced cAMP increase and phosphorylation of its downstream transcription factor cyclic AMP response element-binding protein (CREB)
in H9c2 cells. Finally, the GHRH-R antagonist JV-1-36 completely abolished the
survival effects of GHRH in H9c2 cells, under both serum starvation- and ISOinduced cell death and apoptosis.
Endocrine Abstracts (2007) Vol 14
9th European Congress of Endocrinology, Budapest, Hungary, 2007
These results indicate that GHRH is a survival factor for cardiac myocytes.
Moreover, they suggest that this molecule may play a role in the prevention of
cardiac cell loss in pathological conditions that ultimately lead to the development
of heart failure.
Testosterone replacement attenuates fatty streak formation and
improves the HDLC profile in the Tfm mouse: an effect which is
independent of the classical androgen receptor
Joanne E Nettleship1, Richard D Jones1, Kevin S Channer2 & Hugh T Jones1
Hormone and Vascular Biology Group, Academic Unit of Diabetes,
Endocrinology & Metabolism, Division of Genomic Medicine, University
of Sheffield Medical School, Beech Hill Road, Sheffield, S10 2RX, United
Kingdom; 2Department of Cardiology, Royal Hallamshire Hospital,
Sheffield Teaching Hospitals, NHS Trust, Glossop Road, Sheffield, S10 2JF,
United Kingdom.
Research indicates that low testosterone is associated with CAD in men. Evidence
suggests that men with hypotestosteronemia and concomitant CAD may benefit from
physiological testosterone replacement therapy (PTRT). The mechanism by which
testosterone produces these cardio-protective effects and the role of the androgen
receptor remains largely unknown. The aim of this study was to determine whether
testosterone modulates atheroma formation via its classical signalling pathway, via
conversion to 17b-estradiol or via an alternative-signalling pathway. Group 1:
8-week-old Tfm (exhibiting a dysfunctional androgen receptor and testosterone
deficiency) and control mice were castrated or sham-operated. Group 2: 9-week-old
Tfm and controls were administered either placebo, PTRT, PTRT in conjunction
with ERa-antagonist or Anastrazole. At 10-weeks both groups were administered a
cholesterol-enriched-diet. Mice were sacrificed at 28-weeks. Sections through the
aortic sinus were stained using oil-red-O, and lipid-stained areas quantified via digital
analysis, and expressed as percentage of medial area. Total cholesterol, HDLC,
testosterone and 17b-estradiol were quantified via ELISA. Low endogenous
testosterone was associated with fatty-streak formation following feeding on
cholesterol-enriched-diet. PTRT prevented aortic fatty streak formation in the Tfm
mouse, and increased levels of HDLC. Fatty-streak formation was less marked in
PTRT-treated mice, in conjunction with ERa-antagonist or Anastrazole, although
this was still significantly lower than that of placebo-treated Tfm mice. Improvement
in HDLC was completely attenuated by co-treatment with these agents. PTRT in the
Tfm mouse is associated with a reduction in aortic fatty-streak formation. The
majority of this action is due to a direct non-genomic action of testosterone, with a
component of the response being medicated via conversion to 17b-estradiol and
subsequent activation of ERa. The beneficial effect of PTRT upon HDLC appears to
be solely mediated by conversion of testosterone into 17b-estradiol, via modulation
of genomic ERa-dependent pathways.
Plasma brain natriuretic peptide (BNP) levels predict acute right
ventricular dysfunction in pulmonary embolism – prospective study on
70 patients
Alina Mihaela Pascu1, Mariana Rădoi2 & Mihail Coculescu3
“Transilvania” University, Faculty of Medicine, Department of Pathophysiology, Cardiology Clinic, Brasov, Romania; 2“Transilvania”
University, Faculty of Medicine, Department of Internal Medicine,
Cardiology Clinic, Brasov, Romania; 3“Carol Davila” University of
Medicine and Pharmacy, Department of Endocrinology, “C.I. Parhon”
Institute of Endocrinology, Bucuresti, Romania.
Acute right ventricular dysfunction (RVD) on echocardiography (ECHO) is
critical for risk stratification in pulmonary embolism (PE). Plasma BNP, a
consecrated marker of left ventricular dysfunction, could represent a valuable
biomarker of RVD in PE.
Aim and objective
Assessment of plasma BNP levels in patients with PE in relationship with right
ventricular (RV) function evaluated by ECHO.
Prospective study of 70 patients with confirmed PE, 42 men (60%), mean age
52.5G8.8. Plasma BNP levels were measured on admission using a quantitative
fluorescence immunoassay (Triage BNP). ECHO evaluation of the RV function
was performed in the first hour after admission. Study protocol was approved by
local Ethical Committee. Patients were divided in two groups: group 1 – with
Endocrine Abstracts (2007) Vol 14
acute RVD on ECHO, nZ24 patients (34.3%); group 2 – without acute RVD on
ECHO, nZ46 patients (65.7%).
SPSS 14.0; MedCalc 8.1.
Plasma BNP levels were significantly higher in patients with acute RVD on
ECHO (group 1), median value (25th, 75th percentiles)Z79.75 (45.77, 329.75)
pg/mL vs. 7.85 (6.22, 16.07) pg/mL in patients without acute RVD on ECHO
(group 2), P!0.0001. BNP proved good in discriminating between patients with
and without acute RVD – area under the receiver operating characteristic curveZ
0.86 (95% Confidence Interval C.I. 0.77–0.94), P!0.0001. The cut-off level of
plasma BNPZ50 pg/mL had the best sensitivityZ0.84 (95% C.I. 0.79–0.88) and
specificityZ0.80 (95% C.I. 0.75–0.85) in the same time in identifying acute
RVD. Plasma BNP correlated significantly with RV end-diastolic diameter (RZ
0.74, P!0.0001), RV systolic pressure (RZ0.77, P!0.0001). Logistic
regression analysis showed that plasma BN PO50 pg/mL was the best acute
RVD predictor, odds ratio 21.0 (95% C.I. 5.5–79.5).
Plasma BNP higher than a cut-off level of 50 pg/mL could predict acute right
ventricular dysfunction in patients with pulmonary embolism with a good
sensitivity and specificity.
Carotid IMT and stiffness, aortic stiffness and pulse pressure:
association with hormone therapy in postmenopausal women: baseline
findings from the CASHMERE trial
T Simon1, P Boutouyrie2, S Christin-Maitre1, A Gompel3, R Joanides4,
A Kearny-Schwartz5, Ch Kuntz6, S Laurent2, B Pannier7, B Pornel8,
HH Struijker-Boudier9, Ch Thuilliez4, L Van Bortel10, F Zannad5,
I Pithois-Merli11 & P Jaillon1
Saint Antoine-UPMC ParisVI university-Hospital, Paris, France; 2HEGPParis V-University Hospital, Paris, France; 3Hotel Dieu-Paris V-University
Hospital, Paris, France; 4CHU Rouen, Rouen, France; 5CHU Nancy, Nancy,
France; 6CHU Strasbourg, Strasbourg, France; 7Service de Cardiologie,
Fleury-Mérogis, France; 8Centre de Ménopause, Bruxelles, Belgium;
Cardiovascular Department, Maastricht, Netherlands; 10Cardiovascular
Department, Ghent, Belgium; 11Pfizer, Paris, France.
Common carotid artery intima media thickness (CCA-IMT), aortic stiffness (carotidfemoral pulse wave velocity-PWV) and central pulse pressure (PP) are early markers
of atherosclerosis. The influence of hormonal replacement treatment (HRT) on
arterial parameters in menopausal women remains to be investigated.
We used baseline data of 665 menopausal women with hypercholesterolemia,
screened for the CASHMERE study, a 12-month double-blind randomized trial
comparing the effects of atorvastatin (80 mg/day) versus placebo, GHRT, on the
progression of CCA-IMT. CCA-IMT, PP, PWV were measured by using a highdefinition echotracking device (Esaotw), aplanation tonometry (Sphygmocorw), and
Compliorw respectively. Mean age was 58G6 years with a mean duration of
menopause (M) of 8G7 years. Age at M was 50G5 years. Among them, 17% were
smokers, 23% had hypertension and 28% were HRTusers.
Age at M
(5 yrs)
M duration
(5 yrs)
Current use
of HT (yes)
Mean BP
(10 mmHg)
Central PP
(10 mmHg)
Total R2
CCA-IMT (mm)
Central PP (mmHg)
0.003 K0.3
0.002 K2.7
PWV (m/s)
R : % of explained variance, b coef: slope of the multivariate correlation.
Duration and age at menopause were associated with thickening and stiffening of
large arteries. Current users of HRT had significantly thinner and more distensible
arteries than non users.
9th European Congress of Endocrinology, Budapest, Hungary, 2007
Effects of ezetimibe and/or simvastatin on LDL receptor protein
expression and on LDL receptor and HMG-CoA reductase gene
expression in mononuclear blood cells: a randomized trial in healthy
Ioanna Gouni-Berthold, Heiner Berthold, Helena Gylling, Yon Ko,
Jogchum Plat & Wilhelm Krone
Department of Internal Medicine II, University of Cologne, Cologne,
Germany; Drug Comission of the German Medical Association, Berlin,
Germany; Department of Clinical Nutrition, University of Kuopio, Kuopio,
Finland; Medical Poliklink, University of Bonn, Bonn, Germany;
Department of Human Biology, University of Maastricht, Maastricht,
this group (PZ0.004). History of angina and prevalence of hypertriglyceridemia
was more frequent in the long repeat allele group (P!0.05). SHBG levels
correlated inversely with BMI and waist perimeter (P!0.05).
Longer (TAAAA)n repeats in the SHBG gene promoter are associated with more
severe CAD in women undergoing coronary angiography, a finding not previously
reported. This association may reflect the life-long tissue exposure to higher free
androgens and supports the adverse cardiovascular effect of androgenic exposure in
this highly selected group of women.
Ezetimibe and simvastatin are often used in combination to lower blood lipid
levels. The consequences of this combination at the molecular level are unknown.
To examine their effects on the LDL receptor (LDLR) protein expression and on
the LDLR and HMG-CoA reductase gene expression in peripheral blood
mononuclear cells (PBMC).
Design, setting and participants
Prospective, randomized, parallel 3-group trial. Twenty-four healthy men (mean
age 32G9 years) received a 14-day treatment with either ezetimibe (10 mg/day),
or simvastatin (40 mg/day) or their combination. Blood was drawn before and
after treatment.
Main outcome measures
LDLR protein expression, and LDLR and HMG-CoA reductase gene expression,
lipid levels, non-cholesterol sterols and the ratio of precursor sterols over
cholesterol concentrations, a valid marker of cholesterol synthesis and HMG-CoA
reductase activity.
LDL-C decreased by 22G10%, 41G12%, and 60G10% in the ezetimibe,
simvastatin and combination groups, respectively (all P!0.0001). The HMGCoA reductase gene expression increased significantly in the simvastatin (C33%;
PZ0.032) and combination groups (C36%; PZ0.0056) and remained unchanged
in the ezetimibe group (C14%; PZ0.27). Similarly, the LDLR gene expression
increased significantly in the simvastatin (C72%; PZ0.024) and combination
groups (C56%; PZ0.0012), but not in the ezetimibe group (C14%; PZ0.49). The
LDLR protein expression, however, remained unchanged in all groups.
Unlike simvastatin, the lipid-lowering effects of ezetimibe do not involve an
upregulation of the HMG-CoA reductase or LDLR gene expression. The
simvastatin-induced upregulation of the LDLR gene expression did not lead to
an increase in the LDLR protein. Further studies are necessary to fully clarify the
posttranscriptional mechanisms regulating LDLR protein abundance.
The importance of the TAAAA(n) alleles at the SHBG gene promoter
for the severity of cardiovascular disease in women
Katerina Saltiki2, Nectaria Xita3, Adriana Cimponeriu1, Ioannis Kanakakis2,
Emily Mantzou1, Charalambos Doukas2, Ioannis Georgiou3 &
Maria Alevizaki1
Endocrine Unit, Evgenidion Hospital, Athens University School of
Medicine, Athens, Greece; 2Dept Medical Therapeutics, Alexandra
Hospital, Athens University School of Medicine, Athens, Greece; 3Medical
Genetics Unit, Dept of Obstetrics and Gynaecology, Medical School,
University of Ioannina, Ioannina, Greece.
Androgen may be detrimental in the development of coronary artery disease
(CAD) in women. We investigated possible associations between the (TAAAA)n
polymorphism of sex hormone binding globulin (SHBG) gene promoter, which
influences transcriptional efficiency of the SHBG gene and the severity of CAD in
One hundred and twenty women (37–82 yrs), undergoing coronary angiography.
CAD severity, history of angina, myocardial infarction and reproductive history
were recorded and hormonal parameters measured. According to the number of
SHBG gene promoter repeats polymorphisms, patients were classified as short
(%7), medium length (Z8) and long repeat (R9) allele groups.
Significant CAD was more prevalent in the group with the long-repeat allele
carriers: 75% of the patients with 3 vessels with severe stenosis belonged to the
long repeat allele group while only 37% of patients with mild CAD belonged to
Evaluation of tolvaptan, an oral vasopressin V2 receptor antagonist, in
‘asymptomatic’ hyponatremia: effects on sodium concentration and
patient reported health outcomes
Peter Gross1, Joseph Verbalis2, Guy Decaux4, John Ouyang3, Mary Hobart3,
Cesare Orlandi3 & Frank Czerwiec3
Universitätsklinikum Carl Gustav Carus, Dresden, Germany; 2Georgetown
University, Washington, DC, United States; 3Otsuka Maryland Research
Institute, Rockville, MD, United States; 4Erasme University Hospital,
Brussels, Belgium; 5For the SALT Study Investigators, in Europe, Canada
and the, United States.
Hyponatremia (NaC%134 mmol/L), the most common electrolyte derangement, is
caused by inappropriate vasopressin-mediated water resorption in the kidney.
Treating symptomatic hyponatremia is difficult and risky; as difficult as maintaining
normal sodium levels. We tested if tolvaptan, an oral vasopressin V2 receptor
antagonist, improves hyponatremia and self-reported health outcomes.
Two multicenter, randomized, double-blind, placebo-controlled trials evaluated
tolvaptan in asymptomatic, non-hypovolemic hyponatremia patients. Upon
obtaining local Ethics Committee approval and patients’ consent, oral placebo
(nZ223) or tolvaptan (nZ225) was given for 30 days. The first single daily dose
(15 mg) was monitored in-hospital with optional fluid restriction. Patients were
discharged and fluid intake and study drug (30 or 60 mg) were titrated as clinically
indicated. Co-primary endpoints were the average daily area under the curve of
serum sodium concentration change from baseline to day 4 and 30. Overall SF-12
Physical (PCS) and Mental Component Summary (MCS) score changes from
baseline to day 30 were secondary endpoints. A hyponatremia disease-specific
survey (HDS) was also tested.
Serum sodium increased more with tolvaptan than placebo over the first 4 days
(P!0.001) and the entire 30-days (P!0.001). On stopping tolvaptan therapy,
sodium concentrations fell to placebo levels. The day 30 PCS was unchanged,
however the MCS was significantly improved in the tolvaptan group (PZ0.02).
MCS improvements correlated positively with rise in serum sodium (rZ0.2, PZ
0.001). Tolvaptan differed from placebo in the HDS survey in the moderately
severe hyponatremia subjects (!130 mmol/L) in mental concentration, calculation
and memory (P!0.05 or better). Side effects associated with tolvaptan included
increased thirst, dry mouth, and increased urination.
Tolvaptan, an oral V2 receptor antagonist, effectively increased and maintained
serum sodium concentrations in hyponatremic patients. These changes were
associated with improved perception of mental/cognitive health.
Reproduction 1 – OC7
Kallmann syndrome: mutations in the genes encoding prokineticin-2
(PROK2) and prokineticin receptor-2 (PROKR2)
Catherine Dodé & Jean-Pierre Hardelin
Institut Cochin, Paris, France.
Kallmann syndrome (KS) combines hypogonadotropic hypogona dism and
anosmia. Anosmia is related to the hypoplasia of the olfactory bulbs and tracts.
Hypogonadism is due to deficiency in gonadotropin-releasing hormone (GnRH),
and probably results from a failure of the embryonic migration of GnRHsynthesizing neurons. This is a genetically heterogeneous disease, which affects
1:8000 males and five times less females. Loss-of-function mutations in KAL1
and FGFR1 account for the X-chromosome linked form and an autosomal
dominant form of the disease, respectively. KAL1 encodes anosmin-1, a locally
restricted glycoprotein of embryonic extracellular matrices, which is likely to be
Endocrine Abstracts (2007) Vol 14
9th European Congress of Endocrinology, Budapest, Hungary, 2007
involved in FGF-signaling through FGFR1. Nearly 80% of the KS patients,
however, do not carry a mutation in either of these genes.
We considered the genes, encoding the PROKR2 and PROK2, most relevant
candidates because olfactory bulbs do not develop normally in prokr2K/K or in
prok2K/K mice. Prokr2K/K mice have a severe atrophia of the reproductive system
related to the absence of GnRH-synthesizing neurons in the hypothalamus. We
sought mutations in PROKR2 and PROK2 in a cohort of 192 unrelated individuals
affected by KS. Ten different PROKR2 mutations were detected in 14 patients in
heterozygous, homozygous, or compound heterozygous state, and heterozygous
PROK2 mutations were found in 4 KS patients. Notably, PROKR2 and PROK2
mutations were also present in some clinically unaffected individuals. These results
shed new light on the complex genetics of KS.
techniques. By 2 and 6 weeks of gonadotrophin suppression, the proportion of
TUNEL-labelled spermatogonia was increased to 354% and 268% of control (P!
0.001), respectively. The proportion of TUNEL-labelled spermatocytes was
increased (139% and 303% of control, respectively, not significant (NS)), with no
TUNEL-labelled spermatids being observed. No difference in the number of PCNAlabelled cells was observed in gonadotrophin-suppressed men compared to control.
By 2 and 6 weeks of gonadotrophin suppression, there was a trend that aCaspase 9
activity was increased to 130% of controls (NS), with no changes in aCaspase 8
activities. This study demonstrates for the first time that gonadotrophins act as
survival factors for the spermatogonial (and possibly spermatocyte) population,
possibly by regulating the intrinsic pathway of apoptosis. Understanding the
mechanisms by which germ cells progress may provide important clues in infertile
men where germ cells fail to progress due to hormonal pertubations.
(1) McLachlan et al. Journal of Clinical Endocrinology and Metabolism 2002
87: 546.
OC7.2 – ESE Young Investigator Award
Neuropilin-2 and its ligands are involved in the migration of GnRHsecreting neurons
Anna Cariboni2, Sonja Rakic1, Jason Hickok3, William Andrews1,
Shelley Tischkau3, Roberto Maggi2 & John Parnavelas1
University College London, London, United Kingdom; 2University of
Milan, Milan, Italy; 3University of Illinois at Urbana-Champaign, UrbanaChampaign, United States.
Capacitation and acrosome reaction in human ejaculated spermatozoa
involve activation of a novel SRC tyrosine kinase
Gabriele Varano, Adriana Lombardi, Gianni Forti, Elisabetta Baldi &
Michaela Luconi
University of Florence, Dept. Clinical Physiopathology, Florence, Italy.
Reproduction in mammals is centrally regulated by neuroendocrine neurons scattered
in the hypothalamus and secreting the decapeptide GnRH (gonadotropin releasing
hormone). During development, GnRH-secreting neurons originate in the olfactory
placode – at least in rodents – and migrate along olfactory nerves (the vomeronasal
and the terminalis) to gain access to the forebrain and reach their final destinations in
the hypothalamus. Defects in the migration of these neurons in humans result in
infertility. The mechanisms underlying the establishment of the migration route and
the movement of GnRH neurons are not very well understood and are thought to
involve different classes of molecules. Candidates comprise semaphorins and their
receptors (neuropilins) because of their high levels of expression in the developing
olfactory system, which is intimately related with the development of the GnRH
neurons. Moreover, reproductive problems and defects in the fasciculation of the
vomeronasal nerves have been reported in the mutant mice for Neuropilin-2 (Npn-2),
one of the class III semaphorins receptors, leading to investigate the role of these
molecules in the migration of GnRH neurons. Analysis of newborn Npn-2K/K mice
showed a significant reduction in number of GnRH neurons within the brain but an
abnormal presence of such neurons stacked in the nasal regions. Expression studies
performed on RNA derived from GFP-GnRH FACS-sorted cells showed presence of
Npn-1, 2 and their ligands (Sema3A, 3F), suggesting the importance of these
molecules in this system. In vitro experiments using immortalized GnRH neurons
(GN11) showed that semaphorins 3A and 3F inhibit their migration, whereas VEGF,
another Npn-2 ligand, reverted this effect, suggesting the possibility that in vivo the
migration of the GnRH neurons might be influenced by a balance between positive
(VEGFs) and negative (semaphorins) cues, acting through common receptors
(neuropilins). These findings provide new insights into the molecular mechanisms of
the migration of GnRH neurons and propose new candidate genes, likely involved in
the pathogenesis of hypogonadotropic hypogonadisms.
Tyrosine phosphorylation of proteins is one of the main processes associated with
the development of some specific functions of ejaculated human spermatozoa.
Although this process, as well as the identity of the phosphorylated targets, has
been well characterized, only few tyrosine kinases (TKs) have been identified so
far. Moreover, their roles in regulating sperm functions are still unknown.
In the present work, we report the presence and localization of Src kinase in
ejaculated human spermatozoa and investigate the role played by this TK during
capacitation. Immunoprecipitation and western blot analysis of protein lysates from
human spermatozoa using specific anti-p60src antibodies identified a single band of
about 70 kDa molecular weight. Immunofluorescence analysis of fixed and
permeabilized sperm localized positivity mainly in the post-acrosomal region of
sperm head and midpiece in over 80% of the sperm population. By both
immunoprecipitation and immunofluorescence techniques with antibodies recognizing tyrosine phosphorylation of Src at 416 or at 527 position, which identify the
active or inactive kinase respectively, we showed an increased phosphorylation in
Y416 during sperm capacitation. Blocking Src activity with its inhibitor SU6656
resulted in a significant reduction in tyrosine phosphorylation of sperm proteins, in
particular in the 80–115 kDa molecular weight range. Moreover, such inhibitor
completely blocked progesterone-induced acrosome reaction and interfered with
calcium response to progesterone evaluated in fura-2 loaded sperm. No effects on
sperm motility and hyperactivation parameters resulted from incubation of sperm
with SU6656. Finally, by the use of TK and PKA inhibitors (erbstatin A and H89,
respectively), we demonstrated that Src activation during capacitation is dependent
on tyrosine kinase but not on protein kinase A activity. In conclusion we identified a
novel Src isoform in human spermatozoa and demonstrated its involvement in
capacitation and acrosome reaction.
Gonadotrophins regulate germ cell survival, not proliferation, in
normal adult men
Saleela Ruwanpura, Robert McLchlan & Sarah Meachem
Prince Henry’s Institute, Clayton, VIC, Australia; Monash University,
Clayton, VIC, Australia.
Estrogens regulate epididymal contractility through RhoA/Rho-kinase
Sandra Filippi3, Annamaria Morelli1, Linda Vignozzi1, Rosa Mancina1,
Sara Mungai1, Stefano Ambrosini4, Gabriella Barbara Vannelli4,
Gianni Forti2 & Mario Maggi1
University of Florence, Department of Clinical Physiopathology, Andrology Unit, Florence, Italy; 2University of Florence, Department of Clinical
Physiopathology, Endocrinology Unit, Florence, Italy; 3University of
Florence, Interdepartmental Laboratory of Functional and Cellular
Pharmacology of Reproduction, Dept. of Pharmacology and Clinical
Physiopathology, Florence, Italy; 4University of Florence, Department of
Anatomy, Histology and Forensic Medicine, Florence, Italy.
Men with suppressed gonadotrophins, as induced by androgen-based contraceptive
treatment, exhibit a 70% reduction in germ cell numbers (1). The mechanisms by
which the germ cell populations are decreased are unknown. This study aimed to
quantify the amount of germ cell apoptosis and proliferation and to identify the
pathway(s) involved in gonadotrophin-induced germ cell loss in men. Testicular
tissues from normal fertile men that received no treatment or testosterone (200 mg
i.m. weekly) plus depot medroxyprogesterone acetate (300 mg i.m. once) for 2 or 6
weeks (nZ5/10 per group) to suppress gonadotrophins and consequently
spermatogenesis were used (1). Apoptosis and proliferation were identified by
TUNEL (a DNA fragmentation marker) and PCNA (a cell cycle marker) labelling
methods, respectively. Intrinsic and extrinsic apoptotic pathways were identified by
co-localisation of TUNEL-labelled germ cells with the pathway-specific proteins:
activated caspase (aCaspase) 9 and 8 by confocal microscopy. The proportion of cells
labelled and co-labelled by each method was quantified using stereological
Endocrine Abstracts (2007) Vol 14
Epididymis (epi) is a sex steroid-sensitive duct provided with spontaneous motility,
allowing sperm transport. We previously demonstrated that human epi expresses a
high abundance of mRNA for ER-alpha and ER-beta. We demonstrated that in epi
estrogens up-regulate either oxytocin (OT) responsiveness, acting at the receptor
level, and responsiveness to endothelin-1 (ET-1), another well-known stimulator of
epididymal motility. However, we did not find any significant change either at gene
or protein level in ET-1 and its receptors. Hence, other molecular effectors should
9th European Congress of Endocrinology, Budapest, Hungary, 2007
mediate the increased sensitivity to ET-1. In particular we hypothesized that
estrogens up-regulate some contractile effectors, such as RhoA/Rho-kinase pathway,
downstream to the ET-1 receptors. To investigate the effect of changing endocrine
milieu on RhoA/Rho-kinase pathway, we induced hypogonadism (hypo) in rabbits
with a single administration of a long-acting GnRH analog, triptorelin, and we
replaced weekly hypo rabbits with different sex steroids (Testosterone, T or estradiol
valerate, E2). After 8 weeks from GnRH analog administration, T plasma levels were
decreased and the relaxant effect of the Rho-kinase inhibitor, Y-27632 on ET-1 precontracted epididymal strips, was significantly decreased. T administration restored
T plasma levels, but not Y-27632 sensitivity in the epididymal strips. E2 not only
completely restored Y-27632 responsiveness but even amplified it, as indicating that
the RhoA/Rho-kinase calcium sensitizing pathway is up-regulated by E2.
Accordinly, real time RT-PCR studies, western blot and immunohistochemistry
analysis indicate that Rho kinase gene and protein was induced by E2 but not by T. To
verify whether endogenous estradiol is involved in the regulation of Y-27632
responsiveness, we treated intact rabbits with an aromatase inhibitor, letrozole.
Blocking aromatase activity abolished Y-27632 responsiveness in epi. In conclusion,
our results support the hypothesis that epi is a male target for E2, which regulates its
motility tuning up contractile hormones and local peptides responsiveness by
increasing RhoA/Rho-kinase signalling and therefore calcium sensitivity.
Serum anti-Müllerian hormone levels in men with normo- and
Frank Tüttelmann1, Nina Dykstra1, Axel PN Themmen2, Jenny Visser2,
Eberhard Nieschlag1 & Manuela Simoni1
Institute of Reproductive Medicine of the University, Münster, Germany;
Department of Internal Medicine, Erasmus MC, Rotterdam, Netherlands.
Anti-Müllerian hormone (AMH) has recently been evaluated as a marker for follicle
reserve and as a new marker for ovarian function in women. In the male, it is produced
in Sertoli cells (SC) in the testis. We evaluated serum levels of AMH as a marker of SC
function and male fertility by comparing normo- and oligozoospermic men.
Materials and methods
Serum levels of AMH were determined by enzyme immunoassay in two groups of
men with normal (nZ105) and reduced (nZ79) sperm concentration (above or below
20!106/ml). These data were retrieved from the institute’s database Androbaseq.
Significant differences (P!0.001) between the two groups were observed in sperm
concentration (58.6G37.9 in normo- vs. 9.1G10.6!106/ml in oligozoospermic,
meanGS.D.) and count (202.6G147.4 vs. 33.8G40.2!106) as well as in the
percentage of progressively motile sperm (50.6G7.0% vs. 40.8G13.9%),
percentage of normal morphology (12.3G5.1% vs. 7.2G4.7%) and testicular
volume (55.8G14.6 ml vs. 44.0G13.8 ml), which were all lower in the
oligozoospermic men as expected. Follicle-stimulating hormone (FSH) was higher
in this group (4.1G3.0 U/l vs. 7.0G7.2 U/l), AMH showed a trend towards lower
levels (7.7G4.8 ng/ml vs. 6.7G4.8 ng/ml, PZ0.06), but neither LH (3.6G1.9 U/l
vs. 4.0G2.2 U/l) nor testosterone (T, 15.2G5.1 nmol/l vs. 14.2G4.3 nmol/l) was
different between the groups. We found a significant (P!0.01) negative correlation
between AMH and FSH (rZK0.48), and relatively weak positive correlations with
sperm concentration/count (rZ0.44 and 0.39) and sperm motility (rZ0.35). By
contrast, in the normozoospermic men AMH correlated only very weakly with T and
free T (P!0.05, rZ0.21 and 0.22) but with no other hormone or semen parameters.
In contrast to normozoospermic men, AMH correlates with FSH and sperm parameters
in oligozoospermic men and might serve as a new marker for reduced SC function.
Use of atorvastatin, but not simvastatin in men with Type 2 diabetes is
associated with lower total testosterone levels with no effect on
bioavailable or free testosterone
Roger D Stanworth1, Dheeraj Kapoor2, Kevin S Channer3 & T Hugh Jones4
Academic Unit of Endocrinology, University of Sheffield, Sheffield, United
Kingdom; 2Department of Diabetes and Endocrinology, Barnsley Hospital
NHS Foundation Trust, Barnsley, United Kingdom; 3Faculty for Health and
Wellbeing, Sheffield Hallam University, Sheffield, United Kingdom;
Department of Cardiology, Sheffield Teaching Hospitals NHS Foundation
Trust, Sheffield, United Kingdom.
There is a high prevalence of low testosterone levels in men with type 2 diabetes
(DM2) and low testosterone predates the onset of DM2. Testosterone replacement
therapy for hypogonadal men with DM2 improves insulin sensitivity and
glycaemic control as well as reducing central obesity. This may lead to an
increase in biochemical assessment of hypogonadism in men with DM2.
Androgens and other steroid hormones are produced from cholesterol and it
has been postulated that treatment with HMG-Co-enzyme A reductase inhibitors
(statins) could decrease testosterone levels by reducing the availability of
cholesterol and/or inhibiting steroidogenesis. Low testosterone levels in men with
DM2, and the widespread use of statins in DM2 mean that any such effect would
be particularly important in this group.
We compared androgen status with statin use in a group of 355 Caucasian men
with DM2. Data was collected in year 2002–2003. In our group, 168 patients were
treated with statins (mainly simvastatin and atorvastatin) and 187 men were
untreated. There were no significant differences between treated and untreated
men in terms of glycaemic control, blood pressure or obesity. Statin use was
associated with lower total testosterone (TT) (PZ0.009) and SHBG (PZ0.005)
levels but bioavailable (BioT) and calculated free testosterone (cFT) were not
significantly reduced. ADAM hypogonadal symptom score was not affected.
Atorvastatin was associated with reduced TT (PZ0.006) and SHBG (PZ
0.005) compared with no treatment and there was an apparent dose response effect
with the lowest levels of testosterone seen in men treated with higher doses of
atorvastatin. Simvastatin did not cause a significant reduction in testosterone
or SHBG levels. Our study illustrates the importance of using measured or
calculated bioavailable or free testosterone in the assessment of hypogonadism in
men with DM2 treated with statins, particularly atorvastatin.
Neuroendocrinology clinical – OC8
Growth hormone response during OGTT: the impact of assay method,
gender and BMI on the estimation of reference values in patients with
acromegaly and in healthy controls
Ayman M Arafat1, Mathias Möhlig1, Martin O Weickert1, Frank
H Perschel2, Johannes Purschwitz1, Joachim Spranger1, Christian
J Strasburger3, Christof Schöfl1 & Andreas FH Pfeiffer1
Department of Endocrinology, Diabetes and Nutrition, Charité-University
Medicine Berlin, Campus Benjamin Franklin and the German Institute of
Human Nutrition, Berlin, Germany; 2Department of Clinical Chemistry and
Pathobiochemistry, Charité-University Medicine Berlin, Campus Benjamin
Franklin, Berlin, Germany; 3Department of Clinical Endocrinology,
Charité-University Medicine Berlin, Campus Mitte, Berlin, Germany.
Besides the measurement of IGF-1, GH suppression during OGTT to assess the
biochemical status in acromegaly is recommended. However, as a consequence of
the development of highly sensitive and specific GH assays a critical
re-evaluation of the criteria for the diagnosis and follow-up management of
acromegaly is mandatory. The aim of our study was to evaluate the betweenmethod discrepancies in GH determinations by different immunoassays
considering further confounders like age, gender, and BMI.
GH was measured during a 75-g OGTT in 10 controlled and 22 uncontrolled
acromegalics (12 men; age 31–62 years; BMI 21–30 kg/m2) and in 213 apparently
healthy subjects (66 men; age 20–76 years; BMI 19–62 kg/m2) using 3 different
assays (DPC Immulite 2000, Nichols and DSL-10-19100) that are calibrated
against recommended standard (IS 98/574). Ethical Committee approval was
There was a strong correlation between all assays (rZ0.72–0.994, P!0.0001).
However, the results obtained with DPC were, on average, 2.4-fold higher than those
obtained with Nichols and 11-fold higher than those obtained with DSL. GH-nadir in
controlled acromegalics was 0.98G0.26 mg/l (DPC) and 0.5G0.15 mg/l (Nichols),
whereas in those with an active disease was 7.98G1.7 and 4.5G1.2, respectively. In
controls, GH-nadir was 0.13G0.01 mg/l (DPC), 0.06G0.01 mg/l (Nichols) and
0.018G0.004 mg/l (DSL). Both basal and nadir-GH were significantly higher in
females than in males (DPC: 2.2G0.28 vs. 0.73G0.15 mg/L and 0.16G0.013 vs.
0.08G0.01 mg/L, P!0.001, respectively). Age, BMI and waist/hip ratio correlated
negatively with both basal and nadir-GH (rZK0.2, K0.32 and K0.48, P!0.01). In
multiple regression analysis age, BMI and waist/hip ratio were independent
predictors for both the basal and the nadir-GH (b-values ranging from K0.2 to K0.3
and K0.14 to K0.3, respectively).
Post-glucose GH-nadir values are assay-, gender-, age- and BMI-specific indicating
the need of individual cut-off limits for each assay.
Endocrine Abstracts (2007) Vol 14
9th European Congress of Endocrinology, Budapest, Hungary, 2007
OC8.2 – ESE Young Investigator Award
Effect of GH receptor antagonist pegvisomant on cardiovascular risk
and atherosclerosis in acromegalic patients resistant to somatostatin
Maria Cristina De Martino1, Renata S Auriemma1, Gregorio Brevetti2,
Mariano Galdiero1, Monica De Leo1, Gaetano Lombardi1,
Annamaria Colao1 & Rosario Pivonello1
Departments of Molecular and Clinical Endocrinology and Oncology,
Federico II University, Naples, Italy; 2Department of Internal Medicine,
Division of Cardiovascular and Immunological Sciences, Federico II
University, Naples, Italy.
Idiopathic central hypothyroidism: report of a human natural model of
congenital TRH receptor (TRHR) absence
Marco Bonomi1, Marta Busnelli1, Alba Pilotta2, Elena Prandi2,
Mario Maggi3, Fabio Buzi2, Paolo Beck-Peccoz1 & Luca Persani1
Dept. of Medical Sciences, University of Milan; Istituto Auxologico
Italiano IRCCS and Fondazione Ospedale Policlinico IRCCS, Milan, Italy;
Growth and Development Unit, Children’s Hospital, Brescia, Italy; 3Dept.
of Physiopathology, University of Florence, Florence, Italy.
Acromegaly is known to be associated to an increased cardiovascular risk, due
to the increased prevalence of glucose intolerance and dyslipidemia and
pre-atherosclerotic lesions. The aim of this study was to evaluate the effect of
treatment with the GH receptor antagonist pegvisomant on cardiovascular risk
and atherosclerosis in patients with acromegaly resistant to somatostatin
analogues. Twelve patients (4 m, 8 f, 28–58 yrs) and 24 sex-, age- and
BMI-matched controls entered the study. The patients were evaluated before
and after 18 months of treatment with pegvisomant at the dose of
10–40 mg/day. In all patients and controls, serum total, LDL and HDL
cholesterol, triglycerides, glucose, insulin and fibrinogen levels, total/HDL
cholesterol ratio and HOMA index, as well as common carotid intima-media
thickness (IMT) were measured and correlated with serum GH and IGF-I
levels. At baseline, increased GH and IGF-I levels were confirmed in all
patients. HDL-cholesterol were significantly lower (P!0.05) whereas
total/HDL-cholesterol ratio (P!0.001), glucose levels (P!0.05), HOMA
index (P!0.001) and fibrinogen levels (P!0.001) were significantly higher in
patients than controls. Moreover, maximal IMT were significantly higher in
patients than in controls (1.13G0.55 vs 0.69G0.1 mm; P!0.001). At
18-month follow-up, serum IGF-I levels were normalized in 9 (75%) patients
and significantly reduced in the remaining patients. Both serum glucose levels
(5.62G1.33 vs 4.86G0.73; P!0.05) and HOMA index (3.31G2.24 vs
1.10G0.22; P!0.05) were significantly decreased after treatment. A trend to a
decrease in maximal IMT (1.13G0.55 vs 0.96G0.16 mm) was also found after
18 months of treatment with pegvisomant. A significant correlation was found
between the changes in serum IGF-I levels and maximal IMT (P!0.05). The
results of the current study demonstrated that the treatment with pegvisomant
is able to improve the cardiovascular risk, especially through the improvement
of glucose tolerance, and prevent the progression of atherosclerosis in patients
with acromegaly resistant to somatostatin analogues.
Pituitary imaging abnormalities in patients with and without
hypopituitarism after traumatic brain injury
Harald J. Schneider1, Chiara G. Croce2, Ginevra Corneli2, Ezio Ghigo2,
Günter K. Stalla1 & Gianluca Aimaretti2
Internal Medicine/Endocrinology and Clinical Chemistry, Max Planck
Institute of Psychiatry, Munich, Germany; 2Division of Endocrinology and
Metabolism, Department of Internal Medicine, Turin, Italy.
Recent evidence shows that patients with traumatic brain injury (TBI) are at
substantial risk of hypopituitarism. However, the pathomechanisms are still not
completely understood. Little is known about the association of morphological
changes in the sella region with pituitary function in TBI. In this study, we
assessed morphological abormalities of the sella region in patients with TBI and
their relation to endocrine function.
We have studied MR or CT scans of 22 patients with TBI (17 men, 5 women,
age [mean C/K SD] 43.5C/K 10.6 years). Of these, 15 patients had some degree
of hypopituitarism.
We found abnormalities of the sella region in 80% of the patients with
hypopituitarism and 29% of those without hypopituitarism (PZ0.03). The most
common abnormality was loss of volume or empty sella, followed by
inhomogeneities, perfusion deficits, and lack of neurohypophyseal signal.
This is the first study to investigate the association of morphological alteration
and pituitary function in TBI. Our results indicate that pituitary imaging
abnormalities are more common in TBI patients with than without hypopituitarism. Possibly, necrosis and/or hemorrhage play a potential role in posttraumatic
Endocrine Abstracts (2007) Vol 14
Central Hypothyroidism (CeH) is a rare thyroid hormone production defect due to
an insufficient stimulation of a normal thyroid gland. Candidate genes for isolated
CeH include TSHb (several cases reported) and TRHR (only one case reported so
far). Here, we report the clinical and genetic studies in 2 males and 3 females
affected with isolated CeH with normal/low TSH levels (0.05–0.95 mU/L) and
low FT4 levels (3.6–4.6 pM). None of the patients was detected at neonatal
screening, but came to medical attention during childhood or even adulthood
(3–42 years). MRI alterations were detected only in one case (empty sella).
Ultrasound showed hypoplastic/normal thyroids. None of the patients presented
thyroid autoimmunity. In 3 subjects, TRH test showed absent TSH but normal
PRL responses but TSHb gene analysis was negative. The fourth patient
presented CeH associated with severe obesity and type 2 diabetes mellitus and a
normal TSH response to TRH. No mutations were identified in TRH as well as in
Leptin and LeptinR genes. The last case presented with growth delay at 11 years.
Absent TSH/PRL responses after TRH stimulation suggested TRH resistance. We
identified a C to T homozygous nonsense mutation in TRHR gene resulting in a
premature stop codon (R17X) and the production of a truncated receptor lacking
the 7 transmembrane domains. This is the 2nd patient with TRHR mutations and
represents a natural model of TRHR congenital absence associated with CeH and
absent/poor neonatal manifestations. Since TRH is considered to play an essential
role in postnatal adaptation to extrauterine life and maturation of thyroid axis, our
findings may challenge this view or uncover the possible existence of other TRHR
isoforms also in humans. The lack of mutations in 4/5 cases suggests the existence
of still unknown candidate genes for CeH.
Inoperable pituitary tumours treated with 90Y-DOTA-TATE – initial
Grzegorz Kaminski1, Norbert Szalus1, Grzegorz Zielinski1,
Zbigniew Podgajny1, Wojciech Zgliczynski2, Anna Kasperlik-Zaluska2,
Joanna Cyperling-Kaminska3 & Eugeniusz Dziuk1
Military Institute of Health Services, Warsaw, Poland; 2Medical Center of
Postgraduate Education, Warsaw, Poland; 3LIM Medical Center, Warsaw,
The patients with inoperable hormone - secreting pituitary tumours are treated
with cold somatostatin analogues, but it is not always effective. DOTA-TATE
preparation is a somatostatin analogue coupled with b (K) emitter 90 Y. The
efficacy of the treatment is based on excessive expression of somatostatin
receptors (SSTR) in these tumours.
The aim of the study
To assess the feasibility of treatment of pituitary tumours with 90Y-DOTA-TATE
Material and methods
Y-DOTA-TATE preparation was used in 4 patients with inoperable tumour: 3
patients with acromegaly and 1 with the Nelson’s syndrome. The presence of
SSTR was confirmed in scintigraphy with 99 mTc-HYNIC-TATE preparation
earlier. Both radiopharmaceuticals are produced by POLATOM – Swierk/Poland.
In 2 pts with acromegaly the dose was repeated twice. 1 pt with acromegaly and
1 pt with Nelson’s syndrome were treated with the 90Y-DOTA-TATE four times
(3.7 GBq per dose). The renal protection was provided by 10 hours infusion of
1000 ml 10% amino acids preparation with max. speed of 120 ml/h. The local
Ethical Committee approval has been obtained before the study.
There were no serious adverse events observed after 90Y-DOTA-TATE
treatment. An insignificant, transient decrease of thrombocytes and lymphocytes
was noted. In patients with the Nelson’s syndrome the ACTH serum
concentration decreased by 31%, in patients with acromegaly GH serum
concentration decreased by about 30–40%, and clinical improvement was
Y-DOTA-TATE radiopharmaceutic is feasible and promising in treatment of
inoperable pituitary tumours.
9th European Congress of Endocrinology, Budapest, Hungary, 2007
Improved glucocorticoid replacement therapy by a novel oral
hydrocortisone modified-release tablet
Stanko Skrtic2, Hans Lennernäs3, Anna Nilsson1,
Ragnhildur Bergthorsdottir1, Thomas Hedner2 & Gudmundur Johannsson1
Dept of Endocrinology, Sahlgrenska University Hospital, Goteborg,
Sweden; 2Dept of Clinical Pharmacology, Sahlgrenska Academy, Goteborg
University, Goteborg, Sweden; 3Dept of Biopharmacy and Pharmacokinetics, Uppsala University, Uppsala, Sweden.
Mortality rate in patients with primary and secondary adrenal insufficiency is
increased. A contributing factor could be the dose and the pattern of
glucocorticoid replacement therapy. Hydrocortisone administered twice or thrice
daily produces high serum peaks and low trough values in-between. A novel, once
daily, hydrocortisone modified release tablet with combined immediate and
extended release characteristics was developed.
The aim was to determine single-dose pharmacokinetics and dose-proportionality of oral 5 and 20 mg modified-release hydrocortisone tablets in healthy
Material and methods
Studies were performed with betamethasone suppression. The two first study days
were blinded and randomized between the 5 and 20 mg tablet in a fasting state and
the third was open with the 20 mg tablet taken 30 min after a high calorie, high fat
meal. The plasma samples were assayed using a validated (GLP) LC-MS/MS
method. The plasma pharmacokinetic variables were calculated using noncompartmental data analysis.
Results and discussion
The time to reach a clinically significant serum concentration of cortisol
(O200 nmol/L) was within 25 minutes and a peak of 400–450 was obtained
within 50 min after the 20 mg tablet. Serum cortisol levels remained above
200 nmol/L for around 6 h thereafter whereas all serum concentrations 18–24 h
after intake were below 50 nmol/L. In the fed state the time to 200 nmol/L was
delayed by 45–50 minutes. The 5 mg and 20 mg tablets produced almost
superimposable profiles.
This modified-release tablet allows for a once-daily administration producing a
near physiological serum cortisol profile. The time to clinically significant
cortisol concentrations was short and after the peak level a slow decline occurred
throughout the day allowing for a cortisol-free interval 18–24 hour after intake.
This new tablet for once-daily administration may help to improve compliance
and outcome in patients with adrenal insufficiency.
Adding the criteria of ACTH levels O4 pmol/l at 24 hours, the PPV of the
IDST increased to 100%. Conclusions: IDST is a reliable, simple and
accurate test for diagnosing hypercortisolism. Measuring cortisol levels before
and 24 h after 8 mg i.v. dexamethasone administration is required to
adequately diagnose patients with CS. ACTH levels at 24 h may increase
the test’s PPV. The sensitivity, specificity and PPV of the IDST are equal or
higher than those reported for other commonly used non-invasive tests.
Further studies are required to determine if IDST can discriminate effectively
between pituitary disease and EAS.
Signal transduction – OC9
OC9.1 – ESE Young Investigator Award
Investigation of the role of MRAP in the functional expression of the
melanocortin 2 receptor
Sadani Cooray, Lou Metherell, Mike Cheetham & Adrian Clark
William Harvey Research Institite, London, United Kingdom; Institute of
Ophthalmology, London, United Kingdom.
Mutations in the ACTH receptor (Melanocortin 2 receptor/MC2R) are
associated with Familial Glucocorticoid Deficiency/FGD. FGD is an
autosomal recessive disorder that results from ACTH insensitivity at the
adrenal cortex. However, only about 25% of FGD are caused by mutations
in the MC2R suggesting the genetically heterogeneous nature of the disease.
The transfection-mediated functional expression of the MC2R can only be
achieved in cell lines of adrenal origin implying that the receptor may
require an adrenal specific accessory factor/factors for functional expression.
The causative gene for FGD type 2 (normal MC2R) was identified in our
lab. It encoded a novel single transmembrane domain protein of unknown
function that we subsequently named MRAP (melanocortin receptor
accessory protein). We demonstrated that MRAP assists the MC2R to the
cell surface as determined by confocal microscopy on CHO and SKN-SH
cells. MRAP was also shown to play a role in the production of a functional
MC2R in these cell lines as was indicated by the enhanced cAMP response
to ACTH when co-transfected with MC2R and MRAP (Metherell L.A.,
et al., Nature Genetics 2005 37 166–170). The knockdown of MRAP
expression by transient transfection of MRAP siRNA (small interfering
RNA) duplexes in Y1 mouse adrenocortical cells resulted in a reduction in
MC2R signalling as determined by the significant decrease in cAMP when
stimulated with ACTH. The expression and function of MRAP was restored
in the clonal cell lines expressing mouse MRAP shRNAs by the transfection
of the human MRAP sequence. Co-immunoprecipitation studies showed an
interaction between MRAP and MC2R but not the other four melanocortin
receptors. The production of cAMP through MC1R, MC3R, MC4R and
MC5R was not enhanced in the presence of MRAP. In summary MRAP was
found to be essential for the functional expression of the MC2R.
A single intravenous bolus of dexamethasone for the diagnosis of
Cushing’s syndrome
Gabriel Munter1, Moriah Kirshner2, Rosler Ariel2, Shilo Shmuel1,
Leibowitz Gil2 & Glaser Benjamin2
Shaare Zedek Medical Center, Jerusalem, Israel; 2Endocrinology Service,
Hadassah-Hebrew University Medical Center, Jerusalem, Israel.
The diagnosis of Cushing’s syndrome (CS) is based primarily on diagnostic
tests evaluating the cortisol response to dexamethasone suppression. Tests
based on oral administration of dexamethasone may be compromised by poor
compliance. We evaluated the diagnostic accuracy of a novel intravenous
dexamethasone suppression test (IDST). The test is performed by intravenous
(iv) bolus injection of 8 mg dexamethasone, with blood cortisol determinations made before injection, then hourly during the first 6 h and finally at
24 h. ACTH is measured prior to dexamethasone injection and at 6 and 24 h
following injection. We performed a retrospective analysis of patients studied
for suspected CS in Hadassah, between 1994–2004. The study included 101
patients: 54 patients with pituitary CS, 22 with adrenal CS, 4 with ectopic
ACTH CS (EAS) and 24 in whom the diagnosis of CS was excluded. Patients
without CS showed rapid suppression of cortisol and ACTH that persisted for
24 hours. Patients with pituitary CS showed suppression of cortisol and
ACTH levels at 6 hours with subsequent escape at 24 hours. Patients with
adrenal CS or with EAS failed to suppress cortisol or ACTH levels. Using
60% suppression of blood cortisol at 24 h as the cutoff for the diagnosis of
CS, IDST had 94% sensitivity, 95% specificity and 98% positive predictive
value (PPV) for the diagnosis of CS. Similar results were obtained by using a
cortisol level of 200 nmol/l at 24 hours as the cutoff for the diagnosis of CS.
The human orexin receptor type 2 gene: Alternative promoters
determining tissue-specific expression and identification of alternate
splice variants and altered translational activities
Jing Chen & Harpal Randeva
University of Warwick, Medical School, Coventry, United Kingdom.
Orexins, acting via their receptors, are involved in the control of feeding,
sleep-wakefulness, arousal, neuroendocrine homeostasis and autonomic
regulation. However, the 5 0 structure and regulation of human orexin type
2 receptor (OX2R) gene remains is not known. We present original findings
regarding the 5 0 structural organization of the human OX2R gene and
identify four OX2R mRNA transcripts that differ in their 5 0 -untranslated
region (UTR). The four transcripts revealed that the three alternative exons
arise from alternative splicing. These exon 1 variants, arising from a single
OX2R gene, were distributed over a region of 29504 bp and designated as
exons 1A, 1B and 1C on the basis of their 5 0 to 3 0 order. In transfection
studies, different transcripts exerted cell-specific effects on mRNA, but
consistently reduced protein expression. Tissue-specific expression of these
transcripts in human tissues has been demonstrated by RT-PCR. We show
those 5 0 -flanking regions to exon 1A and exon 2, but not exon 1C, drive
alternative promoter activity in HEK-293 and SH-5YSY cells. Using
progressive deletion analysis, a proximal promoter region between K456
and K123 (relative to the translation start site) was shown to exhibit the
higher activities in HEK-293, SH-5YSY and NT2 cells. One CRE, GATA-2
Endocrine Abstracts (2007) Vol 14
9th European Congress of Endocrinology, Budapest, Hungary, 2007
and Oct-1 motif was identified within this region, which was responsible for
the stimulation both by Dibutyryil-cAMP (db cAMP) and phorbol12-myristate-13-acetate (PMA). Mutational studies demonstrated that these
motifs functioned co-operatively to stimulate hOX2R gene transcription.
Using the chromatin immunoprecipitation assay, we demonstrated that three
motifs bind to the region of hOX2R proximal promoter. These novel data
suggest that usage of alternate promoters, 5 0 -UTR and alternative splicing
may contribute regulatory mechanisms for tissue-specific expression of the
hOX2R gene.
Orexin-A inhibits glucagon secretion and proglucagon gene expression
Eva Göncz1, Carsten Grötzinger1, Marily Theodoropoulou2,
Bertram Wiedenmann1, Mathias Strowski1 & Ursula Plöckinger1
Charite, Medizinische Klinik mit Schwerpunkt Hepatologie, Gastroenterologie & Interdisziplinäres Stoffwechsel-Centrum/Endokrinologie und
Diabetes Mellitus, Campus Virchow-Klinikum, Berlin, Germany; 2Max
Planck Institut für Psychiatrie, München, Germany.
Background and aim
Orexin-A (OXA) increases insulin secretion and inhibits glucagon secretion,
suggesting a role in regulating glucose homeostasis. The effects of OXA
on pancreatic A-cells on the cellular level have not yet been demonstrated.
Aim of our study was therefore to characterise the underlying signal
transduction pathways and to study the OXA effects on proglucagon gene
The effects of OXA on glucagon secretion were evaluated using an in situ
perfused rat pancreas model and clonal pancreatic A-cells (InR1-G9). OXR1 expression in InR1-G9 cells was detected by western blot and
immunofluorescence. The effects of OXA on intracellular cyclic AMP,
AKT, PDK-1, CREB and EGR-1 were measured by ELISA and western
blots, intracellular calcium (Ca2C) by Fura-2. Proglucagon and Foxo1
mRNA levels were quantified by real-time PCR. Foxo1 was silenced using
short interfering RNA (siRNA).
Pancreatic A-cells express OX1R. OXA reduced glucagon secretion and
proglucagon gene expression. OXA decreased intracellular cyclic AMP and
Ca2C concentrations, and increased the phosphorylation of AKT und PDK-1.
PI-3 kinase inhibitor blocked the effects of OXA on proglucagon gene
expression. OXA reduced the expression and phosphorylation of CREB, and
EGR-1. Silencing of Foxo1 had no effects on basal proglucagon gene
expression; however the inhibitory effect of OXA on glucagon gene expression
was reversed.
We demonstrate for the first time the direct interaction of OXA with
pancreatic A-cells and identify cAMP/AKT/PDK-1 and Ca2C as intracellular
target molecules for OXA action. We identify transcription factors Foxo1,
CREB and EGR-1 as downstream targets for OXA signalling, suggesting a
role in mediating the inhibitory effects of OXA on glucagon gene
expression. We have now increasing evidence that OXA affects glucagon
Inhibition of glucagon secretion by OXA may have potential implication at
lowering hyperglucagonemia frequently encountered in type 2 diabetes.
Signalling and internalisation properties of corticotrophin-releasing
hormone (CRH) receptor type 2
Danijela Markovic, Hendrik Lehnert & Dimitris Grammatopoulos
Warwick Medical School, University of Warwick, Coventry, United
The family of urocortins (UCNs) exert important pathophysiological actions
in the control of peripheral homeostatic mechanisms, through activation
of the type 2-corticotropin releasing hormone receptor (CRH-R2).
Endocrine Abstracts (2007) Vol 14
This G-protein coupled receptor preferentially binds urocortins (UCN,
UCNII and UCNIII) than CRH. In most tissues, CRH-R2 activation leads
to increased cAMP production. In this study we used HEK293 cells stably
overexpressing recombinant CRH-R2b receptors to investigate intracellular
events controlling receptor functional activity and their potential link
to activation of distinct signalling cascades. Our results showed that agonistinduced CRH-R2b activation is followed by receptor endocytosis.
Interestingly, we identified important agonist-specific temporal differences
in receptor internalization kinetics; UCNII (a CRH-R2 specific agonist)
induced CRH-R2b internalization within 15 min whereas the weaker agonist,
CRH, induced CRH-R2b internalization only after 30–45 min of treatment.
The role of intracellular molecules involved in GPCR internalization
was also investigated. Confocal microscopy studies revealed that b-arrestin
and clathrin were recruited to the plasma membrane as early as 2 min
following UCNII treatment, and 5 min following CRH treatment. Furthermore, clathrin, but not b-arrestin, co-localize with the internalized receptor
in the cytoplasm. We also investigated agonist induced ERK1/2 activation;
both UCNII and CRH induced a transient ERK1/2 activation that returned
to basal within 30 min. Confocal microscopy studies showed that activated
ERK1/2 was uniformly distributed in the cytoplasm and nucleus. Receptor
internalization inhibitors (conconavalin A and MDC) as well as expression
of a dominant negative b-arrestin (319–418) markedly reduced UCNII
and CRH induced ERK1/2 phosphorylation. In conclusion, we provide
novel evidence of agonist-specific differences in the internalization
characteristics of CRH-R2b which involve recruitment to clathrin coatedpits and b-arrestin to the plasma membrane. Receptor transport to the
cytoplasm involves association with clathrin but not b-arrestin. This
mechanism appears to be crucial for activation of distinct signaling cascades
such as ERK1/2.
The third intracellular loop of human SST5 is crucial for receptor
internalization after SS28 stimulation
Erika Peverelli1, Giovanna Mantovani1, Andrea G Lania1,
Davide Calebiro1, Andrea1 Doni2, Sara Bondioni1, Paolo Beck-Peccoz1 &
Anna Spada1
Endocrine Unit, Dpt. of Medical Sciences, Fondazione Ospedale Maggiore
Policlinico Mangiagalli e Regina Elena IRCCS, University of Milan, Milan,
Italy; 2Istituto Clinico Humanitas, Rozzano, Milan, Italy.
Somatostatin (SS) is a widely distributed polypeptide that exerts inhibitory
effects on hormone secretion and cell proliferation by interacting with five
different receptors (SST1-SST5), that display important differences in tissue
distribution, coupling to second messengers, affinity for SS and intracellular
trafficking. SS analogues currently used in the treatment of acromegaly
inhibit hormone secretion and cell proliferation by binding to SST2 and 5.
Beta-arrestins have been implicated in regulating SST internalization but the
structural domains mediating this effect are largely unknown. The aim of
this study was to characterize the intracellular mechanisms responsible for
internalization of human SST5 in the rat pituitary cell line GH3. To this
purpose we evaluated by fluorescence microscopy SS28-mediated trafficking
of receptor fused to DsRed and beta-arrestin2 fused to GFP. To identify the
SST5 structural domains involved in these processes, we evaluated
progressive C-terminal truncated proteins, SST5 mutants in which serine
or threonine residues within the third cytoplasmic domain were mutated
(S242A, T247A) and a naturally occurring R240W mutant in the third loop
previously found in one acromegalic patient resistant to somatostatin
analogues. We tested the ability of these mutants to associate with betaarrestin2 and to internalize under agonist stimulation. The truncated mutants
are comparable to the wild-type receptor with respect to beta-arrestin
recruitment and internalization, whereas third cytoplasmic loop mutants
show a significantly reduced internalization and arrestin translocation upon
SS28 stimulation. Surprisingly, SST5 with both C-terminal truncation and
third loop mutation exhibits normal internalization and beta-arrestin
recruitment. Our results indicate SST5 third intracellular loop as an
important mediator of beta-arrestin/receptor interaction and receptor
internalization, while the role of the C-terminal tail would be to sterically
prevent beta-arrestin/receptor interaction in basal conditions. Further
elucidation of the molecular signals underlying SST5 intracellular trafficking
will provide a better understanding of its function during prolonged agonist
9th European Congress of Endocrinology, Budapest, Hungary, 2007
Somatostatin receptor subtype-2 and -3 – selective agonists inhibit
insulin secretion from INS-1 cells through modulation of the R-type
Ca2C channel
Stefan Mergler, Vandana Singh, Sylvia Zacharias, Bertram Wiedenmann,
Ursula Plöckinger & Mathias Strowski
Hepatology & Gastroenterology, Berlin, Germany.
Somatostatin (SST) inhibits insulin secretion from pancreatic B-cells through a
reduction of intracellular free calcium ([Ca2C]i). The influx of Ca2C is mediated
by voltage-operated Ca2C channels (VOCCs). The role of VOCCs of the R-type
(CaV2.3) in SST-mediated processes is unknown. Therefore, we designed a study
to identify SST-receptor subtypes (SSTR) in insulinoma cells (INS-1) and
characterize the role of the CaV2.3 in mediating the effects of SST in these cells.
The expression of SSTRs in INS-1 cells was detected by RT-PCR. The effects of
highly SSTR-selective agonists (SSTR-Ag) on cyclic AMP, insulin secretion and
[Ca2C]i were measured by ELISA, RIA and cell fluorescence imaging. VOCCs
were characterized by patch-clamp technique.
INS-1 cells express SSTR2 and SSTR3. SSTR2-selective agonist (SSTR2-Ag)
more potently reduced cyclic AMP production than SSTR3-Ag. SSTR2-Ag
transiently increased [Ca2C]i which then rapidly decreased below the basal.
Blockade of L- and R-type channels modulated [Ca2C]i changes in response to
SSTR2-Ag treatment. In contrast, SSTR3-Ag lowered [Ca2C]i after 30 min, only.
Blockade of R-type channels of cells treated with SSTR3-Ag less potently
influenced [Ca2C]i than SST or SSTR2-Ag. SST (EC50: 0.04 nM) and SSTR2-Ag
(EC50: 0.06 nM) more potently inhibited 20 mM glucose/10 nM exendin-4stimulated insulin secretion than SSTR3-Ag. The specific R-type channel blocker
SNX-482 more potently reduced the inhibition of insulin secretion by SST and
SSTR2-Ag as compared to SSTR3-Ag.
INS-1 cells express SSTR2 and SSTR3. SSTR2-Ag more effectively reduces
intracellular cyclic AMP-accumulation and insulin secretion than SSTR2-Ag.
Blockade of R-type Ca2C channels prevents SSTR2- and SSTR3-induced
inhibition of insulin secretion, suggesting that these agonists inhibit insulin
secretion through modulation of R-type channel activity.
Seven transmembrane receptors mediated actin cytoskeleton
rearrangement: comparison with constitutively active mutants of G
protein alpha-subunits
Alenka Hrovat, Robert Frangez, Azra Pogacnik & Milka Vrecl
Veterinary Faculty, University of Ljubljana, Ljubljana, Slovenia.
Reorganization of the actin cytoskeleton could coincide with the activation of
several seven transmembrane receptors (7TM receptors) (1). Stimulation of Rho
family members leads to rapid remodeling of the actin cytoskeleton and
subsequent stress fiber formation and certain 7TM receptors were shown to
induce Rho-dependent responses via heterotrimeric G-proteins. Ga12, Ga13 as
well as Gaq/11 can link 7TM receptors to RhoA activation. However, some
controversy exists over the exact role of Gaq/11 (2).
The study’s aim was to examine whether activation of the Gaq/11- and Gascoupled 7TM receptors involves changes in cell morphology and reorganization
of the actin cytoskeleton. Actin cytoskeletal organization was also monitored in
cells transfected with constitutively active mutants of Gprotein a-subunits and
compared with the receptor-mediated redistribution pattern. Autofluorescentlytagged b-actin (pEYFP-actin) was co-expressed together with receptor constructs
(neurokinin type 1 receptor (NK1-R) and b2adrenergic receptor, b2-AR)) or
constitutively active mutants of Gaq, Ga12, and Gas in the HEK 293 cells.
Evaluation of the autofluorescently-labeled actin filaments was performed with
the use of confocal microscope.
The acquired data shows that the Gaq/11-coupled NK1-R activation caused
changes in cell morphology, enhancement in the cortical actin signal and stress
fiber formation. After the activation of other Gaq/11-coupled receptors
comparable results were also observed. Furthermore, the presence of overexpressed constitutively active Gaq and Ga12 also lead to noticeable stress fiber
formation. In contrast, neither the b2-AR activation nor constitutively active
mutant of Gas caused any apparent changes in actin cytoskeleton status in the
HEK-293 cells. Based on these findings it could be assumed that only Gaq/11coupled receptors activation coincides with the robust changes in the actin
cytoskeleton organization.
1. Merrifield CJ. Trends in Cell Biology 2004 14 352–358.
2. Barnes WG, Reiter E, Violin JD, Ren XR, Milligan G, Lefkowitz RJ. Journal of
Biological Chemistry 2005 280 8041–8050
Obesity and metabolism – OC10
The selective neuronal deletion of cannabinoid type 1 receptor is still
able to provide resistance to diet-induced obesity
Cristina Cervino1, Daniela Cota2, Luigi Bellocchio1, Giacomo Mancini3,
Beat Lutz3, Giovanni Marsicano4, Renato Pasquali1 & Uberto Pagotto1
Endocrine Unit and CRBA Hospital S.Orsola-Malpighi, Bologna, Italy;
Psychiatry Department, Cincinnati, United States; 3Physiological Chemistry Department, Mainz, Germany; 4Avenir INSERM, Bordeaux, France.
It is well known that cannabinoid type 1 receptor (CB1) antagonist drugs may
reduce body weight and improve metabolic profiles in obese animals and
humans by a double mechanism: at first, targeting mesolimbic and hypothalamic
nuclei and, thereafter, peripheral organs involved in energy storage and
expenditure. However, it is still unknown which of these sites of action may
have a predominant role in the endocannabinoid effect on energy balance
regulation. To solve this question we generated a mouse line in which the CB1
coding region is flanked by two loxP sites (CB1f/f). By crossing this with mice
that express Cre recombinase under the control of the regulatory sequences of
the Ca2C/calmodulin-dependent Kinase IIa gene (CB1CaMKIIaCre mice), we
obtained CB1f/f;CaMKIIaCre mice in which CB1 receptor is deleted in all principal
neurons of the forebrains, including those at mesolimbic and hypothalamic level
modulating the positive incentive to palatable food and the orexigenic signals,
respectively. Here we show that adult male CB1CaMKIIaCre (n. 15 each group, age
16–21 weeks for each diet) were still statistically significant leaner than the wild
type littermates either undergoing standard diet or with high fat diet (40% kcal
given by fat). However, when cumulative food intake was investigated, adult
male CB1CaMKIIaCre mice did not show any statistically significant difference in
caloric intake as compared to wild types with both diets. These data seem to
indicate that other neuronal pathways may overcome the lack of the central CB1
orexigenic drive; on the other hand, it may suggest that CB1 may still play a
crucial role at cerebral level as a sensor of yet unknown peripheral signals
involved in energy homeostasis.
11beta-hydroxysteroid dehydrogenase type 1 (11beta-HSD1) mRNA
expression in liver of patients with non-alcoholic steatohepatitis
Sarah Konopelska1, Tina Kienitz1, Matthias Pirlich1, Jürgen Bauditz1, Paul
M. Stewart2, Herbert Lochs1, Christian J. Strasburger1 & Marcus Quinkler1
Internal Medicine, Center for Gastroenterology, Hepatology and Endocrinology, Charite Campus Mitte, Charite Universitaetsmedizin Berlin,
Berlin, Germany; 2Division of Medical Sciences, Institute of Biomedical
Research, University of Birmingham, Birmingham, United Kingdom.
Non-alcoholic fatty liver disease (NAFLD) is recognized as common liver
disorder that represents the hepatic manifestation of the metabolic syndrome
including visceral obesity, type 2 diabetes, insulin resistance and hyperlipidemia.
Non-alcoholic steatohepatitis (NASH) is the progressive form of liver injury with
the risk for progressive fibrosis, cirrhosis and end-stage liver disease. The
pathophysiology that leads to NAFLD and NASH is not well understood. We
hypothesize that an altered cortisol metabolism in the liver may be a pathogenetic
factor. Hepatic 11beta-HSD1 regenerates cortisol from its inactive metabolite
cortisone and requires NADPH as cosubstrate, which is supplied by hexose-6phosphate-dehydrogenase (H6PDH).
76 patients (29 men, 48 women) underwent liver biopsy due to elevated liver enzymes.
We quantified 11beta-HSD1 and H6PDH mRNA expression by real-time PCR with
18S as housekeeping gene using a BioRad iCycler. In addition, anthropometric
measurements and analysis of 24 hour excretion rates of glucocorticoids using gas
chromatographic-mass spectrometric (GC-MS) analysis were performed.
11beta-HSD1 mRNA expression correlated significantly (r2Z0.803; P!0.001) with
H6PDH mRNA expression. We detected a significant correlation between 11betaHSD1 mRNA expression and waist-to-hip ratio (r2Z0.211; P!0.05), but not to
urinary (THFC5alphaTHF)/THE ratio, total cortisol metabolite excretion, age or
BMI. No gender specific differences were seen in mRNA gene expression.
Endocrine Abstracts (2007) Vol 14
9th European Congress of Endocrinology, Budapest, Hungary, 2007
Our data suggest that 11beta-HSD1 gene expression highly depends on H6PDH gene
expression. Surprisingly, 11beta-HSD1 gene expression did not correlate with any
urinary glucocorticoid ratio showing the limitation of urinary analysis. In our
patient’s cohort a higher waist-to-hip-ratio (abdominal obesity) was associated with a
lower 11beta-HSD1 mRNA expression in the liver.
Selective leptin resistance within the brainstem of histamine deficient
Anna Földes, Veronika Márkus & Krisztina Kovács
Institute of Experimental Medicine, Budapest, Hungary.
Histamine is an important anorexic factor that suppresses food intake via hypothalamic
H1 receptors and increases energy expenditure by stimulating lipolysis. Mice with
targeted deletion of the key enzyme of histamine biosynthesis, histidine decarboxylase
(HDC-KO), are unable to synthesize histamine. These animals display a metabolic
phenotype with adult onset obesity, selective increase in visceral fat depots, impaired
glucose tolerance and hyperleptinemia. To test the possibility that changes in the
leptin-induced signal transduction pathways are responsible for leptin resistance in
histamine deficient mice, we have analyzed phosphorylation of signal transducer and
activator of transcription (STAT-3) a key component of leptin action in target cells.
Adult male, wild type and HDC-KO animals were injected ip with leptin and
phosphoSTAT-3 (Tyr 705) immunoreactivity was revealed 30 min after injection by
conventional avidin-biotin-peroxydase histochemical reaction and the number of
phosphoSTAT-3 cell nuclei was counted. Wild type mice display leptin-induced
phosphoSTAT-3-ir in the arcuate-, dorsomedial- and ventromedial nuclei in the
hypothalamus, in the midbrain as well as in the dorsal vagal complex (DVC) of the
brainstem. In histamine deficient mice, the distribution of leptin-responsive neurons
and the number of pSTAT-3 ir profiles within the hypothalamus was similar to those
seen in wild type animals. In contrast, cells in the dorsal vagal complex of HDC-KO
mice display significantly less phospho-STAT-3 -immunoreactivity than the wild type
controls in response to exogenous leptin. These data suggest that leptin action in the
brainstem, but not in hypothalamus, is specifically impaired in histamine-deficient
mice. Defects in leptin signaling in neurons within the DVC may contribute in the
pathogenesis of leptin-resistant obesity as well as in the inability of HDC-KO animals
to mobilize their energy stores.
Mice lacking CRF receptor type 1 (CRFR1) have reduced vulnerability
to diet-induced obesity
Yolanda Diz-Chaves1, Maud Monsaingeon1, Luc Penicaud2,
Daniel Ricquier3, Angelo Contarino1 & Antoine Tabarin1
Lab Nutrition et Neurosciences, Bordeaux, France; 2Lab Neurobiologie et
Metabolisme, Toulouse, France; 3Lab Metabolisme Mitochondrial, Paris,
Evidence has accumulated about the involvement of the CRF system in the
regulation of energy balance. The effects of CRF are mediated by two receptors:
CRFR1 and CRFR2. The role of the CRFR1 in the regulation of energy balance is
not well defined. To address this issue, adult male CRFR1 KO mice and WT
littermates were given low fat (LFD) or high-fat (HFD) diets for 4 months. Under
LFD no differences between genotypes were seen on body weight (BW) and
caloric intake. KO mice had lower fat mass (13.6G0.6% vs 19.1%G1.7; P!
0.01) and increased lean mass (26.0G0.4 g vs 23.9G0.6 g, P!0.01). During a
HFD, KO mice had similar intake of calories but gained only 10% of the fat mass
that the WT mice did, indicating a reduced feeding efficiency. 24-h locomotor
activity was similar between genotypes. Plasma FFA and Betahydroxybutyrate
levels in KO mice suggested increased fat oxidation and KO mice had a increased
expression of UCP 1 in BAT. Since CRFR1 deletion impairs the HPA axis
activity, KO mice were given 5 mg/ml of Cort (KO-Cort) or vehicule (KO-Veh) in
drinking water. After two weeks on HFD, BW increases in KO-Cort mice and
reached that of WT mice after 16 weeks. Cort supplementation decreased
biological markers of fat oxidation in KO-cort mice to the levels of WT mice. No
difference in muscle expression of enzymes involved in FFA oxidation was found
between groups. Conclusion: CRFR1 have constitutively reduced fat mass,
increased fat oxidation and BAT thermogenic activity resulting in a reduced
vulnerability to diet-induced obesity. The decreased vulnerability to HFDinduced obesity in CRFR1 KO mice seems to depend mainly of their
constitutively low corticosterone secretion.
Supported by Grants from ATC Nutrition, FRM and Conseil Régional
Restoration of signalling capabilities in total loss of function MC4R
Harald Brumm1, Florian Bolze2, Susann Friedel3, Anke Hinney3,
Martin Klingenspor2, Johannes Hebebrand3, Annette Grüters1 &
Heike Biebermann1
Charité Universitätsmedizin Berlin, Inst. Exp. Ped. Endocrinology, Berlin,
Germany; 2Phillipps-Universität, Inst. Biologie/Tierphysiologie, Marburg,
Germany; 3Rheinische Kliniken Essen, Universität Duisburg Essen, Klinik
für Psychiatrie und Psychotherapie des Kinder- und Jugendalters, Essen,
The melanocortin 4 receptor (MC4R) belonging to the large superfamily of
G-protein coupled receptors plays a crucial role in hypothalamic weight
regulation. In approximately 3–5% of investigated obese patients inactivating
MC4R mutations are the underlying molecular cause for early onset obesity.
Functional characterisation revealed for specific partial loss of function MC4R
mutations that restoration of receptor function is possible by usage of highly
potent MC4R analogs. The analogue NDP-a-MSH is capable to restore wild type
signalling in some cases of partial loss of function. However, for total loss of
function receptors this procedure is insufficient.
To prove functional restoration cell surface expression was determined by cell a
surface ELISA approach with N-terminal HA-tagged mutant MC4R. Signalling
was determined by cAMP measurement with radioisotope labelled adenine.
In the present study we set out to investigate the restoration of specific total loss of
function mutations by usage of bioactive agents. We are able to show that in
dependence of the location and the kind of the mutation a functional rescue is
possible to different degrees.
This study is the first to show that in vitro restoration of signalling properties in
total loss of function MC4R is possible.
Endocrine Abstracts (2007) Vol 14
3-Iodothyronamine (T1AM) is a novel modulator of metabolic rate and
glucose homeostasis
David K. Grandy, Katherine L. Suchland, Thomas M. Keck, Feifei Yan,
Show-Ling Shyng & Thomas S. Scanlan
Oregon Health & Science University, Portland, Oregon 97239, United
3-Iodothyronamine (T1AM) is a novel endogenous derivative of thyroid hormone
(TH), recently described by Scanlan et al. (Nat. Med. 10: 638, 2004). In vitro,
T1AM can stimulate the production of cAMP via activation of a heterologously
expressed G protein-coupled receptor (GPCR) now referred to as trace amineassociated receptor 1 (TAAR1; Lindemann et al. Genomics 85: 372, 2005). In
adult, unanesthetized C57Bl6/J mice, T1AM produces profound and long-lasting
anergia, bradycardia, hypophagia, and hypothermia (K10 8C @ TambiZ24 8C). In
an effort to better understand these manifestations of T1AM, we evaluated its
effect on metabolic rate. In addition, experiments were performed to characterize
T1AM’s effect on blood sugar and the pancreatic hormones glucagon and insulin.
Finally, the effect of T1AM on an in vitro cellular model of glucose-stimulated
insulin release was investigated. Within minutes of its injection (i.p.) into male
mice housed at TambZ22 8C, and prior to the development of hypothermia, T1AM
(25 mg/kg) reversibly depressed metabolic rate w50% of vehicle-injected
controls, as measured by oxygen consumption (ml/g/min). Also within minutes,
T1AM dose-dependently elevated blood sugar, reaching a maximum of
w320 mg/dL, almost 3 times normal, by 3.5 hrs post injection. By 2 hrs postinjection, T1AM had produced a dose-dependent increase in circulating glucagon
(w400 pg/ml) that was nearly twice the vehicle controls. Furthermore, T1AM
(50 mg/kg) administered to fasted mice (26 hrs) prior to their receiving a bolus of
D-glucose (3 g/kg, i.p.) blocked the sugar’s ability to stimulate circulating insulin
levels compared to vehicle-treated mice. Finally, in vitro studies revealed T1AM
could dose-dependently prevent glucose-stimulated insulin release from cultures
of rat INS1823/13 insulinoma cells. Taken together, these results support the
thesis that T1AM is a rapid-acting novel modulator of metabolism with actions
opposite in direction to those of TH. As such, T1AM and its related compounds
may signal via one or more GPCRs to fine-tune TH’s effects and thereby help the
organism efficiently meet its metabolic needs minute-to-minute.
9th European Congress of Endocrinology, Budapest, Hungary, 2007
Serum level of retinol binding protein 4 in obese individuals with insulin
resistance and with type 2 diabetes mellitus treated by metformin
Mária Tajtáková1, Zuzana Semanová1, Gabriela Ivancová2,
Jozefı́na Petrovicová3, Viera Donicová2 & Eva Zemberová4
1st Department of Internal Medicine, University of P.I.Šafárik, Košice,
Slovakia; 2Department of Diabetes, Košice, Slovakia; 3Institute of Medical
Informatics, University of P.I. Šafárik, Košice, Slovakia; 4RIA Laboratory,
Košice, Slovakia.
To reveal whether there are differences in serum level of retinol binding protein 4
(RBP4) in obese individuals with insulin resistance (IR) and without diabetes in
comparison to those with 2 type diabetes mellitus (2 DM) treated by metformin
and not obese controls.
The serum level of retinol binding protein 4 was examined by RIA method in 28
obese individuals with insulin resistance, 11 patients with 2 type diabetes mellitus
treated by metformin and 17 controls. The results were compared within groups.
RBP4 in the group with IR and in controls was correlated with insulin.
The highest level of RBP4 (561.6G209 ng/ml) was found in obese individuals
with IR (IRHOMA 3.9) and the lowest level in patients with 2 DM treated by
metformin (391.1G133.5 ng/ml, P!0.01). The controls had significantly lower
level of RBP4 in comparison to obese individuals with IR (452.8G104.6 ng/ml
P!0.05), however, RBP4 was not significantly higher in comparison to obese
individuals with 2 DM treated by metformin (391.1G133.5 ng/ml). RBP4
correlated with insulin (rZ0.46, P!0.03).
The increase of RBP4 in obese individuals through a back regulation GLUT4 in
adipocytes contributes to the development and worsening of IR. Thus, metformin
by influencing the expression of RBP4 in adipocytes can improve the overall
insulin sensitivity in obese individuals (also with MS) and slower the
manifestation of 2 DM. RBP4 could be considered as a marker of the worsening
tolerance of glocose in obese individuals.
Reproductive Endocrinology 2 – OC11
Hypogonadotrophic hypogonadism in mice lacking a functional Kiss-1
Xavier d’Anglemont de Tassigny1, Mark Carlton2 & William Colledge1
PDN, University of Cambridge, Cambridge, United Kingdom, 2Paradigm
Therapeutics Ltd, Cambridge, United Kingdom.
Activation of the G-protein coupled receptor GPR54 (AXOR12, OT7T175) by
peptide ligands (kisspeptins) encoded by the Kiss-1gene is central to acquisition of
reproductive competency in mammals. Administration of exogenous kisspeptins
stimulates GnRH release from hypothalamic neurons in several species including
humans. To confirm that kisspeptins are the natural agonist of GPR54 in vivo and to
determine if these ligands have additional physiological functions, we have
generated mice with a targetted disruption of the Kiss-1gene. Kiss-1 null mice are
viable but fail to undergo sexual maturation at puberty. Mutant female mice do not
progress through the oestrus cycle, have thread-like uteri, small ovaries and do not
produce mature Graffian follicles. Mutant males have small testes and spermatogenesis arrests mainly at the early haploid spermatid stage. Both sexes have low
circulating gonadotrophin (LH and FSH) and sex steroid (b-estradiol or testosterone)
hormone levels. Migration of GnRH neurons into the hypothalamus appears normal
with appropriate axonal connections to the median eminence and total GnRH
content. The hypothalamic-pituitary axis is functional in these mice as shown by
robust LH secretion after peripheral administration of kisspeptin-10. These data
provide the first direct proof that kisspeptins are the true physiological ligand for the
GPR54 receptor in vivo and that loss of Kiss1 cannot be overcome by compensatory
Leukemia inhibitory factor promotes the chemomigration of immature
GnRH neurons
Elena Dozio1, Massimiliano Ruscica1, Anna Cariboni1, Hajime Watanobe2,
Marcella Motta1, Roberto Maggi1 & Paolo Magni1
University of Milan, Milano, Italy; 2University of Health and Welfare,
Otawara, Japan.
Leukemia inhibitory factor (LIF), a pleiotropic cytokine of the interleukine-6
superfamily, is involved in several functions including the control of
reproduction at the embrionic-endometrial interface and the regulation of
energy homeostasis. LIF activates a cell-surface receptor complex (LIF-Rs)
composed of one ligand-specific low affinity LIF receptor b (LIFRb) subunit
and the gp130 subunit. Since little is known about the involvement of LIF in
the modulation of the neuroendocrine circuitry governing the reproductive
function and, specifically, of the migration of gonadotrophin releasing-hormone
(GnRH) neurons from the olfactory placode to the hypothalamus, we tested
whether LIF could exert a chemoattractant or chemotropic action on GN11
immortalized cells, an in vitro model of immature and migratory GnRH
neurons. GN11 cells were found to express LIFRb and gp130 genes and
proteins. Exposure to 100 ng/mL LIF activated the Janus kinases (Jak)-signal
transducer and activator of transcription 3 (STAT3), the mitogen-activated
protein kinase (MAPK)-extracellular regulated kinase 1/2 (ERK1/2) and the
phosphatidylinositol 3-kinase (PI3-K)-Akt pathways. The selective inhibition of
Jaks, MEK, and PI3-K indicated that in GN11 cells the three signalling
pathways were activated independently and that Jak2 is not the main Jak
involved in LIF signalling. LIF stimulated chemotaxis at a concentrationdependent manner, with a plateau at 100 ng/mL after both 3 and 20 h of
incubation. A 3-h treatment with 100 ng/mL LIF also induced chemokinesis.
All the three signalling pathways activated by LIF in GN11 cells were
independently involved in LIF-induced cell migration. In conclusions, the
present results indicate that LIF promotes the chemomigration of immature
GnRH neurons, and suggest that LIF may modulate the development of the
reproductive axis by directly influencing the migration of GnRH neurons to the
Sex steroid and leptin regulation of KISS1/GPR54 system, a new
regulator of the neuroendocrine reproductive axis, in human fetal
GnRH-secreting neurons
Annamaria Morelli1, Mirca Marini2, Rosa Mancina1, Linda Vignozzi1,
Anna Pezzatini3, Michaela Luconi3, Sara Mungai1, Benedetta Fibbi1,
Sandra Filippi4, Gabriella Barbara Vannelli3, Gianni Forti3 & Mario Maggi1
University of Florence, Dept. Clinical Physiopathology, Andrology Unit,
Florence, Italy; 2University of Florence, Anatomy, Histology and Forensic
Medicine, Florence, Italy; 3University of Florence, Dept. Clinical
Physiopathology, Endocrinology Unit, Florence, Italy; 4University of
Florence, 2Interdep. Lab of Functional and Cellular Pharmacology of
Reproductio, Florence, Italy.
The molecular mechanisms underlying the reawakening of hypothalamic
GnRH neurons at puberty remain to be elucidated. Recently, the G proteincoupled receptor 54 (GPR54) and its endogenous ligand kisspeptin, encoded by
the KISS1 gene, have been involved. In fact, GPR54 mutations cause
idiopathic hypogonadotropic hypogonadism in human and mice. We used the
previously characterized primary culture of human fetal olfactory GnRHsecreting neurons, FNC-B4, to study in vitro the KISS-1/GPR54 regulation.
Kisspeptin and GPR54 were immunolocalized in fetal olfactory mucosa, and in
FNC-B4. Using confocal microscopy, co-expression of GnRH and GPR54 or
GnRH and kisspeptin was found in fetal olfactory mucosa and FNC-B4. The
24 h exposure to sex steroids regulated both gene (qRT-PCR) and protein
(western blot and immunocitochemistry) expression of KISS1/GPR54 in FNCB4. Increasing doses of 17beta-estradiol (0.01–1 nM) significantly and dosedependently decreased KISS1/GPR54 mRNA. Conversely, androgens (DHT,
0.01–1 nM) significantly stimulated KISS1/GPR54 mRNA. Immunofluorescence with anti-kisspeptin confirmed that 1 nM 17beta-estradiol significantly
reduced, whereas 1 nM DHT significantly increased, the % of kisspeptinpositive FNC-B4 cells. Testosterone treatment showed no effect, but, blocking
its aromatization with letrozole, it mimicked DHT stimulatory activity. In
addition, 24 h exposure to leptin (1 nM), an adypocyte-derived hormone acting
on the hypothalamus to influence puberty, significantly increased
KISS1/GPR54 gene and protein expression. Leptin treatment in FNC-B4
significantly increased also the androgen receptor (AR) mRNA, as well as the
mRNA of its own receptor (LEPR), which resulted induced also by 1nM DHT.
These data suggest a synergistic action between AR and LEPR to finally
up-regulate KISS1/GPR54 system, which, in contrast, was inhibited by
estrogen. In conclusion, our results revealed for the first time that sex steroids
and leptin regulate KISS-1/GPR54 system in human GnRH neurons, providing
new insights into the comprehension of those permissive signals for pulsatile
GnRH secretion and puberty onset.
Endocrine Abstracts (2007) Vol 14
9th European Congress of Endocrinology, Budapest, Hungary, 2007
EGFR ligands mediate key events of female reproduction: reduced litter
size due to impaired fertilization in a transgenic mouse model
Marlon R. Schneider1, Ana A. Gratao1, Maik Dahlhoff1, Fred Sinowatz2 &
Eckhard Wolf1
Institute of Molecular Animal Breeding and Biotechnology, University of
Munich, Munich, Germany; 2Institute of Veterinary Anatomy, University of
Munich, Munich, Germany.
Visceral fat amount as predictor for subclinical cardiovascular disease
in women with polycystic ovary syndrome
Teresa Cascella1, Stefano Palomba2, Ilario De Sio3, Francesco Manguso4,
Laura Vuolo1, Francesco Giallauria5, Alessandra Grieco1,
Gaetano Lombardi1, Annamaria Colao1, Domenico Tafuri6 &
Francesco Orio7
Department of Molecular & Clinical Endocrinology and Oncology,
“Federico II” University of Naples, Naples, Italy; 2Department of Obstetrics
and Gynecology, University “Magna Graecia” of Catanzaro, Catanzaro,
Italy; 3Department of Internal Medicine, Hepatology, and Gastroenterology,
Second University of Naples, Naples, Italy; 4Gastroenterology Unit,
“Cardarelli” Hospital, Naples;, Naples, Italy, 5Department of Clinical
Medicine, Cardiovascular and Immunological Sciences, Cardiac Rehabilitation Unit, Institute of Internal Medicine and Metabolic Disease, “Federico
II” University of Naples, Naples, Italy; 6Teaching and Methods of Sportive
Activity, “Parthenope” University of Naples, Naples, Italy; 7Endocrinology,
Faculty of Motor Science, “Parthenope” University of Naples and
Department of Molecular & Clinical Endocrinology and Oncology,
“Federico II” University of Naples, Naples, Italy.
EGFR ligands, a family of seven related peptide growth factors, are emerging as key
factors regulating different aspects of female reproduction including oocyte
maturation and ovulation, and implantation. Betacellulin (BTC) is a rather neglected
EGFR ligand whose biological activities have been mostly associated with the
endocrine pancreas. During the routine breeding of recently established BTC
transgenic mouse lines (Schneider et al., Endocrinology 146, 5237–5246, 2005),
reduced female fertility became evident. Thus, a systematic study of different aspects
of female reproduction was carried out. While puberty onset and estrous cyclicity
were not affected in the transgenic animals, controlled matings revealed reduced
litter size as the major reproductive deficit of BTC transgenic females (5.3G0.7 vs.
9.9G0.3 pups/litter in non-transgenic controls). Embryo implantation (visualized by
injection of blue dye) was shown to be delayed. However, the number of embryos
implanted or recovered from the uterus was already reduced by about 50% in the
transgenic group, indicating that delayed implantation was not the cause of reduced
litter size. Collection of oocytes from transgenic and control females mated to nontransgenic males revealed that the number of ovulated oocytes was not different
between the groups (10.4 vs 10.7, respectively). However, the proportion offertilized
oocytes recovered from transgenic females was significantly reduced (54% vs.
81.7%). Next, in vitro maturation (IVM) and fertilization (IVF) were carried out to
study these aspects more closely. While IVM rate was only slightly affected, the
proportion of fertilized oocytes obtained from transgenic females was strongly
reduced as compared to the rate observed in oocytes derived from the control group
(57.5% vs 84.6% cleavage rate). Localization of strong transgene-derived BTC
levels in the cumulus and granulosa cells of transgenic follicles supports this
observation. In summary, excess of BTC perturbs oocyte maturation and
fertilization. Implantation is delayed but appears to have no consequence for the
overall reproductive performance of transgenic females.
Integration of the EGF network with early LH signal in preovulatory
Sara Panigone1, Minnie Hsieh2, Luca Persani1 & Marco Conti2
Lab Experimental Endocrinology, IRCCS Istituto Auxologico Italiano,
University of Milan, Cusano Milanino, MI, Italy; 2Division of Reproductive
Biology, Department of Obstetrics and Gynecology, Stanford, University
School of Medicine, Stanford, CA, United States.
Recent studies demonstrate an essential role of the EGF network in propagating
the LH signal within ovarian preovulatory follicles. However, the molecular bases
for the integration are poorly characterized. Here, we propose that the early LH
signal leading to ovulation is amplified through activation of the EGF network.
For this study, preovulatory follicles from euthanized gonadotropin-primed
mice were isolated and cultured with or without recombinant LH (rLH) and/or
specific inhibitors. Primary granulosa cells were used in additional experiments.
Analysis of EGF receptor (EGFR) and MAPK activation was performed by
immunoprecipitation, western blot and immunohistochemistry (IHC). An increase
in EGFR phosphorylation was detected as early as 30 minutes after LH stimulation.
This activation is most likely cAMP dependent and sensitive to AG1478, an EGFR
kinase inhibitor, as well as to inhibitors of matrix-metalloproteases (GM6001 and
TAPI-1), suggesting the involvement of shedding of EGF-like factors in
LH-induced EGFR transactivation. A target of EGFR signaling is the MAPK
pathway. In IHC assays, signal for phosphorylated MAPK was observed in mural
granulosa cells of preovulatory follicles within 15–30 minutes of hCG stimulation,
and in both granulosa and cumulus cells after 1 h. In cultured follicles, LH-induced
MAPK activation is partially inhibited by AG1478 and GM6001, indicating that
this pathway is regulated in part by the EGF network. Furthermore, treatment of
granulosa cells with a combination of neutralizing antibodies against amphiregulin, epiregulin and betacellulin (EGF-like factors described as regulators of
ovulation) significantly inhibits EGFR phosphorylation and MAPK activation,
supporting a role for these ligands in the LH-induced EGFR signaling in mural
granulosa cells.
In conclusion, we provide evidence of early activation of EGF network
following LH stimulation, involving rapid shedding of EGF-like ligands and EGFR
transactivation. This mechanism partecipates in the rapid amplification and
propagation of the LH signal within preovulatory follicles.
Endocrine Abstracts (2007) Vol 14
Introduction and aim
Polycystic Ovary Syndrome (PCOS) is a common disorder associated with a wide
range of endocrine and metabolic abnormalities. Obesity is present in about
45–50% of PCOS women. Increased cardiovascular risk factors and evidence of
subclinical cardiovascular disease (CVD) have been reported in PCOS. The aim
of the present study was to evaluate whether visceral fat amount may be
considered as predictor for early CVD in PCOS women.
Patients and methods
The procedures used were in accordance with the guidelines of the Helsinki
Declaration on human experimentation. The study was approved by the local
Ethical Committee. Two-hundred PCOS women and 100 healthy age- and body
mass index-matched women were enrolled in this prospective baseline-controlled
clinical study. Non-invasive markers of early CVD [carotid intima-media
thickness (IMT), brachial arterial flow-mediated dilation (FMD)] and visceral
fat amount [using abdominal ultrasonography] were evaluated. Inflammatory
biomarkers [C-reactive protein (CRP), fibrinogen, white blood cells (WBC)
count, plasminogen activated inhibitor (PAI)-1], hormonal and metabolic
parameters were also investigated.
Subjects with PCOS had significantly (P!0.001) higher visceral fat compared to
healthy women [31.4C7.3 vs. 28.0C6.1, mmCSD), respectively] which were
directly related to HOMA (rZ0.918, P!0.001), AUCINS (rZ0.879, P!0.001)
and WC (rZ0.358; P!0.001). Stepwise linear regression model showed that
visceral fat amount was an independent predictor of IMT, FMD and CRP.
The early impairment of endothelial structure and function, the increase of lowgrade chronic inflammation and insulin resistance in women with PCOS are
associated with increased central fat excess. Visceral fat amount could be an
important predictor of subclinical CVD in PCOS.
The current definitions of the metabolic syndrome underestimate the
prevalence of nascent metabolic abnormality in adolescents with PCOS
Didier Dewailly, Sophie Catteau-Jonard & Anne-Céline Reyss
Lille University Hospital, Lille, France.
The prevalence of the metabolic syndrome (MS) is notably higher in patients with
PCOS than in the general population. Presumably, this prevalence increases as a
function of age but the subgroups of patients less than 20 yr. old studied so far are small.
In order to further document this issue, we have selected for this study 498 patients
with PCOS aged 12.5–38 yr (Rotterdam definition) and 188 control women aged
15.5–38.5 yr, that have been consecutively included in a database and in whom the
required clinical, hormonal and ultrasound data were available. A metabolic score has
been calculated according to the ATP-III classification and defined the MS when R3.
The prevalence of the MS was significantly higher in the PCOS than in the control
group (15.2% vs 4.8%, P!0.0001). It did not differ significantly (PZ0.063) between
the 3 subgroups of patients with PCOS according to age, i.e., 12.8% in patients aged
% 0 yr (nZ47), 13.9% in patients aged 21–30 yr (nZ301) and 18.7% in patients
aged 31–40 yr (nZ150). However, we observed that a metabolic score of 1 or 2
tended to be more frequent in the adolescent group than in the groups of older patients
9th European Congress of Endocrinology, Budapest, Hungary, 2007
(cumulated rate 1C2: 66.0% vs 51.8% and 48.7%, respectively, PZ0.09). In the
patients having a scoreZ1, a HDL-Cholesterol (HDL-C) !0.5 g/L was found in
57.1% adolescents vs 26.3% and 27% patients aged 21–30 and 31–40 yr, respectively
(PZ0.068). In the same group, a waist circumference (WC) O80 cm was found in
35.7% adolescents vs 69.7% and 70.3% patients aged 21–30 and 31–40 yr,
respectively (PZ0.047). In patients with a scoreZ2, a HDL-C !0.5 g/L and a
WCO80 cm were found in 100% of cases in every subgroup.
By requiring some items that reflect relatively late complications of insulin resistance
(hypertriglyceridemia, hypertension, glucose intolerance or diabetes), the current
definitions of the MS in adults underestimate the prevalence of nascent metabolic
abnormality in adolescents. Our data indicate that a HDL-C !0.5 g/L is the most
sensitive marker of such abnormality, while a WC O80 cm seems to be less sensitive
than in adults.
ABCC8 (nZ141), KCNJ11 (nZ140), Gck (nZ21), GLUD1 (nZ27), SCHAD
(nZ10), and UCP2 (nZ46), (number of investigated patients in brackets).
In 53 of all patients (37%), a genetic explanation was found, while 90 patients had
no mutations detected. Of these, 46 had persistent or recurrent medical-responsive
hyperinsulinaemic hypoglycaemia and available DNA for UCP2 analysis. No
mutations were found in UCP2. The well-known polymorphism A55V was seen
in 29 patients.
UCP2 mutations are rarely – if ever – found in CHI patients with persistent or
recurrent CHI. Other genetic explanations should be considered.
Diabetes – OC12
Hypoglycemia and cerebral ATP synthesis in Type 1 Diabetes
Martina Mandl1, Stefan Zbyn1, Vladimir Mlynarik2, Miriam Promintzer1,
Anton Luger1, Michael Krebs1, Christian Anderwald1 & Martin G. Bischof1
Division of Endocrinology and Metabolism, Department of Internal
Medicine III, Medical University of Vienna, Vienna, Austria; 2MR Center of
Excellence, Medical University of Vienna, Vienna, Austria.
The mechanisms responsible for the progressive failure of hypoglycemia counterregulation in type-1 diabetes (T1DM) are poorly understood. Alterations of brain
energy metabolism could influence glucose sensing by the brain and, thus contribute
to hypoglycemia associated autonomic failure. Thus, we measured intraneuronal
kinetics of total ATP-synthesis from PCr (kfor) in T1DM patients and effects of hypo/
hyperglycemia on this brain energy metabolism. Healthy nondiabetic humans
(CON; 5 m/1f, BMIZ23.5G1.0 kg/m2, ageZ25G1 yr, HbA1cZ5.1G0.1%),
T1DM patients with good (T1DMgood; 5 m/1f, BMIZ25.5G0.4 kg/m2, ageZ
24G2 yr, HbA1cZ6.8G0,1%) and poor (T1DMpoor; 5 m/1f, BMIZ24.9G
1.6 kg/m2, ageZ25G2 yr, HbA1cZ8.9G0.3%) glycemic control were examined
before, during and after hyperinsulinemic-(1.5 mU$kgK1$minK1)-hypoglycemic(w50 mg/dl) or –hyperglycemic-(w250 mg/dl)-clamp tests. kfor in the occipital lobe
was measured by 31P-nuclear-magnetic-resoance spectroscopy (3T) using saturation
transfer, and calculated with McConnell equations. In T1DMpoor, kfor was increased
during hypoglycemia (0.58G0.07 sK1), when compared to CON (0.36G0.03 sK1;
PZ0.006), T1DMgood (0.41G0.02 sK1; PZ0.03), and baseline (0.43G0.05 sK1;
PZ0.03). During post-hypoglycemic recovery, T1DMpoor showed higher kfor
(0.57G0.07 sK1), when compared to CON (0.40G0.05 sK1, P!0.05), and
T1DMgood (0.37G0.01 sK1, PZ0.03). HbA1c-levels were positively correlated
with kfor during hypoglycemia (rZ0.47, PZ0.02), but not at baseline (rZ0.20, PZ
0.37) or during recovery (rZ0.39, PZ0.07).
P NMRS with saturation transfer can be used for non-invasively measurement of
cerebral ATP-synthesis during hypoglycemia in vivo. The positive correlation of
HbA1c levels and kfor during hypoglycemia hints at an involvement of the CK
system in the pathogenesis of hypoglycemia associated autonomic failure.
Uncoupling protein 2 mutations – a new explanation for congenital
Henrik Thybo Christesen1, Khalid Hussain3, Lone Svargo2, Bendt Brock
Jacobsen1 & Klaus Brusgaard2
HC Andersen Children’s Hospital, Odense, Denmark; 2Dept. of Clinical
Genetics, Odense University Hospital, Odense, Denmark; 3London Center
for Paediatric Endocrinology and Metabolism, Great Ormond Street
Hospital, London, United Kingdom.
Congenital Hyperinsulinism (CHI) is genetically unexplained today in up to 50%
of the patients with persistent or recurrent disease. The uncoupling protein 2
(UCP2) gene is a candidate gene for medical-responsive CHI, since knock out
studies have shown that UCP2 deficiency leads to increased glucose-stimulated
insulin secretion.
Patients and methods
In a large series of 142 patients with transient, persistent or recurrent CHI, we
examined for mutations using DHPLC and direct sequencing, or cutting with
restriction enzyme for specific variations, in the known disease-causing genes
Adhesion molecules two years after gestational diabetes
Thomas Prikoszovich1, Giovanni Pacini2, Christine Winzer1, Anton Luger1,
Oswald Wagner3 & Alexandra Kautzky-Willer1
Medical University Vienna, Department of Internal Medicine III, Division
of Endocrinology and Metabolism, Vienna, Austria; 2Institute of Biomedical Engineering, CNR, Padova, Italy; 3Medical University Vienna,
Department of Medical and Chemical Laboratory Diagnostics, Vienna,
We investigated in women with prior GD (pGD) at risk of diabetes and premature
atherosclerosis in comparison to women with normal glucose tolerance during
and after pregnancy (C) parameters of inflammation, endothelial dysfunction and
glucose tolerance in a follow-up study.
119 pGD and 41 C underwent an oral glucose tolerance test 3 months, 1 and 2
years after delivery with measurements of plasma concentrations of circulating
adhesion molecules (cAMs: VCAM, ICAM-1, ELAM), endothelin, leptin, sCRP,
IL-6, fibrinogen, PAI-1 and ADMA. Intima-media-thickness (IMT) of the
common carotid artery was measured by ultrasound and insulin sensitivity (SI)
was calculated from insulin-modified FSIGTs at baseline.
At baseline ICAM (P!0.0001), VCAM (P!0.005), ADMA (PZ0.0005), sCRP
(PZ0.04) and PAI-1 (PZ0.01) were higher and SI (PZ0.001) was lower in pGD
than in C. SI inversely related to all cAMs (rZK0.20; P!0.02), sCRP (rZK0.52;
P!0.0001), IL-6 (rZK0.25; PZ0.01), and fibrinogen (rZK0.22; PZ0.006).
All cAMs also related to leptin (rZ0.17; P!0.04) and BMI (rZ0.18; P!0.03).
IMT was associated with SI (rZK0.32; PZ0.03), BMI (rZ0.31; PZ0.02) and
PAI-1(rZ0.30; PZ0.03). After two years ELAM (P!0.02), ADMA (P!0.0007),
PAI-1 (P!0.001), vWF (P!0.04), blood pressure (P!0.001) decreased, while
ICAM-1, VCAM and BMI remained unchanged. Leptin (PZ0.01), TNFa (P!
0.001) and endothelin (P!0.04) increased compared to baseline. Higher age
(P!0.05) and BMI (P!0.0001), increased levels of ELAM (P!0.003), Leptin
(P!0.0005) and a lower insulin sensitivity (OGIS;PZ0.01) at baseline
characterised those pGD with deterioration of their initial normal glucose tolerance
(nZ15) in comparison to those who retained normal glucose tolerance (nZ65)
within 2 years. Logistic regression revealed BMI (OR[CI]: 1.313[1.03-1.67]) and
ELAM (OR[CI]: 1.064[1.01-1.12]) as independent predictors of a deterioration of
glucose tolerance.
Women with pGD are characterised by higher plasma ICAM and VCAM relating
to insulin-resistance and inflammatory parameters. Moreover the degree of
obesity and ELAM at baseline predicted deterioration of glucose tolerance within
2 years after delivery.
Polymorphisms of PSMA6 gene and its adjacent genomic sites and their
association with type II diabetes mellitus in the Latvian population
Ilva Poudziunas, Tatjana Sjakste, Martins Kalis, Maris Lagzdins,
Valdis Pirags, Nikolajs Sjakste & Jelizaveta Sokolovska
University of Latvia, Riga, Latvia.
A possible involvement of proteasomes in the pathogenesis of type II diabetes
mellitus has been recently reported. Therefore, association of polymorphism of
proteosomal genes with type II diabetes mellitus is of particular interest. In this
study, molecular markers of the proteasomal alpha subunit 6 gene PSMA6 and its
adjacent genomic sites have been analyzed.
The goal of this study was to characterize polymorphisms of the HSMS801,
HSMS702, HSMS701 and HSMS602 HSMS006 HSMS602 microsatellite
Endocrine Abstracts (2007) Vol 14
9th European Congress of Endocrinology, Budapest, Hungary, 2007
repeats and SNPs at positions –110 and –8 from the translation start of PSMA6
gene and to investigate their eventual association with type II diabetes mellitus.
In this study, 250 DNA samples of type II diabetes and healthy controls were
used. Genotyping was performed using allele-specific PCR and restriction
fragment analysis.
For the HSMS006 marker, the 193 bp allele was more common the group of cases
rather than controls (0.154 and 0.085 respectively, PZ4.64%). HSMS801 allele
of 155 bp was found more often in the control group, as the HSMS602 marker
allele of 169 bp. HSMS801 genotype of 148 bp/152 bp was more frequent in the
control group (0.000 and 0.041 respectively, PZ4.22%). Significant differences
were observed between cases and controls in all ten haplotype distributions
created by combinations of all the microsatellites by two. In these combinations
linkage disequilibrium was revealed, indicating the non-random association of
alleles in two or more loci on a chromosome. Genotype –8CG was significantly
more frequent in type 2 diabetes patients, and haplotype CK110/GK8, compared to
CK110/CK8 was associated with a higher risk of type II diabetes.
These results show association between microsatellite and SNP alleles of PSMA6
gene and its adjacent genomic sites with type II diabetes mellitus.
The influence of concomitant diabetes mellitus on mortality in
Addison’s disease
Ragnhildur Bergthorsdottir1, Maria Leonsson-Zachrisson1, Anders Odén2 &
Gudmundur Johannsson1
Department of Endocrinology, Sahlgrenska University Hospital, Gothenburg, Sweden; 2Department of Mathematical Sciences, Chalmers University
of Technology, Gothenburg, Sweden.
The prevalence of type 1 diabetes mellitus (DM) among patients with primary
adrenal insufficiency (Addison’s disease) is 3-4 times higher than the expected
prevalence in the population. The mortality rate due to DM is more than 3-fold the
mortality rate in the background population. The impact of DM on mortality rate
in patients with Addison’s disease is not known.
To study the frequency of DM and its impact on mortality rate in patients with
Addison’s disease.
Study design
In a population-based retrospective observational study between the years 1987
and 2001 using the Swedish Hospital Register we followed patients from the first
registered hospitalisation where the diagnosis of Addison’s disease appeared until
end of follow-up or death. We looked for the concomitant presence of DM at the
time of detection.
We identified 1675 patients, 995 women and 680 men, diagnosed with primary
adrenal insufficiency. Concomitant DM was observed in 199 (12%) of the
identified patients. DM had a significant influence on total mortality with the
relative risk (RR) for death 1.82 (CI 1.29–2.06) for men and 1.52 (CI 1.11–2.07)
for women with Addison’s disease and DM compared with those patients with
Addison’s disease without DM.
The impact of DM on the excess mortality in the whole group of Addison’s
patients was limited since excluding patients with concomitant DM only
decreased the RR for death by 7% in both men (2.19 vs 2.04) and women (2.86
vs. 2.68).
Having DM and Addison’s disease significantly increased the risk of death when
compared with having Addison’s disease alone. However, the overall impact of
concomitant DM on the total mortality in all patients with Addison’s disease was
Short-term effects of atorvastatin on endothelial functions and oxidized
LDL levels in type 2 diabetic patients
Aysen Akalin1, Gokhan Temiz2, Nevbahar Akcar3 & Banu Sensoy3
Osmangazi University Medical Faculty Department of Endocrinology,
Eskisehir, Turkey; 2Osmangazi University Medical Faculty Department of
Endocrine Abstracts (2007) Vol 14
Internal Medicine, Eskisehir, Turkey; 3Osmangazi University Medical
Faculty Department of Radiology, Eskisehir, Turkey.
We aimed to investigate the short term effects of atorvastatin on endothelial
function and oxidized LDL (oxLDL) levels and to evaluate the association of
endothelial dysfunction to oxLDL levels and inflammatory markers in type 2
diabetic patients.
Material and methods
After ethical committee approval thirty type 2 diabetic and 11 healthy subjects
with LDL levels between 100–160 mg/dl. Without a history of cardiovascular
event were included in the study.Both groups were matched with respect to age,
gender, body mass indices, body composition and lipid levels. Flow-mediated
dilatation (endothelium-dependent, FMD) and nitroglycerine-induced dilatation
(endothelium- independent, NID) were measured in the brachial artery using
high-resolution ultrasound in all participants. Carotid artery intima media
thickness (IMT) was also evaluated. OxLDL levels, lipid parameters, blood
glucose, C-peptide, HbA1c and inflammatory markers including C-reactive
protein(CRP), fibrinogen, erithrocyte sedimentation rate (ESR) were studied.
Type2 diabetic patients recived 10 mg. Atorvastatin for 6 weeks and FMD, NID,
IMT reevaluated and ox-LDL levels and inflammatory markers were measured.
Basal FMD, NID, IMT and ox-LDL levels besides inflammatory markers were
not significantly different between patients and controls. No correlation was found
between inflammatory markers and FMD and NID. Only IMT correlated with the
NID and fibrinogen levels obtained before treatment. In nondiabetics, IMT also
correlated with oxLDL levels (P:0.013). FMD and NID significantly improved
after atorvastatin therapy (7.62G7.6 vs. 12.65G7.8, P!0.001 and 18.22G9.57
vs. 21.43G9.6, PZ0.007, respectively). Atorvastatin significantly reduced
ox-LDL levels (57.85G10.33 vs. 44.36G6.34, P!0.001) and IMT (0.627G
0.17 vs. 0.597G0.16, P 0.02) in diabetics.
Atorvastatin improves endothelial functions and reduces oxLDL levels in type 2
diabetics with average lipid levels in the short term and may have beneficial
effects in the prevention of early atherosclerotic changes.
A propensity-based comparison of haemodialysis and peritoneal
dialysis among diabetic patients with end-stage renal disease in the
United States
LA O’Shea & AG Stack
Department of Renal Medicine, LGH, Co. Donegal, Ireland.
Renal transplantation is the optimal treatment strategy for patients with endstage renal disease (ESRD); few are afforded the opportunity due to limited
organ supply. Of the alternatives, peritoneal dialysis (PD) and hemodialysis
(HD), it is unclear which confers the greater survival advantage, as prior
comparisons have demonstrated conflicting results due to lack of case-mix
adjustment, limited follow-up, and failure to consider switches in modality over
We compared all-cause and cause-specific mortality between PD and HD in
national cohort of 263,556 new ESRD patients in the U.S. who began treatment
between 5/1995 and12/2000, and followed until 12/2001. A propensity analysis,
predicting the probability of assignment to PD, was used to control for baseline
differences through regression adjustment and matching based on 23
demographic and comorbid indicators. The C-statistic for this model was
0.75, indicating excellent discrimination between treatments. Time-dependent
Cox regression, stratified by age and diabetes, compared PD and HD using an
intent-to-treat and as-treated approach and patients were censored at
transplantation, loss to follow-up or end of study.
There were 122,672 deaths (46.5%), 24,596 renal transplants (9.3%) and
17,432 (6.6%) patients lost to follow-up within the 6-yr period. The adjusted
relative PD/HD hazards ratios [RR] with 95% Confidence Intervals for all-cause
and cause-specific mortality are shown (intent-to-treat analysis).
Mortality risks were significantly greater for PD compared with HD among
diabetic patients and were principally confined to older patients. The excess
mortality could be accounted for, in decreasing order, by increased death risk
from infection, cardiac, stroke and the other causes of death category.
In conclusion, haemodialysis should be preferentially considered over PD
among older (O50 yrs) diabetics with ESRD in order to improve patient
9th European Congress of Endocrinology, Budapest, Hungary, 2007
Poster Presentations
Endocrine Abstracts (2007) Vol 14
9th European Congress of Endocrinology, Budapest, Hungary, 2007
Comparative Endocrinology – presented on Sunday
Human adrenal NCI-H295R cells produce more C19 steroids than NCIH295A cells – a possible model to study regulation of androgen
Elika Samandari, Petra Kempna, Gaby Hoffer, Primus E Mullia & Christa
E Fluck
University Hospital, Bern, Switzerland.
The human adrenal cortex consists of three layers in which specific steroid
hormones are produced. Human adrenal NCI-H295A (A) and NCI-H295R (R)
cells, originate from the same adrenocortical tumor and express all genes
essential for steroidogenesis. Therefore they often serve as a suitable model to
study human steroidogenesis. No data are available comparing steroidogenesis
of A vs. R cells. Assuming no difference, research data from these two cell
lines are directly compared. To characterize A and R cells, we investigated
steroidogenesis of both cell lines. We found differences in the steroid profile
of A and R cells. A cells converted [3H]-pregnenolone predominantly to
aldosterone and cortisol while only traces of androgens were produced. R
cells converted [3H]-pregnenolone to aldosterone, cortisol and androgens. The
observed differences may be either due to differences in gene expression and
/or posttranslational modifications which may lead to different activities of
specific enzymes. Having found a profound difference in androgen synthesis,
we compared HSD3B2 and CYP17 gene expression performing RT and real
time PCR. We observed higher HSD3B2 expression in A cells compared to R
cells while no difference in the expression of CYP17 was found. Functional
studies were performed for P450c17 and 3betaHSDII enzymes. To study the
activities of P450c17 (17alpha-hydroxylase and 17, 20 lyase), cells were
treated with trilostane (3betaHSD inhibitor) prior to [3H]-pregnenolone or
[3H]-17alpha-hydroxypregnenolone incubations. R cells showed higher 17, 20
lyase activity. To study 3betaHSDII activity, cells were incubated with [3H]DHEA. Interestingly, lower 3betaHSDII activity was detected in R cells. In
summary, we show that A and R cells differ in their steroid profile. R cells
produce significantly more androgens. Further comparative studies of A vs. R
cells may help to understand mechanism/s regulating human androgen
production in health and disease.
Study of the hypothalamic-pituitary-adrenal axis in patients with the
antiphospholipid syndrome
Renato Carignola1, Valeria Data1, Rosetta Vitetta1, Adriana Severino1,
Tiziana Bertero2, Mario Bazzan3, Giuseppe Reimondo1, Fulvia Daffara1,
Alberto Angeli1 & Massimo Terzolo1
Dipartimento di Scienze Cliniche e Biologiche – Medicina Interna I, ASO
San Luigi, Orbassano, Italy; 2UONA Immunologia e Allergologia Clinica,
Ospedale Mauriziano, Torino, Italy; 3UOA Ematologia e Malattie
Trombotiche, Humanitas Cellini, Torino, Italy.
The Antiphospholipid Syndrome (APS) is a thrombophilic disorder characterised
by recurrent venous and/or arterial thromboses and increased pregnancy
morbidity. There is growing evidence supporting a functional interplay between
the neuroendocrine and immune system; the hypothalamic-pituitary-adreal
(HPA) axis plays a pivotal role in this network. Previous studies have described
normal cortisol levels in APS patients while occurrence of acute adrenal failure
was reported as a manifestation of this syndrome. However, it is still unknown
whether subtle alterations of the HPA axis do exist in APS patients without overt
In the present study, we performed either a low-dose (1 mg) short Synacthen test
(LDSST) or a 250 mg Synacthen test (SST) in 15 subjects of both sexes with
primitive APS (diagnosed according to the Sapporo Criteria) and in 11 age and
sex-matched healthy subjects. In addition, the patients underwent 1 mg
dexamethasone suppression test (DST). None of the evaluated subjects were
receiving any drug known to affect the HPA axis. The local Ethical Committee
approval has been obtained.
The patients with APS showed significantly higher cortisol levels than controls
either at baseline (31.2G15.6 vs. 18.3G9.0 mg/dl, P!0.01) or at C30 min
following 250 mg ACTH (57.3G14.2 vs. 39.6G12.8 mg/dl, P!0.01). Cortisol
levels after 1 mg ACTH were also significantly increased in the subjects with APS
compared to controls (P!0.01). Moreover, in only 2 patients we observed cortisol
levels lower than 1.8 mg/dl after 1 mg DST (mean, 3.4 mg/dl; range 1.4–9.2) and
two patients had cortisol values above 5.0 mg/dl after suppression.
In conclusion, although APS may cause adrenal insufficiency in selected cases,
the present data seem to suggest that the HPA axis is not suppressed in APS
patients. A possible explanation might be the state of chronic stress that usually
accompanies long-standing autoimmune diseases.
Effects of ethanol and blokade of synthesis of nitric oxide on level of
ACTH in female rats
Dragoslava Djikic, Sanja Vranjes-Djuric, Mirela Budec & Andjelka Spasic
University of Belgrade; Institute for Medical Research, Belgrade, United
States, Institute for Nuclear Sciences “Vinca”, Belgrade, United States;
University of Belgrade, School of Medicine, Institute for Forensic Medicine,
Belgrade, United States.
We showed previously that a single dose of ethanol acts as a stressor in female rats
(Milovanovic et al., 2003). In order to extend this observation, we investigated
whether the effect of ethanol on ACTH is dose-related and possible interactions
between nitric oxide (NO) and alcohol on the level of ACTH. To this end, adult
female Wistar rats showing diestrus day 1 were treated with: (a) ethanol (2 or
4 g/kg, i.p.), (b) Nu-nitro-L-arginine-methyl ester (L-NAME), which blocks the
activity of all isoforms of nitric oxide synthase, (30 mg or 50 mg/kg, s.c.)
followed by ethanol (2 or 4 g/kg, i.p.) 3 h later and (c) L-NAME (30 mg or
50 mg/kg, s.c.) followed by saline 3 h later. Untreated rats were used as controls.
The animals were sacrificed 0.5 h after ethanol administration. Blood ethanol
levels were measured using gas chromatography. Plasma concentrations of
ACTH were determined by radioimmunoassay. Obtained results showed that
acute ethanol treatment significantly, dose-relatedly, enhanced the level of ACTH
(P!0.01). The same phenomenon was observed in the groups treated with
different doses of L-NAME followed by ethanol (P!0.05). Elevated
concentration of ACTH was also found in the groups injected with L-NAME
followed by saline (P!0.05).
Our results suggest that acute ethanol treatment increases the level of ACTH in
dose-dependent manner. Although endogenous NO exerts negative influence on
ACTH, it seems that it is not involved in the observed effect of ethanol under these
experimental conditions.
Milovanovic T. et al. J Stud Alcohol 64:662–668, 2003.
(Supported by grant 145087 from the Ministry of Science of Serbia)
Endocrine Abstracts (2007) Vol 14
Survey of thyroid function of Hungarian Vizsla population in Hungary
Julianna Thuroczy1, Aniko Tibold1 & Lajos Balogh2
SzIU, Faculty of Veterinary Science, Budapest, Hungary; 2FJNCH,
National “FJC” Research Institute for Radiobiology and Radiohygiene,
Budapest, Hungary.
The prevalence of hypothyroidism in women of childbearing age is relatively high.
The incidence of hypothyroidism during pregnancy has been calculated as between
0.3% and 0.7%. Overt abnormalities in thyroid function are common endocrine
disorders affecting more than 19.2% of pregnant women in certain geographic
areas of Hungary. 80% of Hungarian inhabitants are living in an iodine deficient
area. The aim of this study was to investigate the prevalence of thyroid dysfunction
in Hungarian Vizsla, a traditional breeding dog population.
A screening study was done on 95 Hungarian Vizsla, females and males. Serum
total thyroxin, free thyroxin, triiodotyronine, total cholesterol and triglyceride
concentrations were measured. The owners were asked to fill in a questionnaire
concerning feeding and reproductive problems. TT4, freeT4 and T3 concentrations
were determined by ELISA validated for use in canine serum.
The means and standard errors of the data were calculated and subjected to
ANOVA and Student’s t-test where appropriate. Significance was set at P%0.05.
Total T4 concentration of 36 dogs was lower (15.72G2.62 (meanGS.D.)) than
the reference range (20.0–45.0 nmol/l). Total T4 level of 56 dogs was in reference
range 26.83G4.68 and of five was higher, 92.97G64.86, than range. Total T4, free
T4 and K values were different in the three groups at level of significance. T3
concentrations of suspected hypothyroid dogs (0.66G0.24), dogs with normal
thyroid function (0.77G0.45) and dogs with suspected hyperthyroidism (0.67G
0.06) were not different at level of significance. TT4 concentrations of 25 (26.3%)
dogs with familiar relations were out of reference range.
Our approach of a clinical investigation-based screening was rather efficient in
suspicion of overt thyroid dysfunction but not for detecting many cases with
9th European Congress of Endocrinology, Budapest, Hungary, 2007
subclinical dysfunction. The high incidence of TT4 values out of range indicates a
suspicion that the effect of iodine deficiency on thyroid function of dogs is similar
to that in human subjects.
Effects of melatonin on glutathione peroxidase activity after adriamycin
in normal and pinealectomized rats
Katarzyna Dabrowska1, Michal Stuss1, Jolanta Gromadzinska2,
Wojciech Wasowicz2 & Ewa Sewerynek1
Department of Bone Metabolism; Medical University of Lodz, Lodz,
Poland; 2The Nofer Institute of Occupational Medicine, Lodz, Poland.
Pancreatic polypeptide (PP) radioimmunoassay in acute phase and
regression of cerulein induced pancreatitis
Grazyna Orlicz-Szczesna & Jolanta Zdanowska-Filipczak
Department of Internal Diseases University School of Medicine, Lublin,
Acute pancreatitis is a real medical problem with high patients mortality.
Pathogenic interdependence between pancreas follicles function and islet
endocrine secretion is under research. PP cells are pancreatic polypeptide (PP)
producing cells, they determine about 1% islets, but their function is not
completely known yet. Vagus nerve and peptidergic stimulation regulates PP
The aim of study was to estimate cerulein induced pancreatitis effects on rat
serum PP concentration and pancreas morphology characteristics.
The study was conducted on male Wistar rats. They were anaesthetized with
ketamine. We measured serum PP concentration during experimental ceruleininduced acute pancreatitis and different inflammatory process regression stages.
Acute pancreatitis was developed through i.v. cerulein infusion 5 mg/kg per hour.
Rats were divided into several groups in dependence on infusion time –
3,6,9,12 hours. Then rats had free access to standard nourishment and water.
Blood samples from rat group with 12 hours cerulein infusion were taken after
3,6,9 and 12 days of observation. Control groups received i.v. 0.9% NaCl
infusion. Pancreas histological changes were analyzed. Serum amylase and PP
concentrations were assessed with DRG International Inc. (USA) kit. Both rabbit
serum with antibodies against PP and goat’s anti-rabbit gamma-globulin in buffer
were used.
After 12 hours lasting cerulein infusion we obtained full biochemical and
morphological acute pancreatitis picture. These changes start to regress after
cerulein infusion withdrawal. Serum PP concentration was decreased after
3 hours of cerulein infusion, still decreased until the end of infusion (0.99 pg/ml).
After cerulein cessation, progressive PP increase was observed, attained control
PP concentration after 9 days (2.4 pg/ml) and exceed it after 12 days (3.5 pg/ml).
Cerulein significantly influence on serum PP concentrations - decreases it
during pancreatitis induction and increases in regression stage. PP determines
exocrine function stimulation, correlates with tissue destruction degree and
pancreas enzymes disturbances.
Evaluation of neuroendocrine disfunction in hypothalamo-pituitaryadrenal axis in diagnosis of depressive and non-depressive alcoholdependent persons
Martina Matovinovic, Darko Katalinic, Andreja Maric, Miljenko Solter,
Josip Ivica, Josip Resetic, Jure Murgic & Milan Vrkljan
Sestre Milosrdnice University Hospital, Zagreb, Croatia.
Acute and chronic alcohol intake and alcohol withdrawal induce dysfunction
of neuroendocrine and other regulatory systems. The aims of this study were
to assess a possible hypothalamo-pituitary-adrenal (HPA) axis dysfunction in
population of alcoholics, using dexamethasone suppression test (DST). The
study was approved by local Ethical Committee. The serum and urinary
cortisol were compared between the groups of 89 male patients (64.5%
depressive and 35.5% nondepressive alcoholics) (Hamilton test), before and
after DST. In nondepressive patients, 50% was nonsupressive in DST. In
depressive patients 46% was suppressive in DST test (serum cortisol). Twentyfour hours urinary excretion in group of nondepressive patients was supressed
in 78% of cases; depressive patients showed 50.9% nonsupressors. Basal
serum cortisol secretion was significantly lower in group of nondepressive than
depressive patients. Also, serum concentration at 16 hours were significantly
higher in group of the depressive nonsupressive patients. Basal urinary cortisol
excretion was in normal range in all patients, but after dividing the patients
into suppressible and nonsuppressible groups, significantly higher (P!0.002)
basal urinary cortisol concentrations were found in latter. We concluded on the
basis of DST test, as well basal cortisol measurement, that the neuroendocrine
dysfunction of alcoholic patients could be present even if the depression is
Adriamycin (ADR) is a potent chemotherapeutic agent, effective in treatment of
leukemias, lymphomas and of many solid tumours. However, its clinical usage is
often limited by cardiotoxicity, induced by oxygen radical damage of membrane
Melatonin (MEL), is a well-known antioxidant. It has been shown that
melatonin can scavenge free radicals, both directly or indirectly, stimulating the
activity of antioxidative enzyme, e.g., glutathione peroxidase (GSH-Px).
The aim of the study was to examine the effect of Mel on the GSH-Px activity
in serum, erythrocytes and the heart after adriamycin.
Materials and Methods
Wistar rats were divided into the 3 groups: pinealectomized (PX), sham-operated
(Sham-PX) and control animals (Intact). Each of the groups was divided into 4
subgroups, injected with: 1 – saline, 2 – MEL, 3 – ADR and 4 – MEL C ADR.
ADR was administered 2 months after PX as a single dose (15 mg/kg, i.p.), 1 hour
after the fourth melatonin injection. Melatonin (5 mg/kg, i.p.) was administered
for 4 days before and 4 days after ADR. After 8 days of treatment the rats were
killed by decapitation. Their hearts and blood were collected for measurements.
The activity of GSH-Px in the heart increased significantly in all the examined
groups after ADR injections. On the contrary, in serum, GSH-Px activity
decreased in all the groups after ADR. In erythrocytes, GSH-Px decreased after
ADR in Px-animals. Mel did not change GSH-Px activity after ADR.
MEL did not influence the activity of GSH-Px, either in normal or in
pinealectomized rats after ADR.
Grant No 502-11-293 of the Medical University of Łódź.
Cytokines and growth factors – presented on Sunday
Is there any role for anti-inflammatory cytokine Interleukin-10 in
advanced congestive heart failure?
Azza Farrag, Nouran El Gahndour & Mohab Halim
Cardiology Department, Cairo University, Cairo, Egypt; Internal Medicine
Department, Cairo University, Cairo, Egypt; Biochemistry Department,
Cairo, Egypt.
CHF manifestations can be explained by the biologic effects of tumor necrosis
factor-alpha (TNF-alpha). Interleukin-10 (IL-10) has potent deactivating properties and is considered a potent anti-inflammatory cytokine that inhibits TNF-alpha
production. This study was designed to examine the role of IL-10 in patients with
CHF and to test its correlation with pro-inflammatory markers.
Fifty patients with CHF were studied. Patients were classified according to
NYHA functional class into 29 (NYHA II), 11 (NYHA III) and 9 patients (NYHA
IV). Serum samples for TNF-alpha, IL-10, soluble TNF receptors (sTNF-R1 and
sTNF-R2), transforming growth factor-beta (TGF-beta) as well as high sensitivity
C-reactive protein (hs-CRP) were taken from all patients and also from healthy,
age and sex matched 50 controls.
CHF patients had a significantly lower level of IL-10 compared to controls
(2.28G1.1 vs 5.39G1.4 pg/ml, P!0.0001). Patients with NYHA class IV had
the lowest serum levels of IL-10 and TGF-alpha which were statistically
significant when compared to patients with NYHA class III (0.67G0.4 vs 1.9G
0.5 pg/ml, P!0.001) and (1348G92 vs 1653G111 pg/ml, P!0.05) respectively, but they had the highest serum level of TNF-alpha, sTNF-R1, sTNF-R2 and
hs-CRP when compared to the same group (8.6G1.9 vs 7.1G0.8 pg/ml, P!
0.01), (2380G141 vs 1831G185 pg/ml, P! 0.01), (3410G174 vs 2841G
191 pg/ml, P!0.01) and (26.4G2.7 vs 14.4G3.9 mg/L, P!0.01) respectively.
Patients with CHF had a significant decrease in their serum level of IL-10 and
increase in TNF-alpha, sTNF-R1, sTNF-R2 and hs-CRP when compared to
normal subjects and these levels change significantly with advanced NYHA
Endocrine Abstracts (2007) Vol 14
9th European Congress of Endocrinology, Budapest, Hungary, 2007
Regulation of GAGEC1, a cancer-testis associated antigen family
member, by sex steroid hormones and TGF-beta: implications for
prostatic disease
Natalie Sampson1, Gerlinde Schuhfried1, Eugen Plas2 & Peter Berger1
Institute of Biomedical Aging Research, Austrian Academy of Sciences,
Innsbruck, Austria; 2Ludwig Boltzmann Institute for Andrology and
Urology, Hospital Lainz, Vienna, Austria.
Blocking undesired leptin action in vivo with leptin antagonists
prepared by site-directed mutagenesis of human, ovine, rat and mouse
leptin site III
Leonora Niv-Spector, Dana Gonen - Berger, Gili Salomon,
Isabelle Callebaut, Jean Djiane & Arieh Gertler
Institute of Biochemistry, Food Science and Nutrition, Faculty of
Agricultural, Food and Environmental Quality Sciences, The Hebrew
University of Jerusalem, Rehovot 76100, Israel.
Prostate homeostasis and function are regulated by complex interactions between
the fibromuscular stroma and secretory epithelium via locally-derived and
systemic paracrine- and autocrine-acting growth factors and sex steroid
hormones. Stromal tissue remodelling due to alterations in transforming growth
factor beta (TGF-b) and sex steroid hormone signalling are associated with
benign prostatic hyperplasia (BPH) and prostate cancer (PCa), two of the most
common proliferative disorders affecting elderly men.
We previously demonstrated that GAGEC1, a member of cancer-testis
associated antigens, is up-regulated in response to TGF-b in in vitro models of
age-associated prostatic stromal remodelling. GAGEC1 expression is restricted to
male and female reproductive tissues and is up-regulated in the prostates of
patients with symptomatic BPH and PCa. Consistent with its restricted expression
profile to classical steroidogenic tissues, GAGEC1 is induced by sex steroid
hormones, particularly oestradiol and dihydrotestosterone. Transiently expressed
recombinant GAGEC1 undergoes constant shuttling between cytoplasmic and
nuclear cell compartments, a process that may be regulated via post-translational
Our data suggest that age/disease-associated changes in TGF-b1 and sex
steroid hormones may account for the reported increase in GAGEC1 expression in
BPH and PCa. Functional analyses indicate that the biological activity of
GAGEC1 is regulated via phosphorylation-dependent nucleo-cytoplasmic
trafficking raising the possibility that GAGEC1 is involved in signal transduction
mechanisms. Given that its expression is restricted in males to the prostate and
testis, GAGEC1 represents a promising target for therapeutic intervention of BPH
and PCa.
Recent reports have revealed that leptin’s effects are not restricted to central
control of body weight, demonstrating instead that leptin is a pleiotropic hormone
with a wide variety of different biological actions. Leptin exhibits undesirable
effects in autoimmune diseases, in atherosclerosis, and possibly in several types of
cancer, and increases the risk of cardiovascular disease in obese people.
Therefore, preparation of reagents capable of abolishing leptin’s action is both
valid and timely.
As no structural information on the 3D structure of leptin receptor (LEPR) is
available, the model of interleukin 6 (IL6) was applied. We identified leptin’s
putative binding site III, which does not affect binding but is necessary for
receptor activation, by modeling LEPR on the basis of its alignment with gp130,
and fitting leptin on IL6 in the IL6/gp130 complex.
Six muteins of human, ovine, rat, and mouse leptins, mutated to Ala in amino
acids 39–41 or 39–42, were prepared by site-directed mutagenesis of the putative
site III, and purified to homogeneity. All muteins had typical cytokine secondary
structure, acted as true antagonists—namely, they interacted with LEPR with an
affinity similar to that of the wild-type hormone (as evidenced by SPR and RRA),
were devoid of biological activity in several leptin-response bioassays, and
specifically inhibited leptin action in vitro and in vivo. These muteins can be
prepared in gram amounts and thus serve as a novel tool for studying leptin
function in vitro and in vivo. To prolong their lives in circulation, some muteins
were pegylated using 40-, 30- and 20-kDa polyethylene glycol. Although
pegylation decreased their in-vitro activity, increasing circulation half-life can
compensate for this deficit in vivo.
Antagonizing leptin has been suggested as a possible therapy in autoimmune
diseases and heart failure. Thus, leptin antagonists not only offer a novel tool to
elucidate the role of leptin in mammalian physiology but have a potential role as a
therapeutic drug.
Normalization of serum testosterone level alters local GnRH-II and IL2R mRNA expression in peripheral lymphocytes in patients with
idiopathic hypogonadotrophic hypogonadism (IHH)
Fatih Tanriverdi1, Hilal Akalin2, Okay Caglayan2, Umit Demirkoparan1,
Yusuf Ozkul2, Munis Dundar2, Fahri Bayram1 & Fahrettin Kelestimur1
Erciyes University Medical School Department of Endocrinology, Kayseri,
Turkey; 2Erciyes University Medical School Department of Genetics,
Kayseri, Turkey.
Although the existence of the interaction between sex steroids and immune
system is well known, the mechanisms of this interaction are still unclear.
Recently a second form of GnRH (GnRH-II) has been described in human,
which is significantly expressed in immune tissues suggesting a potential
function. In a recent in-vitro study it has been demonstrated that GnRH-II
decreases local expression of IL-2R in peripheral lymphocytes (1). However
in-vivo interactions of testosterone, IL-2R and GnRH-II expression at
lymphocyte level have not been investigated yet. Therefore in the present
study we investigated the effects of conventional gonadotrophin therapy on
local GnRH-II and IL-2R expression in peripheral lymphocytes in patients
with IHH.
Fourteen males with IHH (24.5G6.3) and 15 age-sex matched controls
were investigated. Patients were treated with hCG and hMG for 12 months.
Quantitative Real-Time RT-PCR (2 independent repeats) was used to
determine the expression of GnRH-II (target gene), IL-2R (target gene) and
beta-actin (reference gene) in peripheral lymphocytes derived from patients
before and after treatment, and the controls.
Serum testosterone level before treatment in patient group was significantly
low when compared to controls. After gonadotrophin treatment testosterone
level significantly increased. Baseline GnRH-II and IL-2R mRNA levels (%
of the control) were % 1451G300 and % 285G46 in the patient group,
respectively. Significant decrease in GnRH-II and IL-2R mRNA levels were
found after treatment.
In-vivo interactions between testosterone, IL-2R and GnRH-II at lymphocyte level were shown first time in the literature. Present findings clearly
suggest that some immune effects of the sex steroids may occur via regulating
the local GnRH-II and IL-2R expression.
Endocrine Abstracts (2007) Vol 14
Role of soluble Fas-antigen (sFas), interleukin-6 (IL-6) and vascular
endothelial growth factor (VEGF) in adrenocortical carcinoma patients
Nikolai Kushlinsky, Timur Britvin, Irina Kazantseva & Arian Kalinin
Russian N.N.Blokhin Cancer Research Center of RAMS, Moscow, Russia;
M.F.Vladimirsky Moscow Regional Clinical and Research Institute,
Moscow, Russia.
The numerous growth factors and cytokines take part in mechanisms of tumor
growth and metastasing.
The aim of this study was determination of sFas, IL-6 and VEGF serum
levels in 19 patients with adrenal cortical carcinoma (11 women and 8 men
aged 21–72 years). The control group comprised 40 practically healthy donors
(22 women and 18 men aged 19–70 years). sFas, IL-6 and VEGF before
adrenalectomy and in the control were measured by ELISA. Mean IL-6
(4.6 ng/ml) and VEGF (438.7 pg/ml) levels in adrenocortical carcinoma
patients were significantly (PZ0.004) higher than in the control (IL-6 –
1.3 ng/ml, VEGF – 126.5 pg/ml). There was no difference in serum sFas
between patients (2.0 ng/ml) and the control (0.8 ng/ml). sFas, IL-6 and VEGF
were markedly elevated in patients with advanced (III-IV) stages of the
disease as compared to early (I-II) stages. In patients with nonfunctional
adrenal cortical carcinoma, serum level of VEGF (571.9 pg/ml) was
significantly (PZ0.046) higher than that in patients with Cushing’s syndrome
(460.1 pg/ml). No differences in serum sFas and IL-6 levels were revealed
between patients with nonfunctional and hormonally-active tumors. Direct
correlation was found between VEGF and IL-6 (PZ0.56; rZ0.009). 5-year
overall survival (100%) of patients with serum VEGF less then 300 pg/ml was
significantly (PZ0.049) higher compared to patients with serum VEGF
exceeding 300 pg/ml (34.3%). 5-year overall survival didn’t depend on the
pretreatment serum sFas and IL-6 levels.
We suggest that VEGF serum level in adrenal cortical carcinoma patients
may be used as a factor of clinical behaviour and prognosis.
9th European Congress of Endocrinology, Budapest, Hungary, 2007
Rosiglitazone interferes with the inflammatory response induced in
human endothelial cells by TNFalpha and IFNgamma through a new
mechanism involving extracellular signal-regulated kinases (ERKs)
Adriana Lombardi1, Elisabetta Piscitelli1, Michela Francalanci1,
Tommaso Mello1, Veronica Santarlasci2, Stefania Gelmini1,
Giulia Cantini1, Andrea Galli1, Lorenzo Cosmi2, Francesco Annunziato2,
Gianni Forti1, Mario Serio1 & Michaela Luconi1
Dept. Clinical Physiopathology, University of Florence, Florence, Italy;
Dept. Internal Medicine, University of Florence, Florence, Italy.
P!0.05). These associations remained significant after adjusting for age, heart
rate and body surface area.
In conclusion, this study shows for the first time that the GH/IGF-1 axis is
responsible for the RV functional remodeling in high-top rowers, improving
mainly the systolic activity. This effect seems to be primarily modulated by the
IGF-1 overproduction, as a physiological adaptation to prolonged training.
Microvascular endothelium is one of the main character and target involved in the
inflammatory response. Upon specific activation, endothelial cells massively
recruit Th1 IFNgamma secreting lymphocytes at the inflammatory site. In the
present study, we investigate the intracellular signalling mediating TNFalpha (T)
and IFNgamma (I) inflammatory response in a human endothelial cell line
(HMEC-1) in vitro and the interfering effects of rosiglitazone (RGZ), a
peroxisome proliferator-activated receptor (PPARgamma) agonist currently
used in clinical treatment of diabetes mellitus. We show that T and I alone
stimulate interferon gamma-inducible protein-10 (IP-10) secretion by HMEC-1,
effect which is dramatically increased when the two cytokines are used in
combination. IP-10 secretion in response to T, I and RGZ is accompanied by a
re-modulation of surface expression of cell adhesion molecules (CAM), such as
VCAM-1 and ICAM-1. Although these stimulatory effects of T and I are
mediated by a similar rapid increase in phosphorylation/activation of ERK1/2, as
demonstrated by the use of ERK inhibitors, confocal microscopy analysis
suggests that the synergistic action of T and I is partly mediated by a different
subcellular localization of the activated ERKs. Concomitant treatment with RGZ
reverts both activation of ERKs and interferes with IP-10 secretion and CAM
expression elicited by T and I through a novel rapid mechanism not involving
transcriptional activity of PPARgamma, as further confirmed by the inability of
BADGE, an inhibitor of such a transactivational action, to revert RGZ effects. Our
findings shed new light on the molecular mechanisms underlying the
inflammatory response in the endothelium and on the possible therapeutic use
of RGZ in such a process.
This study has been supported by project TRESOR of Region of Tuscany
Role of growth hormone/insulin like growth factor 1 system in the
remodelling process of the right ventricle in top levels rowers
Giovanni Vitale1, Maurizio Galderisi2, Annamaria Colao3,
Pasquale Innelli2, Germano Guerra4, Ermelinda Guerra3, Frank Lloyd Dini5,
Antonio Soscia4, Oreste de Divitiis2 & Gaetano Lombardi3
Chair of Endocrinology, Faculty of Medicine – University of Milan, Istituto
Auxologico Italiano, Milan, Italy; 2Cardioangiology and CCU Division,
Department of Clinical and Experimental Medicine, University of Naples
Federico II, Naples, Italy; 3Department of Molecular and Clinical
Endocrinology & Oncology, University of Naples Federico II, Naples, Italy;
Department of Biomorphological and Functional Sciences, University of
Naples Federico II, Naples, Italy; 5Cardiovascular Diseases Unit 2,
Ospedale Santa Chiara, Pisa, Italy.
The intensive physical activity is often associated with cardiac changes,
particularly involving the right ventricular (RV) chamber. However, the
molecular mechanisms involved in the RV physiologic adaptation to long-term
training are not completely understood. In the present study we investigated the
role of the growth hormone/insulin like growth factor 1 (GH/IGF-1) axis in the
RV remodeling of athletes.
Nineteen male top levels rowers and 19 age-matched healthy sedentary male
controls underwent blood determination of fasting serum GH, IGF-1, IGF binding
protein 3 (IGFBP-3) and acid-labile subunit levels and standard Doppler
echocardiography combined with pulsed Tissue Doppler of RV tricuspid annulus.
Myocardial pre-systolic (PSm), systolic (Sm), early diastolic (Em) and atrial (Am)
velocities as well as myocardial time intervals adjusted for heart rate were
Rowers had serum IGF-1 levels (P!0.05), RV internal chamber size (P!0.05)
and RV wall thickness (P!0.0001) significantly higher than controls.
Additionally, rowers had improved RV systolic (higher tricuspid annular systolic
excursion, higher PSm and Sm velocities; lower myocardial pre-contraction time)
and diastolic function (lower A velocity, shorter deceleration time, isovolumic
relaxation time and myocardial relaxation time; higher E/A ratio, Em and Em/Am
ratio) compared to controls. In the rowers, IGF-1 was associated with PSm
velocity (rZ0.55, PZ0.01) and myocardial pre-contraction time (rZK0.57,
PZ0.01), GH with pre-ejection period (rZK0.50, P!0.05) and Em (rZ0.47,
Clinical significance of simultaneously determined serum interleukin-6,
dehydroepiandrosterone and its sulphate levels in melanoma
Mariann Boldizsár, Borbála Vincze, Katalin Gilde, Teodora Bánfalvi,
Zsuzsanna Fejos, Kinga Borbola, Bence Kapuvári, Gabriella Liszkay &
Szabolcs Otto
National Institute of Oncology, Budapest, Hungary.
Among well-known circulating melanoma markers 5-S-cysteinyldopa (5-SCD), a
precursor of pheomelanin biosynthesis and S-100 beta (S-100B) are extensively
investigated. Our earlier observations confirmed that serum concentration of
5-SCD and S-100B correlates well with the stages and progression of the disease.
Interleukin-6 (IL-6) is a multifunctional inflammatory cytokine implicated in
advanced stage of various diseases and tumour recurrence. Malignant melanoma
cells are known to secrete IL-6. According to the recent reports skin could produce
DHEA and DHEA-S due to the presence of key enzymes. This study was aimed to
establish the significance and the possible relationship among different serum
parameters. In 124 melanoma patients with (nZ63) or without (nZ61) metastasis,
concentrations of IL-6, DHEA, DHEA-S were simultaneously measured in
comparison with the metastatic markers of 5-SCD and S-100B. The presence of
metastasis was verified by conventional imaging techniques. Serum 5-SCD
concentration was determined by high pressure liquid chromatography with
electrochemical detection. Serum levels of IL-6, DHEA, DHEA-S and S-100B
were measured by RIA/IRMA and ILMA methods. For statistical analysis
MedCalc Software was used. In patients with metastases compared to the
metastasis-free cases significant increase in 5-SCD, S-100B and IL-6 serum levels
were observed. On the contrary, significant decrease in DHEAS and DHEA
concentrations was found. Correlations between serum concentrations of 5-SCD
and IL-6 (P!0.0001), as well as DHEA and DHEA-S (P!0.0001) were
significant and Spearman’s coefficient of rank correlation (rho) was 0.69 and 0.71,
respectively. Using multiple regression analysis a negative correlation between IL6 and DHEA or DHEAS levels was found. These results suggest that simultaneous
determination of IL-6, DHEA and DHEA-S together with 5-SCD and S-100B
measured in melanoma patients could be predictive factors of the disease.
This research was supported by the Hungarian Research Fund (OTKA No.
T 049814).
Changes in growth hormone messenger RNA (GHmRNA) expression in
rats anterior pituitary after single Interferon (IFN)alpha
Wojciech Romanowski, Ryszard Braczkowski, Aleksander Danikiewicz,
Ewa Nowakowska-Zajdel, Malgorzata Muc-Wierzgon, Zuzanna Muryn &
Barbara Zubelewicz-Szkodzinska
Dept. of Internal Medicine Bytom, Silesian Medical University, Katowice,
Interferon alpha (IFN alpha) is a cytokine with pleiotropic effects and via different
pathways influences secretion of certain cytokines and hormones. Growth
Hormone (GH) secreted from the pituitary has its physiological effects on various
target tissues. The question is how IFN alpha administered in various type of
diseases influences GH secretion. This study investigated acute effect of IFNalpha on GH mRNA expression in rat anterior pituitary
The aim of the study was to measure the cellular expression of GH mRNA by
in situhybridisation in anterior pituitary after IFN alpha single administration
Material and methods
Rats were administered intraperitoneal injection of IFN alpha or saline. Rat
pituitaries were taken 2 and 4 hours after IFN/saline administration and kept
frozen until in situhybridisation histochemistry. 31–base35S-labelled oligonucleotide probe complementary to part of the exonic mRNA sequences coding for GH
mRNA was used. All control and experimental sections were hybridised in the
same hybridisation reaction
Endocrine Abstracts (2007) Vol 14
9th European Congress of Endocrinology, Budapest, Hungary, 2007
Interferon a acute administration increases GH mRNA expression in the anterior
pituitary in 4 hours group in comparison to the control group, and there was no
difference between control group and 2-hours rats.
The influence of single IFN alpha administration on anterior pituitary GH mRNA
expression has been found. These observations may pave the way for presenting a
new possible IFN alpha action.
Does stress test influence Interleukin (IL)-2 and IL-8 concentration in
serum patients with stable ischaemic heart disease?
Wojciech Romanowski1, Janusz Szkodzinski2, Andrzej Kaszuba1,
Adam Blazelonis1, Zuzanna Muryn1, Pietka-Rzycka Anna1 &
Barbara Zubelewicz-Szkodzinska1
Dept. of Internal Medicine Bytom, Silesian Medical University, Katowice,
Poland; 2Silesian Center for Heart Diseases, Zabrze, Poland.
There is growing evidence that adhesion molecules, proinflammatory cells and
cytokines play an important role in a variety of cardiac pathophysiological
conditions; Cytokines are responsible for the modulation of immune and
inflammatory processes. It has been suggested that cytokines such as IL-1, IL-2,
IL-6, IL-10 and TNF alpha are important modulators of atherosclerotic effects
with IL-2 and Interferon g having a proinflammatory atherogenic effect and IL-8
and IL-10 having an anti-inflammatory protective role. Atherosclerotic lesions in
the coronary vessels are heavily infiltrated by cellular components associated with
inflammation (macrophages/monocytes, t-lymphocytes, eosynophils and
NK-cells). These cells are also a source of cytokines and that is why the
Objective of the present study was to measure IL-2 and IL_8 concentration in
serum patients with stable ishaemic heart disease (i.h.d.).
Patients and method
26 patients (11 women, 15 men) age 47–65 years with diagnosed stable ischaemic
heart disease were included into study. The control group consists of 20 patients
matched with age and sex. All patients from examined group fulfilled the
inclusion criteria (stable i.h.d. with standard treatment, rest ECG without
ischaemic changes and with coronary sufficiency belongs to I or II class of CCS(Canadian Cardiovascular Society scale).The exclusion criteria were typical for
the study concerns cytokines.
In all patients we have measured the concentration of IL-2 and IL-8 concentration
in serum by ELISA using R&D System kits
Additionally, patients with diagnosed i.h.d. had IL-2 and IL-8 concentration
measured after the stress test done to assume the cardiac sufficiency in that group.
Concentration of IL-2 and IL-8 in patients with i.h.d. is significantly higher then
in the control group (P!0.05). After stress test in i.h.d. patients there were no
significant changes of IL -2 concentration (PZ0.054) and increase of IL-8 (P!
0.001) concentration observed.
Concentration of inflammatory factors such as CRP (acute phase
response protein) and Interleukin (IL)-6 in serum patients with stable
ischemic heart disease during trimetazidine treatment
Janusz Szkodzinski1, Marek Szewczyk2, Wojciech Romanowski2,
Aleksander Danikiewicz2, Malgorzata Muc-Wierzgon2 &
Barbara Zubelewicz-Szkodzinska2
Dept. of Internal Medicine Bytom, Silesian Center for Heart Diseases,
Zabrze, Poland; 2Silesian Medical University, Katowice, Poland.
The patomechanism of developing ischemic heart disease (i.h.d.) is stenosis
of coronary blood vessels with plaque placed on vascular endothelium built
with monocytes/macrophages, foam cells, oxidized LDL, leukocytes,
platelets and collagen. Atherosclerotic lesions are heavily infiltrated by
cellular components associated with inflammation and influenced by other
inflammatory factors. Trimetazidine, a clinically effective antianginal agent
Endocrine Abstracts (2007) Vol 14
acts by optimizing cardiac energy metabolism through inhibition of free
fatty acid oxidation.
Up to now there have been no study associating trimetazidine possible
anti-inflammatory effect which could be a result of trimetazidine influence
on granulocytes in-flow to ischemic region and atherosclerotic plaque and in
consequence influence on granulocyte products such as cytokines and other
inflammatory predictors.
The aim of the study was to determine if trimetazidine treatment in stable
ischemic heart disease altered the concentration of certain inflammatory factors
such as CRP (acute phase response protein) and Interleukin (IL)-6.
Patients and method
26 patients (11 women, 15 men) age 47–65 years with diagnosed stable
ischemic heart disease were included into study. All of them fulfilled the
inclusion criteria (stable i.h.d. with standard treatment, rest ECG without
ischemic changes and with cardiac sufficiency belongs to I or II class of CCS(Canadian Cardiovascular Society scale).
All patients have measured the concentration of Il-6 and CRP at the onset of
trimetazidine treatment and 3 months after. Il-6 concentration has been
measured by ELISA using R&D System kits and CRP concentration by
immunoturbidometric method.
3-months trimetazidine treatment caused significant decrease of CRP
concentration in serum of patients with stable i.h.d. (P!0.001) and significant
increase of IL-6 concentration (P!0.05).
Decrease of CRP concentration in serum after 3 months of trimetazidine
treatment could be due to trimetazidine hepatoprotective properties. An increase
of Il-6 concentration after 3 months of treatment with trimetazidine is possibly a
result of different mechanism of its action.
Insulin decreases IGF-I bioactivity in patients with impaired glucose
tolerance and in healthy subjects
Ayman M Arafat1, Jan Frystyk2, Martin O Weickert1, Joachim Spranger1,
Christof Schöfl1 & Mathias Möhlig1
Department of Endocrinology, Diabetes and Nutrition, Charité-University
Medicine Berlin, Campus Benjamin Franklin and the German Institute of
Human Nutrition Potsdam-Rehbruecke, Berlin, Germany; 2Medical
Research Laboratories and Medical Department M, Aarhus University
Hospital, DK-8000 Aarhus C, Denmark.
Insulin resistance (IR) is a very common metabolic abnormality in obesity, which
is often associated with reduced growth hormone (GH) secretion. GH deficiency
is associated with increased in intra-abdominal fat and several parameters of the
metabolic syndrome. IGF-I improves IR but the IGF-binding proteins are
supposed to regulate its bioactivity although only little information exists. We
postulated that the elevated insulin levels due to IR do not only suppress GH but
also IGF-I bioactivity, and therefore we tested the effect of insulin on serum levels
of bioactive IGF-I.
24 healthy subjects (12 men; age 21–72 years; BMI 25.9G0.9 kg/m2) and 19
patients with impaired glucose tolerance (IGT; 8 men; age 26–71; BMI 28.9G
1.2) were studied using an OGTT and a hyperinsulinemic euglycemic clamp. IR
was estimated by calculating the homeostatic model assessment (HOMA-IR)
index and the glucose infusion rate (GIR). IGF-I bioactivity was estimated using a
novel IGF-I kinase receptor activation assay (KIRA) under fasting conditions and
during the steady state of the clamp. Ethical Committee approval was obtained.
Insulin significantly decreased IGF-I bioactivity in IGT patients (1.8G0.2 vs.
1.5G0.2 mg/l, PZ0.004) and in healthy controls (1.8G0.2 vs 1.6G0.2 mg/l, PZ
0.001). Age, BMI and fasting IGF-I bioactivity did not significantly differ
between groups. However, patients with IGT showed a higher HOMA-IR and a
lower GIR (2.3G0.4 vs. 1.3G0.2 and 2.5G0.3 vs. 4.7G0.3 mg/kg min, P!0.05,
respectively). Moreover, inverse correlations were seen between bioactive IGF-I
levels and age (rZK0.38, PZ0.01), BMI (rZK0.46, PZ0.002) and waist to hip
ratio (rZK0.51, PZ0.01).
Our data indicate that insulin infusion acutely decreased serum IGF-I
bioactivity in humans. Hyperinsulinemia as seen in IR may per se be
responsible for this reduction. Estimation of IGF-I bioavailability using the
KIRA method may, therefore, have a predictive value in the diagnosis of the
metabolic syndrome.
9th European Congress of Endocrinology, Budapest, Hungary, 2007
Plasma free fatty acids and adipocytokines concentration in relation to
insulin sensitivity in patients with anorexia nervosa.
Monika Karczewska-Kupczewska, Irina Kowalska, Marek Straczkowski,
Agnieszka Adamska, Agnieszka Nikolajuk, Malgorzata KarolczukZarachowicz, Elzbieta Otziomek & Maria Gorska
Department of Endocrinology, Diabetology and Internal Medicine, Medical
University of Bialystok, Bialystok, Poland.
Anorexia nervosa (AN) is an eating disorder, resulting in sustained low weight. In
AN, similarly to syndromes of lipodystrophy, one observes the significant loss of
the adipose tissue. In lipodystrophies, despite the lack of subcutaneous adipose
tissue, insulin resistance is observed. Adipose tissue is known as a source of a
variety of bioactive peptides, known as adipocytokines. The aim of the present
study was to examine the plasma concentration of adipocytokines in relation to
insulin sensitivity in women with AN.
The study group consisted of 16 women with AN, 16 women with obesity
and 18 healthy normal weight female controls. The oral glucose tolerance test
and euglycemic hyperinsulinemic clamp were performed in all the patients.
The plasma concentrations of adiponectin, TNF-a, soluble TNF-a receptors
(sTNFR1, sTNFR2) and IL-6, soluble form of IL-6 receptor (sIL-6R) were
Insulin sensitivity index (M) was not different in AN and healthy controls,
but was significantly increased in AN in comparison to obese women (PZ
0.002). Adiponectin plasma levels were significantly higher in AN than
control subjects and obese women (PZ0.01, PZ0.003, respectively). There
were no differences in plasma concentrations of TNF-a, sTNFR1, sTNFR2,
IL-6, sIL-6R among groups, however plasma free fatty acids (FFA) were
significantly lower in AN than control subjects and obese women (PZ
0.00003, PZ0.00001, respectively). Adiponectin levels were negatively
correlated with BMI (rZK0.40, PZ0,005) and waist girth (rZK0.44, PZ
0.002). Fasting FFA concentrations were related negatively to insulin
sensitivity (rZK0.55, PZ0.00007) and to adiponectin concentrations
(rZK0.34, PZ0.026).
Our data show that lack of adipose tissue observed in anorectic patients has
no influence on insulin sensitivity, probably due to low plasma FFA
concentration. It points out that in AN the adipocytes are still capable of
functioning at the level that is sufficient to prevent the metabolic
Improved glucose metabolism and altered pancreatic structure in
transgenic mice overexpressing betacellulin
Maik Dahlhoff1, Nadja Herbach2, Rüdiger Wanke2, Eckhard Wolf1 &
Marlon R. Schneider1
Institute of Molecular Animal Breeding and Biotechnology, University of
Munich, Munich, Germany; 2Institute of Veterinary Pathology, University
of Munich, Munich, Germany.
Betacellulin, one of several peptides activating the EGFR (ErbB1) and related
receptors, is a multipotent growth factor known to posses the unique ability to
promote growth and differentiation of pancreatic b-cells.
We investigated the effects of betacellulin overexpression in a recently
established transgenic mouse model (Schneider et al., Endocrinology 146,
5237–5246, 2005). In transgenic animals, overall glucose metabolism was
improved as demonstrated by reduced blood glucose levels in fasted animals
and a better response after a glucose tolerance test (associated with increased
serum insulin levels). Unexpectedly, the absolute and relative (proportional to
body weight) pancreas weights were significantly reduced in transgenic mice.
Histomorphometrical analyses revealed a reduction in the volume of the
exocrine pancreas while the islet and b-cell volume remained unchanged. This
resulted in an increase in the relative volume of the latter compartments.
Interestingly, the proportion of b-cells within the islets remained unchanged
in betacellulin transgenic mice. While betacellulin is normally expressed in
the islets, immunohistochemistry revealed that the growth factor is, in
addition, strongly expressed in the exocrine pancreas in transgenic mice. This
uncovers a hitherto unknown negative effect of betacellulin in the exocrine
compartment. Finally, we identified, by immunohistochemistry, an opposite
expression pattern of ErbB1 and ErbB4, the primary receptors for
betacellulin, in the pancreas. In this organ, ErbB1 is expressed predominantly
in the islets, while ErbB4 expression is mostly restricted to the exocrine
compartment. Thus, this particular receptor distribution may provide an
explanation for the opposing effects exerted by betacellulin in the different
pancreatic compartments.
Current experiments involve the study of cell proliferation and apoptosis as well
as functional studies on isolated islets including insulin content and release.
Screening of 120 adipokines in subcutaneous adipose tissue of patients
with growth hormone deficiency reveals changed protein levels
Daniela Gasperikova1, Jozef Ukropec1, Adela Penesova1, Henrike Sell2,
Martina Skopkova1, Miroslav Vlcek1, Zofia Radikova1, Juraj Koska1,
Vitazoslav Belan3, Mikulas Pura4, Peter Vanuga4, Juraj Payer5,
Jurgen Eckel2 & Iwar Klimes1
Institute of Experimental Endocrinology, Bratislava, Slovakia; 2German
Diabetes Center, Dusseldorf, Germany; 3Department of Radiology, Faculty
Hospital, Bratislava, Slovakia; 4National Institute for Endocrinology and
Diabetes, Lubochna, Slovakia; 5V. Clinic of Internal Medicine, Faculty
Hospital, Bratislava, Slovakia.
The role of adipokines and inflammatory cytokines of adipose tissue for
development of the growth hormone deficiency (GHD)-related metabolic
derangements has not yet been completely understood. Therefore, we screened
the protein level of 120 adipokines in subcutaneous adipose tissue (ScAT) of
patients with GHD in adulthood.
Subjects and methods
Sixteen GHD (10M/6F) with BMI 27G1.0 kg/m2, age 30G2 yrs and sixteen
controls matched for BMI, sex and age were included into the study. ScAT
biopsies were performed after an overnight fast. Protein expression of adipokines
was determined in tissue lysates using the RayBiowHuman Cytokine Antibody
Array C Series 1000.
GHD subjects had higher waist circumference, circulating hsCRP levels and
impaired glucose tolerance (as assessed by oGTT) (P!0.05). From 120 proteins,
one showed to have higher (IGFBP-1) and three (BDNF, NT-3, SDF-1) lower
levels in ScAT of the GDH subjects in comparison with controls (P!0.05).
Majority of the observed changes were related to waist circumference, as became
evident when we had separated individuals of both groups according to the IDF
criteria (menR94 cm and femaleR80 cm). Interestingly, CNTF, EGF, GDNF,
IL-1a, MIP3A, TGFb1 and GCP2 were elevated, and GM-CSF lowered in
parallel with increasing waist circumference selectively in the GHD individuals.
On the other hand, HGF and TIMP2 were elevated while IL-7, MIP-3A, GITR,
IGF1 SR, IL-17, IL-2Ra, MIP1b and Oncostatin M lowered with increasing waist
circumference only in the controls.
Our data provide the first information on specific changes in the ScAT adipokine
protein levels in GHD adults. Moreover, they implicate a different regulation of
cytokine ScAT levels in a comparable inflammatory setting, i.e. in equally obese
subjects who differ in their metabolic status.
Supported by APVV-51-0406/02 and Slovak Diabetes Association. The study
was approved by the local Ethics Committee and conforms to the ethical
guidelines of the Helsinki Declaration.
Human somatotrophic (GH) adenoma cells – interleukin (IL)-1b
induces production of il-6 and il-8.
Signe Diness1, Åse Krogh Rasmussen1, Klaus Bendtzen2,
Michael Kosteljanetz3 & Ulla Feldt-Rasmussen1
Department Of Medical Endocrinology, Copenhagen University Hospital,
Copenhagen, Denmark; 2Institute Of Inflammatory Research, Copenhagen
University Hospital, Copenhagen, Denmark; 3Department Of Neurosurgery,
Copenhagen University Hospital, Copenhagen, Denmark.
to establish a human in vitro system for the study of pituitary cells in culture and
subsequently to study the influence of the pro-inflammatory cytokines interleukin
(IL)-1b and tumour necrosis factor (TNF)-a on the function of the somatotrophic
cells inclusive the ability of the cells to produce IL-6 and IL-8.
Pituitary adenomas were obtained from hypophysectomies of patients with
acromegaly. The tissue was enzymatically digested and cultured in 24-chamber
polystyrene plates in medium supplemented with nutritional factors and
Endocrine Abstracts (2007) Vol 14
9th European Congress of Endocrinology, Budapest, Hungary, 2007
antibiotics and with 105 cells per well. GH and cytokines were measured in the
harvested supernatants.
GHRH (GH releasing hormone) (30,000 ng/ml) stimulated significantly 72 h GH
production from the somatotrophic cells (25% (10–50), median (range), nZ12
chambers, P!0.05) compared to controls (3525 mU/l (49-17450)), while
somatostatin (0.1–10,000 ng/ml) inhibited the 72 h GH production from the
cells compared to controls (P!0.05, nZ12–18). The GH production was
significantly lower in cells cultured more than 15 days compared to younger cell
cultures (!15 days). IL-1b (1000 and 100 pg/ml) stimulated modestly the 72 h
GH production from the cells compared to controls (20% (10–50), nZ18) and
(15% (10–60), nZ18), while TNF-a had no influence the function of the cells.
The effect of IL-1b was reversible. IL-1b (10,000, 100, 10 pg/ml) also stimulated
72 h IL-6 and IL-8 production from the cells. IL-1b (10,000 pg/ml) induced a
mean 12.3 and 8.2-fold increase in IL-6 and IL-8, respectively compared to
control (mean 1472 pg/ml and 1948 pg/ml, respectively) in 4 different cultures.
We have established a robust in vitro system for studying the function of GH
producing pituitary cells; GH production from the cells exhibited the expected
responses to GHRH and somatostatin. IL-1b further stimulated the release of IL-6
and IL-8 from the cells, an effect that has been established also in other endocrine
cells such as e.g. thyrocytes. The physiological and/or pathophysiological roles of
these findings remain to be shown.
designed to investigate whether serum resistin concentrations constitute a
significant coronary risk factor, with a particular focus on diabetes and one of its
microvascular complications; nephropathy.
Serum resistin was measured in 86 overweight patients with acute coronary
syndrome (ACS) and 16 overweight healthy controls. Patients were divided into two
groups according to presence or absence of diabetes: IHD with diabetes (nZ46), and
IHD without diabetes (nZ40). In addition, patients with diabetes were subdivided
into two groups: diabetics with microalbuminuria (nZ26) and without (nZ20).
Non-diabetic IHD patients had a significantly higher level of serum resistin when
compared to control participants (15.3G13 vs 6.3G2.7 ng/ml, PZ0.008). IHD
patients with diabetes had a significantly higher level of serum cholesterol, LDL
and resistin compared to IHD patients without (204G43 vs 181G31 mg/dl, PZ
0.048), (129G36 vs 111G23 mg/dl, PZ0.048) and (41G33 vs 15.3G13 ng/ml,
PZ0.002) respectively. Working on diabetic patients, the only significant
difference between patients with microalbuminuria and those without is serum
resistin concentration (55G37 vs 23G14 ng/ml, PZ0.011). Pearson correlations
including all subjects showed that serum resistin concentration had a significant
positive correlation with both total serum cholesterol (rZ270, PZ0.05) and serum
LDL (rZ313, PZ0.026).
This study showed that serum resistin concentration is associated independently
with coronary atherosclerosis in overweight patients. Serum resistin is increased in
patients with diabetes mellitus particularly those with microalbuminuria.
Diabetes and cardiovascular – presented on Sunday
Serum ferritin concentrations in an impaired fasting glucose population
and their normal control group
Faranak Sharifi, Yahya Jaberi & Nuraddin Mousavinasab
Zanjan University of Medical Sciences, Zanjan, Iran.
Some recent studies have revealed the relationship among excess ferritin,
coronary heart disease, and insulin resistance. To assess the association between
serum ferritin concentration and Impaired Fasting Glucose, a prediabetes
situation with insulin resistance, this study was designed in Zanjan, Iran.
Materials & Methods
187 people including 91 impaired fasting glucose (IFG) subjects and 96 normal
glucose subjects who had been recognized in a large epidemiological study in
Zanjan in 2001 were enrolled. The cohorts were well matched for age, sex and
BMI. Body mass index and blood pressure of the participants were measured and
serum cholesterol, triglyceride and ferritin were evaluated. All the data were
analyzed by t-test, x2 test and analysis of variance.
Serum ferritin was higher in the IFG cohort (85.5G6.6 mg/l vs. 49.4G3.7 mg/l, P:
0.001). A positive correlation was found between fasting plasma glucose and
serum ferritin in this study (r: 0.29, P: 0.001). Using multiple regression analysis,
we found an association between serum ferritin and BMI (0.06, P:0.4), blood
pressure (0.15, P:0.01), FPG (0.29, P:0.001), triglyceride(0.08, P:0.01) and
cholesterol(0.07, P:0.03). The odd’s ratio for the association of IFG in male
subjects with the high serum ferritin level was 8.3 (C.I 95%:1.2–11.9, P:0.01) and
for females was 3.06 (C.I 95%:0.58–15, P:0.1).
Our study, implying that hyperferritinemia occurs before elevation of plasma
glucose concentration more than 126 mg/dl. If prospective and interventional
studies Confirm an etiologic role of iron overload in the pathogenesis of insulin
resistance and type 2 diabetes, reduced dietary iron intake, especially in men with
additional risk factors for type 2 diabetes, would appear to be a logical
The protective effect of tribulus terrestris in diabetes
Amr Amin, Mohamed Lotfy & Ernest Adeghate
UAE Universiy, Al-Ain, United Arab Emirates.
Tribulus terrestris (TT) is used in the Arabic folk medicine to Q1 treat
various diseases. The aim of this study was to investigate the protective
effects of TT in diabetes mellitus (DM). Diabetes is known to increase
reactive oxygen species (ROS) level that subsequently contributes to the
pathogenesis of diabetes. Rats were divided into six groups and treated with
either saline, glibenclamide (Glib), or TT for 30 days. Rats in group 1 were
given saline after the onset of streptozotocin (STZ)-induced diabetes; the
second diabetic group was administered Glib (10 mg/kg body weight). The
third diabetic group was treated with the TT extract (2 g/kg body weight),
while the first, second, and third nondiabetic groups were treated with saline
solution, Glib, and TT extract, respectively. At the end of the experiment,
serum and liver samples were collected for biochemical and morphological
analysis. Levels of serum alanine aminotransferase (ALT) and creatinine were
estimated. In addition, levels of malonyldialdehyde (MDA) and reduced
glutathione (GSH) were assayed in the liver. The tested TT extract
significantly decreased the levels of ALT and creatinine in the serum (P!
0.05) in diabetic groups and lowered the MDA level in liver (P!0.05) in
diabetic and (P!0.01) nondiabetic groups. On the other hand, levels of
reduced GSH in liver were significantly increased (P!0.01) in diabetic rats
treated with TT. Histopathological examination revealed significant recovery
of liver in herb-treated rats. This investigation suggests that the protective
effect of TT for STZ-induced diabetic rats may be mediated by inhibiting
oxidative stress.
Implications of serum resistin in overweight diabetic patients with
ischemic heart disease
Azza Farrag, Sameh Salama & Amal Rizk
Cardiology Department, Cairo University, Cairo, Egypt; Cardiology
Department, Cairo University, Cairo, Egypt; Critical Care Medicine, Cairo
University, Cairo, Egypt.
Resistin is a recently discovered adipocyte-secreted hormone that links obesity
with insulin resistance and/or metabolic and cardiovascular risk. This study was
Endocrine Abstracts (2007) Vol 14
Prevalence of I27L polymorphism of hepatic nuclear factor-1[alpha] in
diabetic patients younger than 35 years old.
Norma Amador, Manuel López, Jose Sánchez, Juan Guı́zar,
Alejandra Zapién & Silvia Martı́nez
Mexican Institute Of Social Security, Leon/Guanajuato, Mexico.
In last decades prevalence of type 2 diabetes mellitus (DM) in children and young
people worldwide has been reported increase. It is necessary to know according to
biochemical and genetic characteristics the frequency of DM no corresponding to
type 1 in our population. The objective of this study was to determine the
prevalence of mutations on hepatic nuclear factor 1 [alpha], and 4 [alpha] in
9th European Congress of Endocrinology, Budapest, Hungary, 2007
diabetic patients younger than 35 years old with features of clinical autosomal
dominant inheritance.
Material and Methods
The study included 140 diabetic patients (85 children and 55 young adults). It was
approved by the local Ethical Committee. Glucose, C peptide, and b-cell
autoantibodies measurements were performed. Polymorphisms of HNF [1 alpha]
(I27L, G319S), and HNF [4 alpha] (T130I) were determined in all patients, when
one of the polymorphisms was identified in a patient, all his/her family was
studied by genetic evaluation.
More than 50% patients showed overweight or obesity. The presence of DM in the
father, overweight, and C peptide levels were higher in adults, while obesity,
hypercholesterolemia, and b-cell autoantibodies were more frequent in those
patients younger than 18 years old. Forty one (29.2%) patients showed the I27L
polymorphism (24-Ile27Leu and 17-Leu27Leu). These patients were older, had
higher BMI and C peptide levels than Ile27Ile patients, and only 3 of them showed
b-cell autoantibodies. In 5 patients we identified Thr130Ile, and in one Gly319Ser
polymorphisms. I27L mutation was present in 30 families and T130I in one
family. Patients in these families were older and showed higher BMI and C
peptide levels, but lower glucose levels.
I27L polymorphism was present in almost a third part of diabetic patients
with clinical autosomal dominant inheritance of the disease. These patients
showed clinical and biochemical characteristics of DM no corresponding to
Type 1 DM.
that it is possible to prevent and minimize type 2 diabetes complications if it
is treated appropriately over time. In our Hospital there is, since 1998, an
outpatient clinics of diabetes. This study aimed to determine the quality of
care provided to diabetic patients in our institution.
Subjects and methods
We reviewed the medical records of 776 diabetic patients, receiving care at our
outpatient clinics since 1998.
A total of 588 patients were included in the study, 58% were men with a
mean age of 66.8G27.2. HbA1c levels averaged 7.2G1.65. 25.3% met the
target blood pressure of 130/80 mmHg; 48% met the goal LDL cholesterol
level !100 and 80% !130 mg/dl. 6.8% of patients met the combined ADA
goal for BP, LDL and HbA1c. Concerning therapeutic regimens: 71.5% used
oral hypoglycaemic agents (OAD) alone (52.1% of these were using 2 or
more agents); 28.5% were treated with insulin (16.2% in combination with
HbA1c values reflects a good metabolic control. We emphasise the
importance of combined therapy in the achievement of optimal glycaemic
levels.The percentage of patients treated to the recommended BP of
130/80 mmHg is consistent with the results of other studies. LDL cholesterol
levels compares favourable to the NHANES III study and is comparable with
other published data. Despite the proved benefits of CV risk factors control in
diabetic patients, international recommendations are difficult to achieve in
clinical practice.
Novel mechanism of chronic exposure of oleic acid-induced insulin
release impairment in rat pancreatic b-cells
Takanori Kudo1, Yoshiji Ogawa1, Sechiko Suga2, Ken Tomotsune1,
Noriyuki Hasegawa1, Toshihiro Suda1 & Makoto Wakui3
Third Department of Internal Medicine, Hirosaki University School of
Medicine, Hirosaki, Aomori, Japan; 2Center for Education and Research of
Lifelong Learning, Hirosaki University, Hirosaki, Aomori, Japan; 3Division
of Clinical Research, Hirosaki National Hospital, Hirosaki, Aomori, Japan.
A sustained, high circulating level of free fatty acids (FFAs) is an important risk
factor for the development of insulin resistance, islet beta-cell dysfunction, and
pathogenesis of type 2 diabetes. Here, we report a novel mechanism of chronic
exposure of oleic acid (OA)-induced rat insulin release impairment. Following a
4-day exposure to 0.1 mM OA, there was no significant difference in basal insulin
release when comparing OA-treated and untreated islets in the presence of 2.8 mM
glucose, whereas 16.7 mM glucose-stimulated insulin release increased 2-fold in
control, but not in OA-treated, islets. Perforated patch-clamp recordings showed
that untreated beta-cells exhibited a resting potential of K62.1 C/K0.9 mV
and were electrically silent, whereas OA-treated beta-cells showed more positive
resting potentials and spontaneous action potential firing. Cell-attached singlechannel recordings revealed spontaneous opening of ATP-sensitive potassium
(K(ATP)) channels in control, but not in OA-treated, beta-cells. Inside-out excised
patch recordings showed similar activity in both OA-treated and untreated betacells in the absence of ATP on the inside of the cellular membrane, whereas in the
presence of ATP, K(ATP) channel activity was significantly reduced in
OA-treated beta-cells. Electron microscopy demonstrated that chronic exposure
to OA resulted in the accumulation of triglycerides in beta-cell cytoplasm and
reduced both the number of insulin-containing granules and insulin content.
Collectively, chronic exposure to OA closed K(ATP) channels by increasing the
sensitivity of K(ATP) channels to ATP, which in turn led to the continuous
excitation of beta-cells, depletion of insulin storage, and impairment of glucosestimulated insulin release.
Quality of care in a diabetic outpatient clinic
Ema Lacerda Nobre, Paula Chambel, Andreia Domingues, Marlene Paes da
Silva, Zulmira Jorge, Valentim Santos, Joaquim Raimundo & João
Jácome de Castro
Hospital Militar Principal, Lisboa, Portugal.
Background and aims
Type 2 Diabetes Mellitus affects a growing number of people allover the
world. It is associated with serious complications. Several studies have shown
Cardiovascular risk factors (CVRF) as predictors of microalbuminuria
(MA) in type 2 diabetes mellitus (T2DM) patients
Francisco Javier del Cañizo-Gomez1 & Maria Natividad Moreira-Andres2
Hospital Virgen de la Torre, Madrid, Spain; 2Hospital Universitario 12 de
Octubre, Madrid, Spain.
MA is a marker of greatly increased cardiovascular morbidity and mortality in
T2DM patients.
To perform a prospective study of normoalbuminuric T2DM patients, analysing
the association between CVRF at baseline and the development of MA at followup.
Materials and methods
The prospective observational study was performed at Montes de Barbanza
public health center, a specialized secondary referral center, which provides
services to the 31 urban district of Madrid, Spain, and consisted in 348
T2DM patients. The inclusion criterion at baseline in 2002 was
normoalbuminuria (urine albumin !30 mg/24 h.), and the exclusion criteria
were previously diagnosed micro or macroalbuminuria or nephropathy. The
clinical end-point was MA (urine albumin 30–300 mg/24 h.) at follow-up in
2005. The variables at baseline in 2002 were age, gender, onset-age of
T2DM, HbA1C, systolic (SBP) and diastolic blood pressure (DBP), total
cholesterol (TCh), HDL-Ch, LDL-Ch, triglycerides (TGs), BMI and smoking;
and were obtained from our records. Diagnosis of MA was made by two
consecutive quantitative test of urine collected over 24 h. Comparison of
mean levels were performed with the Student’s “t” test for unpaired
samples, and proportions with the chi-square test. Logistic regression
analyses were performed with MA as a dependent variable, and age,
gender, diabetes duration, and other CVRF as independent variables. An
odds ratio (OR) O1.0 signifying a positive association, and P!0.05 was
considered significant (SPSS, v. 13.0).
Compared to those who still had normoalbuminuria at follow-up, the ones
progressing to MA were males (PZ0.000), and more likely to have a higher SBP
(PZ0.001) and TGs (PZ0.005), and a lower HDL-Ch (PZ0.002). The principal
independent CVRF at baseline for the development of MA at follow-up were
male gender (OR:3.36; PZ0.000), elevated TGs (OR:2.17; PZ0.005) and
increased SBP levels (OR:1.03; PZ0.001).
Male gender, elevated TGs and increased SBP, were independent CVRF for the
development of MA in T2DM patients of the population studied. Other CVRF, as
decreased HDL-Ch, was associated to MA in T2DM patients
Endocrine Abstracts (2007) Vol 14
9th European Congress of Endocrinology, Budapest, Hungary, 2007
The prevalence of metabolic syndrome and its relation to metabolic
control in patients with diagnosed type 2 diabetes
Florian Toti1, Gazmend Bejtja2, Kliti Hoti1, Eduart Shota1 &
Erion Thengjilli2
UHC “Mother Theresa” Service of Endocrinology & Metabolic Diseases,
Tirana, Albania; 2Institute of Public Health, Tirana, Albania.
Background and Aims
The identification of metabolic syndrome (MS) is important so that components
of this syndrome can be managed appropriately to prevent or delay progression of
associated cardiovascular risk factors. The aim of our study was to determine the
prevalence of the Metabolic Syndrome as the NCEP/ATP III criteria in a selected
population of type 2 diabetes from the Tirana Register of Diabetes.
Materials and Methods
In Tirana district we randomly selected 300 patients from the Tirana Register of
Diabetes. 220/300 (73.3%) of the patients responded. All the patients had
completed anthropometric measures and lipid profile after an 8-hour fast. All the
patients having three or more of the criteria were defined as having Metabolic
Syndrome (MS).
The prevalence of the MS was 64.5%, in men 56.8% and 75.7% for women. The
prevalence increased with age, from 16% before 40 years of age to 78% after 70
years. Diabetes duration was not different in patients with MS than those without
it (M: 6.7G3.4 vs 6.9G3.7; F: 7.2G3.8 vs 6.8G3.6 yrs). The number of
components of the MS was related to the age (ANOVA P!0.05) but not to
diabetes duration. Central obesity was present to 36% of men and 85.4% of
women, HTA 49.6 and 60.2%, low HDL 52 and 90%, high triglycerides 70.9 and
66.7% respectively. HbA1c was higher in persons with MS (9.6G2.2 vs 8.7G
1.4%, P!0.01).
The results show that MS is two-fold more prevalent in type 2 diabetes, compared
with the general albanian population (64.5 vs 32%). The levels of cardiovascular
risk factors are increased in type 2 diabetics and urged immediate efforts directed
at controlling the components (mainly obesity, physical inactivity and lipid
control) of MS especially in type 2 diabetes.
Effects of rosiglitazone (RGZ) and pioglitazone (PGZ) on serum
androgens and urinary steroid profile in patients with type 2 diabetes: A
prospective, randomised cross-over study
Bernard Chappuis, Monika Braun, Christoph Stettler, Peter Diem &
Emanuel Christ
Department of Endocrinology; Diabetology and Clinical Nutrition,
University Hospital of Bern, Inselspital, Bern, Switzerland.
Glitazones (GZ) influence androgen biosynthesis in PCO syndrome. At present it
is unknown whether a) steroid hormone metabolism is influenced by GZ in
patients with type 2 diabetes b) there is a differential effect of RGZ and PGZ on
steroid hormone metabolism c) this effect is sex-specific and d) this effect is
mediated by changes in insulin sensitivity. Therefore, urinary steroid profiles and
serum total testosterone and DHEA levels were analysed before and after therapy
with RGZ and PGZ in patients with type 2 diabetes.
17 patients with type 2 diabetes (7 women, 10 men, age: 60.8G9.6, years,
meanGSD; BMI: 29.2G4.7, kg/m2; HbA1c: 7.6G0.6%) were included in the
study and assigned to RGZ or PGZ in a randomised cross-over study design for 12
weeks with an eight-week wash-out period in-between. Identical investigations
(24-h-urinary steroid profile, plasma glucose (FPG), insulin (FI), HbA1C, serum
total testosterone and DHEA concentrations) were performed before and after
each treatment period.
RGZ and PGZ therapy resulted in a similar decrease in HbA1C, FPG and FI
concentrations without sex-specific differences. In men, RGZ resulted in a
significant increase in serum testosterone levels compared to PGZ (RGZ:
C2.5G2.1; nmol/L; meanGSD; PGZ: C0.5G3.3; P!0.04), whereas DHEA
concentrations remained unchanged. In men changes of urinary androstentriol,
an androgen precursor, were significantly different after RGZ compared to
PGZ (RGZ: C45.7G158.1; mcg/24 h; PGZ: K119G161.1; P!0.05). In
women, RGZ therapy resulted in a significant decrease in serum testosterone
concentrations after RGZ compared to PGZ (RGZ: K0.3G0.3; nmol/L; PGZ:
C0.3G0.4; P!0.05). Serum DHEA levels were unaffected by PGZ and
Endocrine Abstracts (2007) Vol 14
RGZ. In women, there were similar effects of PGZ and RGZ on urinary
androgen metabolites.
These data suggest that 1. GZ impact on steroid hormone synthesis, 2. there is a
differential effect of RGZ and PGZ 3. this effect is sex-specific and 4. this effect is
not mediated by a differential effect of RGZ
Abnormal glucose challenge test reflects mild gestational diabetes
Ayse Kafkasli2, Ayse Sertkaya Cikim1, Engin Burak Selcuk3,
Kezban Dogan2, Feza Burak5 & Saim Yologlu4
Inonu University Faculty of Medicine Department of Internal Medicine
Division of Endocrinology and Metabolism, Malatya, Turkey; 2Inonu
University Faculty of Medicine Department of Obstetrics and Gynecology,
Malatya, Turkey; 3Inonu University Faculty of Medicine Department of
Family Medicine, Malatya, Turkey; 4Inonu University Faculty of Medicine
Departmant of Biomedical Statistics, Malatya, Turkey; 5Ozel Dogu
Hastanesi, Malatya, Turkey.
The status of carbohydrate metabolism of pregnant women with positive glucose
challenge test (GCT), but normal oral glucose tolerance test (OGTT); and their
neonates have not defined clearly.
Pregnant women with normal GCT (n: 120), with abnormal glucose challenge test
(AGCT) but normal OGTT (n: 67) and those with gestational diabetes (GDM) (n:
67) were included into the study. Local ethical committee approval was obtained.
Insulin sensitivity was evaluated by fasting insulin level, homeostasis model
assessment of insulin resistance index (HOMA-IR); quantitative insulin check
index (QUICKI) and ISOGTT. Serum insulin and glucose values during OGTT
were documented. The patients with both AGCT and GDM were treated either
with diet or if needed with insulin until achieving the goals for defined glucose
values. Perinatal outcome and delivery modalities were also compared between
these three groups.
Both GDM (31.6G5.9 yrs) and AGCT groups (29.0G4.0 yrs) were older than
control subjects (28.1G4.9 yrs). Body mass index (BMI) was found to increase
with a correlation to the severity of carbohydrate intolerance as the predominant
factor affecting both AGCT and GDM groups (odds ratios were 3.78 and 5.97
respectively). Despite there was no significance between insulin indices; serum
glucose and insulin values were similarly different than controls in both AGCT
and GDM groups. Macrosomic infant and caesarean section rates were higher
than control group in both GDM and AGCT groups in favor of gestational
diabetics (6.6% vs. 18.9%; PZ0.0001 and 20% vs. 27.7% PZ0.0001
Pregnant woman with abnormal glucose challenge test have impaired carbohydrate
metabolism as in gestational diabetics with a lesser severe degree.
Ambulatory blood pressure reduction after rosiglitazone treatment in
normotensive type 2 diabetic patients
Yasemin Kemal1, Neslihan Tutuncu1, Nilgun Guvener1, Asli Unal1,
Ilyas Atar2 & Haldun Muderrisoglu2
Baskent University Faculty of Medicine Department of Endocrinology,
Ankara, Turkey; 2Baskent University Faculty of Medicine Deoartment of
Cardiology, Ankara, Turkey.
The thiazolidinediones are new and potentially useful developments in the
treatment of type 2 diabetes and impaired glucose tolerance. We tested the effects
of the thiazolidinedione, rosiglitazone on blood pressure in normotensive type 2
After receiving approval from the local ethics committee, 25 normotensive
diabetic patients were were enrolled to the study. Before the rosiglitazone
treatment we measured plasma glucose, HbA1c, Hb, lipid profile and BMI. Also
each subject underwent ambulatury blood pressure recording. Subjects were then
placed on rosiglitazone treatment (8 mg per day) for twelve weeks, and baseline
tests were repeated.
9th European Congress of Endocrinology, Budapest, Hungary, 2007
At the end of twelve weeks there were significant decreases in total average
diastolic blood pressure (67.02G8.06 vs 62.58G5.90, P!.009) and daytime
average diastolic blood pressure (68.64G8.51 vs 65.12G6.34, P!.01). In
addition, there were also significant decreases in fasting plasma glucose (PZ
.007), postprandial plasma glucose (PZ.01), HbA1c (PZ.010), and Hb levels
(PZ.005). Correlation analysis revealed that changes in diastolic blood pressures
were not correlated with the decrease in both Hb, HbA1c. Also there was no
significant correlation between the improvement in fasting and postprandial blood
glucose and the decline in blood pressure.
Our study demonstrated a significant and sustained reduction in diastolic blood
pressure with rosiglitazone therapy for 12 weeks, which was independent from the
blood-glucose–lowering effect of the drug. Long-term studies are needed to
determine the TZD-associated effects on blood pressure and other cardiovascular
risk factors.
Time dependent effects of rosiglitazone on heart and fluid dynamics: a
6-month follow up study
Yasemin Kemal1, Nilgun Demirag1, Neslihan Tutuncu1, Aylin Yildirir2,
Asli Atar2 & Asli Unal1
Baskent University Faculty of Medicine Department of Endocrinology,
Ankara, Turkey; 2Baskent University Faculty of Medicine Department of
Cardiology, Ankara, Turkey.
Thiazolidinediones (TZDs) have become a powerful tool for lowering insulin
resistance. The problem of cardiovascular adverse events including fluid retention
and risk of heart failure, although of a low incidence, should be well known and
recognized. We aimed to evaluate the effects of rosiglitazone treatment on cardiac
function and show whether these effects are reversible when we continued this
Fourty-six type 2 diabetic patients -without any symptoms and findings of heart
failure-were randomized to treatment with rosiglitazone, metformin and control
group after receiving approval from the local Ethical Committee. There were no
significant differences between the groups in the duration of diabetes, HbA1c and
plasma brain natriuretic pepetide (BNP) levels, body mass index (BMI) and
myocardial performance indexes (MPI) before the treatment. After three months and
after six months all these parameters were repeated.
After three months period with rosiglitazone treatment, plasma BNP levels increased
rapidly. Except one subject we did not see any clinical adverse effect including
excessive weight gain, edema, and dyspnea so we continued rosiglitazone treatment.
At the end of the six months period, this rapid increase didn’t continue. Similarly,
lateral wall MPIs worsened after three months- although statistically nonsignificantand then improved significantly after six months in rosiglitazone group (PZ0.001).
Also the changes in hemoglobin values were highly correlated with other results that
provide evidence of these reversible findings.
Our study showed the stability and reversibility of the adverse effects of TZDs on
cardiovascular function and fluid dynamics in type 2 diabetics.
Peculiarities of heart rate control in patients with non-insulin
dependent diabetes mellitus and hypertension
Andris Vitols, Daina Voita & Mara Vitola
Institute of Cardiology, University of Latvia, Paul Stradins Clinical
Hospital, Riga, Latvia.
To assess the sensitivity of exercise induced heart rate (HR) and baroreceptor
reflex (BR) chronotrope reaction and HR variability for an early detection of
autonomic nervous system impairment in non-insulin dependent diabetes mellitus
(NIDDM) patients with arterial hypertension.
Design and Methods
On 25 NIDDM pts (group A, 63G1.8 yrs. aged men, HbA1C 10.2G0.9%),
17 essential hypertension (EH) pts without glucose metabolism disturbances
(group B, gender and age matched) and 20 controls (C) at rest and during
handgrip (with force 50% of maximal for 60 s), beat-to-beat HR and finger
mean arterial pressure (MAP) were monitored and bradycardic reaction to
BR activation (by neck suction K60 mmHg) was analysed. HR variability
by time and frequency domain analysis of ECG 512 R-R interval files was
performed in supine and upright postures.
Group A comparing to B and C was characterised by increased HR (81G2
vs.72G3 vs.70G3 bpm; P!0.05) and decreased bradycardic reaction to BR
activation (1.95G0.3 vs. 4.9G0.9 vs.10G0.6 bpm; P!0.05). At 60th sec of
handgrip MAP increase was similar in all groups but HR increase was
reduced in group A vs. B vs.C (12G2 vs. 24G2 vs.18G2 bpm; P!0.05),
but reaction to BR activation disappeared in group A and B, whereas in C
remained in 32G11% of resting value. R-R interval variability in group A
and B was diminished (P!0.01), but its decrease in upright position was
less in group A than in C (108G12 vs. 254G21 ms; P!0.05), whereas the
difference of increase in low-high frequency band ratio (LF:HF) was not
significant in group A and B.
In patients with non-insulin dependent diabetes mellitus and hypertension,
HR reaction to exercise and BR activation has an advantage over HR
variability analysis to ascertain an early impairment of autonomic control of
sinus node.
One injection of Detemir insulin administered before the lunch
improves the metabolic control in type 1 diabetic patients
Juan Carlos Ferrer-Garcı́a1, Juan Francisco Merino-Torres2,
Raquel Segovia-Portolés2, Vicente Campos-Alborg2, Agustı́n
Herrera Ballester1, Francisco Piñón Sellés2 & Carlos Sánchez Juan1
University General Hospital, Valencia, Spain; 2University Hospital La Fe,
Valencia, Spain.
To compare 2 modalities of bolus-basal insulin therapy with aspart-detemir,
according to the moment of administration of detemir (DET), before the lunch or
bed-time, in type 1 diabetic patients with poor metabolic control.
We conducted a prospective study of 40 type 1 diabetic patients, with poor
metabolic control (HbAc 7–12%), randomized to receive treatment with 1
injection of DET before the lunch or bed-time and followed-up during 24 weeks.
Physician decided the addition of one second dose, administering DET every
12 hours (DET-12 h) if the objectives in glycemic control were not obtained.
Insulin analog aspart was used for the post-prandial control. Weight, insulin
units/Kg/day, HbA1c, score in a test of quality of life (ITQ7) and hypoglycemias
were determined.
19 patients in DET pre-lunch group and 16 in DET bed-time group
completed the study. 10 patients of group DET pre-lunch and 12 of DET
bed-time needed DET-12 h. After 24 weeks of bolus-basal insulin therapy, a
reduction of HbA1c was demonstrated, and the group DET pre-lunch
showed a major reduction of HbA1c. By groups of treatment: DET prelunch 8.5 vs 7.1% (P!0,05); DET bed-time 9.0 vs 7.6% (P!0.05.) and
DET-12 h 8.8 vs 8.1% (P!0.05.). The ITQ7 demonstrated an improvement
without differences between the groups (score baseline visit 74.5G17.3
versus 62.0G19.2; P!0.01). There were no differences in weight and
number of non-serious hypoglycemia. Serious hypoglycemia was presented
in one patient of DET bed-time group. An increase in the insulin
requirements was demonstrated in the 3 groups of treatment (average:
0.78G0.2 u/kg/day in baseline visit versus 0.86G0.2; P!0.05).
after this study, we recommend to begin detemir insulin treatment with one
injection administered before the lunch. However, a strict monitoring is
necessary because some patients will require two injections of detemir.
Endocrine Abstracts (2007) Vol 14
9th European Congress of Endocrinology, Budapest, Hungary, 2007
Oral antibodies to insulin receptor are found effective in the treatment
of streptozotocin-induced diabetes in rats
Julia Dugina1, Andrey Martyushev-Poklad1, Irina Kheyfets1,
Alexander Spasov2, Maria Samokhina2, Oleg Epstein1 &
Svetlana Sergeeva1
‘Materia Medica Holding’ Company, Moscow, Russia; 2Volgograd State
Medica University, Volgograd, Russia.
PED levels are increased in peripheral blood leucocytes from
euglycaemic subjects at-risk of type 2 diabetes
Rossella Valentino1, Gelsy Arianna Lupoli1, Pietro Formisano1,
Iolanda Esposito1, Anna Teresa Alberobello1, Anna Perfetti1,
Michele Cirillo2, Nicola Gennarelli2, Giovanna Gargiulo2, Roberto Lobello2
& Francesco Beguinot1
Dpt. Cellular and Molecular Biology and Pathology, Naples, Italy; 2Dpt.
Endocrinology/General and Digestive Surgery, Naples, Italy.
An experimental study was designed to test a drug candidate for the treatment of
diabetes mellitus in rats with streptozotocin (STZ) diabetes.
Diabetes was induced in outbred male rats (280–300 g) by single iv
injection of streptozotocin 50 mg/kg. The animals showing hyperglycemia
(12–15 mM) 72 hours after injection were randomized to receive daily
intragastric doses of distilled water, glibenclamid 8 mg/kg, or polyclonal
antibodies to C-terminal fragment of insulin receptor, beta subunit (ultra-low
doses, anti-InsR); the last group received insulin subcutaneously (12 U/kg).
For 7 weeks, the animals were monitored for fasting glycemia, glycosuria,
and glucose tolerance.
STZ caused a sustained hyperglycemia (12–21 mM versus 2.3–3.2 in
intact rats, maximum at day 42) and glycosuria (2.7–3.7 mM versus 0.8–
1.8 mM in intact rats). Glucose tolerance reduced 3.5–5.5-fold (calculated
by AUC in glucose load test). The rats featured polydipsia (an 2.7–3.2-fold
increase in water consumption), body weight reduced by 50%. Due to
diabetes and its complications, survival rate reduced to 12.5% (from 100%
in intact rats).
Glycemia reduced by 30–50% in insulin group, and by 10–42% glibenclamid
group, though remained abnormal. STZ-induced glycosuria remained unaffected in
both groups. Survival rate increased up to 20%. Peroral anti-InsR was much more
effective in reduction of glycemia (to normal values, 5.0–3.0 mM) and glycosuria
(below 0.8 mM). Anti-InsR enhanced survival to 30%. The increase in glucose
tolerance was most considerable in insulin and anti-InsR groups, less marked in
glibenclamid group.
The peroral anti-InsR agent is regarded as a promising candidate therapeutic for
the treatment of diabetes mellitus.
Phosphoprotein enriched in diabetes (PED) is a scaffold protein widely produced
in different tissues; it is involved in multiple cellular functions, including insulinregulated glucose transport. Previous findings showed that in individuals with
type 2 diabetes (T2D) the PED gene is overexpressed in skeletal muscle (SM) and
adipose tissue (AT), both target tissues for insulin activity. Our group has recently
evidenced that PED protein is also expressed in peripheral blood leucocytes
(PBLs) and overexpressed in about 30% of diabetics.
To investigate the presence of any correlation in PED expression between PBLs
and insulin-sensitive tissues, in order to validate this method as a possible
screening in at-risk subjects for T2D.
Subjects and methods
21 subjects were recruited: 14 euglycaemic (7 T2D first degree relatives (FDR)
and 7 without T2D family history) and 7 T2D patients. We evaluated PED protein
expression analysing lysates from AT and SM, and PBLs by immunoblotting with
specific PED antibodies.
A two-fold increase in PED levels in AT and SM was found both in T2D patients
and in FDR, compared with euglycaemic controls. On the whole, PED levels were
30% higher in PBLs than in SM and AT (P!0.001) from the same subjects.
Moreover, in all subjects there were significant correlations between PED levels
in the PBLs and those in AT and in SM (P!0.001).
PED expression can be detected in PBLs and its expression is correlated with that
in insulin-sensitive tissues. Therefore, this method could become a valid aid to
identify at-risk individuals for diabetes in large scale studies.
1 year endurance training at the level of the ventilatory threshold in
type-2 diabetics reduces by 50% healh costs: a controlled randomized
Brun Jean-Frédéric, Jaussent Audrey, Picot Marie-Louise, Mercier Jacques
& Oréfaut Christian
CERAMM Service Central de physiologie Clinique, Hôpital Lapeyronie,
Montpellier, France.
Effectiveness of a-lipoic acid in prevention of peripheral diabetic
Nino Jikurauli, Ellen Giorgadze, Nino Svani, Vasil Chachibaia,
Felix Bestavashvili, Tea Lominadze, Nia Chanturia & Anna Malazonia
N4 clinical hospital, Tbilisi, Georgia.
This trial was undertaken in order to evaluate the effects of endurance
training on health cost in type 2 diabetes. 35 diabetic patients were
randomly assigned to 2 groups: After 10 drop-outs, 15 followed a training
program (8 sessions followed by training at home at the level of the
ventilatory threshold VT) while 10 had only routine treatment. Both groups
were followed over 1 year with evaluation at 30, 120, 240 and 365 days for
health costs, blood pressure, and a standard maximal exercise test, glycemic
and lipid equilibrium, 6-min walking test, and exercise (Voorips) and quality
of life questionnaires. The effectiveness of training was confirmed in the
trained group by an increase in the Voorips score (5.25G3.3 P!.001) and a
lack of decrease in VO2max and Pmax while in the untrained group VO2max
decreased slightly (K2.16G2.5 PZ0.014). Thus trained subjects at the end
of the study reached a higher percentage of the theoretical maximal power
(PZ0.041). The 6-min walking distance (472.2G98.9 vs 547.6G56.7 PZ
0.020) was also higher than in the control group. Blood pressure, lipid
profile and glycemic control did not significantly improve during this period
in either groups, due decreasing doses in treatments prescribed by their
physicians. In the trained group there was no hospitalization, in contrast
(PZ0.047) with controls in whom there was 1.27G2.20 (ie, 0 to 5 days) of
hospitalization. The total health cost over this period is lowered by 50% in
the trained group (PZ0.018). In conclusion, endurance training at the level
of the VT significantly prevents the progressive decline in aerobic working
capacity evidenced in untrained diabetics over this period of observation. It
results in a marked reduction in health cost due to a decrease in treatment
and fewer hospitalizations.
Endocrine Abstracts (2007) Vol 14
The aim of our study was to assess the effectiveness of a-lipoic acid for the
reducing the risk of developing peripheral diabetic neuropathy.
Subjects and methods
We have studied 38 patients with type I and II diabetes, from age 28 to 35. The
mean duration of disease was 9 years. Patients were divided in two groups. In
group I were included 15 patients which got a-lipoic acid in order to prevent
peripheral diabetic neuropathy in dosage 600 mg-50 ml a day i/v infusion during
3 weeks, then 600 mg a day per-os, during 2 months. The treatment was provided
twice a year during the 2 year period. In group II were included 23 patients, who
did not got a-lipoic acid. In both groups we studied HbAIC, fasting glucose, lipid
profile, sensation screening tests; knee-jerk and tendon reflexes, subjective
complaints were estimated by TSS scale.
In I group of the patients the mean value of HbAIC was 7.0%, fasting glucose
133 mg/dl (G20); total Chol. 208 (G30), Trig 198 (G15), HDL 76 (G10); LDL
112 (G12), vibration sensation was decreased in 4 and a temperature sensation in
2 patients. The tactile and pain sensation were preserved. Knee-jerk and tendon
reflexes were not changed, subjective symptoms by TSS were – 1.00;
In group II HbAIC was 7.2%, fasting glucose 138 mg/dl (G25); total Chol. 234
(G33); Trig 265 mg/dl; HDL 71 mg/dl; (G10); LDL 116 mg/dl, vibration
sensation was decreased in 10, tactile sensation - in 2 and a temperature sensation
in - 6 patients. The tactile and pain sensation were preserved. Knee-jerk and
tendon reflexes were not changed, subjective symptoms by TSS was – 1.33;
Administration of a-lipoic acid for the lowering the risk of developing of
peripheral diabetic neuropathy is required.
9th European Congress of Endocrinology, Budapest, Hungary, 2007
Adhesion molecules s-VCAM-1 and s-ICAM-1 in members of families
with familial combined hyperlipidemia
David Karásek, Helena Vaverková, Milan Halenka, Zdenek Fryšák,
Dalibor Novotný & Marie Budı́ková
University Hospital, Olomouc, Czech Republic.
Low dose cyclosporin and methotrexate administration induces
remission of Type 1 diabetes mellitus
Douglas Sobel, Val Abbassi & Annette Henzke
Georgetown University, Washington, DC, United States.
Familial combined hyperlipidemia (FCH) is the most common familial
hyperlipidemia with a high risk of the early atherosclerosis. The aim of this
study was to compare levels of s-ICAM-1 and s-VCAM-1 in asymptomatic
members of FCH families with healthy controls and to find out relation between
s-ICAM-1, respective s-VCAM-1, and risk factors accompanying FCH. We also
investigate association between adhesion molecules and intima-media thickness
of common carotid artery (IMT) in FCH families.
82 members of 29 FCH families were divided into the 2 groups: HL (probands and
hyperlipidemic first-degree relatives, nZ47) and NL (normolipidemic firstdegree relatives, nZ35). The control groups – HL-C (nZ20) and NL-C (nZ20) –
consisted of sex- and age–matched healthy individuals.
Hyperlipidemic members had significantly higher concentration of s-ICAM-1
(633.7G169.6 ng/ml vs 546.2G155.9 ng/ml, P!0.05). The elevation of
s-VCAM-1 was not significant (880.8G202.9 ng/ml vs 826.5G174.6 ng/ml,
N.S.). Levels of s-ICAM-1, respectively of s-VCAM-1 in normolipidemic
relatives were not significantly different compared to the control group (530.8G
113.9 ng/ml vs 530.0G101.0 ng/ml, respectively 860.2G265.7 ng/ml vs 822.1G
197.0 ng/ml). There was significant correlation between s-ICAM-1 and apoB (rZ
0.42; P!0.01) in hyperlipidemic subjects and between s-ICAM-1 and proinsulin
(rZ0.54; P!0.01) in normolipidemic subjects. S-ICAM-1 correlated with IMT
(rZ0.32; P!0.05) in all members of FCH families.
The increase of s-ICAM-1 in asymptomatic hyperlipidemic members of FCH
families reflects their high cardiovascular risk. The positive association between
s-ICAM-1 and IMT could indicate s-ICAM-1 as a potential predictor of
atherosclerosis manifestation.
This work was supported by grant IGA MZCR NR/ 9068-3.
Although, high doses of cyclosporine (cyclo)has been demonstrated to inhibit the
development of type 1diabetes mellitus (T1D), its usefulness was limited by its
toxicity. Since methotrexate (Mtx) and cyclo have been shown to synergistically
act in other disease processes, we determined if low dose cyclo and Mtx therapy
could inhibit the development of diabetes and reduce or eliminate the need for
insulin therapy in a pilot study.
Insulin dose and glycemic control were compared in 7 children (mean age
13.7 year) with new onset T1D who were administered cyclo at 7.5 mg/kg/day for
6 weeks and then 4 mg/kg/day and Mtx 5 mg/kg/day for one year and in 10 newly
diagnosed diabetic control children (mean age 12.5 year). After 6 weeks, cyclo
doses were adjusted to maintain blood cyclo levels 100–200 ng/ml. All children
were treated with two daily doses of NPH and fast acting insulin. Clinical and
biochemical toxicity of drug therapy was assessed. The study was approved by the
Institutional Review Board.
There were two episodes of mild mucositis which required transient lowering of
the Mtx dose and one case of transient mild elevation of bilirubin. There were no
abnormalities in other liver function tests, creatinine, BUN, or CBC. Mean
HbA1c levels were similar in the experimental and control groups at baseline
(12.6% vs 11.5%) and at 3, 6, 9, and 12 months. Daily Insulin requirements of the
groups were similar at baseline. However the mean insulin dose (u/kg) at 3, 6, 9,
and 12 months were significantly (P!0.001) lower in the experimental group
(0.14 vs 0.56 at 3 months, 0.12 vs 0.61 at 6 months, 0.16 vs 0.55 at 9 months, and
0.22 vs 0.71 at 12 months). No control subjects became non-insulin requiring.
However 4 of 7 experimental drug treated subjects were entirely off insulin
therapy for 2.5, 4.5, 7 and 12 months. While off insulin therapy, the HbA1c levels
of 3 of the 4 subjects were normal. The other subject’s HbA1c was only mildly
elevated at 6.7%. In conclusion. low dose cyclosporine and MTX treatment of
subjects with new onset T1D can safely induce remission of disease and decrease
the amount of required insulin.
Body fat distribution, lipid and adipokine levels in South African type 2
diabetic patients of African and Indian origin
Rita Waisberg, Janice Paiker, Jaya George & Nigel Crowther
NHLS, Johannesburg, Gauteng, South Africa, WITS; Johannesburg,
Gauteng, South Africa.
Progression of diabetic retinopathy in pregestational diabetes mellitus
R Guerrero1, MA Martinez Brocca1, MA Pomares1, S Palma1, I Gonzalez1,
D Acosta1, E Moreno2 & F Villamil1
Departament of Endocrinology and Nutrition, Hospital Universitario
Virgen del Rocı́o, Sevilla, Spain; 2Departament of Obstetrics and
Gynecology, Hospital Universitario Virgen del Rocı́o, Seviila, Spain.
The increased insulin resistance seen in Type 2 diabetic patients has been shown to be
associated with abdominal fat accumulation, hypertension, and dyslipidaemia. The
dyslipidaemia is characterized by raised serum triglycerides and decreased high
density lipoprotein cholesterol (HDL) levels. The aim of the present study was to
investigate the relationship between abdominal fat, lipid and adipokine secretion in
South African type 2 diabetic patients of Indian and African origin.
Plasma and serum samples were collected from 20 African and 20 Indian diabetic
females. Adipokines were measured using ELISA kits. Fasting plasma glucose,
serum cholesterol, HDL-cholesterol, and triglycerides were assayed on the ROCHE
MODULAR System. Insulin resistance was calculated using HOMA. CT-scans were
performed to measure abdominal visceral and subcutaneous fat areas.
Data presented as mean valuesGSEM. The results for diabetic African (DA) and
diabetic Indians (DI), respectively were as follows: Leptin (ng/ml) 40.6G2.49 and
43.6G2.1, soluble leptin receptor (U/ml) 21.0G1.71 and 20.5G1.7, IL-6 (pg/ml)
3.15G0.58 and 3.87G1.08, TNF-alpha (pg/ml) 7.06G1.38 and 2.26G0.42 (PZ
0.003), CRP (mg/l) 11.4G3.09 and 8.97G1.58, cholesterol (mmol/l) 4.78G0.22
and 5.24G5.24, HDL (mmol/l) 1.17G0.05 and 1.76G0.4, and triglyceride
(mmol/l) 1.41G0.11 and 2.11G0.36, respectively. HOMA results for DI were
7.54G0.74 and for DA 6.56G1.26 (PZ0.507). The visceral fat area was higher in
diabetic Indian 117.47G9.94 compared to African diabetic patients 93.85G6.22
(PZ0.044). No difference in BMI was noted between the groups.
Although visceral fat area is higher in diabetic Indian than diabetic African patients
this seems to have no influence on adipokine levels. However, it may influence
triglyceride metabolism.
Pregnancy may adversely affect the progression of diabetic retinopathy and can
have serious implications for the pregnant women.
To asses the impact of pregnancy on the progression of diabetic retinopathy in
women with type 1 and type 2 diabetes mellitus and to identify risk factors for the
progression of retinopathy during pregnancy.
306 diabetic women, 229 (75.4%) with type 1 and 77 (23.9%) with type 2
diabetes, referred to the Diabetes and Pregnancy Unit of the Hospital Virgen del
Rocio from January 1995 through February 2004 were studied retrospectively.
Dilated fundal examination was performed at booking, second and third trimester.
At early postpartum was performed fluorescein angiographies.
Retinopathy at booking was seen in 54 (17.6%). Any women without retinopathy
at booking developed retinopathy during pregnancy or in early postpartum.
Progression to proliferative retinopathy was seen in one patient (0.32%), while
progression to moderate or severe non proliferative retinopathy was found in eight
(2.6%). One women developed during pregnancy macular edema (0.32%).
Progression of retinopathy was significantly increased in women with duration of
diabetes O10 years (6.9% vs 0%, P!0.05). Laser therapy was needed in four
(1.3%). Although glycaemic haemoglobin A1C (HbA1c) at booking was higher
(7.95G1.81 vs 7.02G1.27) and the fall in HbA1c between booking and 16 weeks
was greater (1.66G1.33 vs 1.34G1.08) in those women showing progression of
retinopathy, these changes were not significant.
Progression of retinopathy in pregnancy was uncommon, but significantly more
frequent in women with duration of diabetes more than 10 years. Laser therapy
Endocrine Abstracts (2007) Vol 14
9th European Congress of Endocrinology, Budapest, Hungary, 2007
was necessary in one percent of pregnancies, which is much lower than reported
in earlier studies.
Body composition, emotional state and quality of life in patients with
diabetes mellitus type 2
Lina Lasaite & Jurate Lasiene
Institute of Endocrinology, Kaunas University of Edicine, Kaunas,
Comparison of insulin monotherapy and combination therapy with
insulin and metformin or insulin and rosiglitazone or insulin and
acorbose in type 2 diabetes
Hamiyet Yilmaz, Alptekin Gursoy, Mustafa Sahin, Neslihan Bascil Tutuncu
& Nilgun Guvener Demirag
Baskent University Faculty of Medicine, Department of Endocrinology and
Metabolic Diseases, Ankara, Turkey.
The aim of this study was to compare the efficacy of treatment with insulin
alone, insulin plus acarbose, insulin plus metformin or insulin plus
rosiglitazone in type 2 diabetic subjects who were previously on insulin
monotherapy, and to evaluate the effects of these treatments on cardiovascular
risk factors including lipid profile, C-reactive protein (CRP) and fibrinogen.
Sixty-six poorly controlled type 2 diabetic patients on insulin monotherapy
were involved. They were randomized to insulin alone, insulin plus acarbose,
insulin plus metformin or insulin plus rosiglitazone groups for six months
period. Mean fasting and postprandial glucose values as well as HbA1c levels
significantly decreased in all groups except for insulin plus acarbose group.
The greatest improvement in HbA1c was observed in insulin plus rosiglitazone
(2.4%) and insulin plus metformin (2%) groups. Daily total insulin dose
increased 12.7 units/day in insulin alone group, decreased 4.7 units/day in
insulin plus rosiglitazone group, 4.2 units/day in insulin plus metformin group,
and 2.7 units/day in insulin plus acarbose group. Least weight gain occurred in
insulin plus metformin group (1.4 kg) and greatest weight gain occurred in
insulin plus rosiglitazone group (4.6 kg). Except for the improvement of total
cholesterol levels in insulin plus rosiglitazone group, no significant change in
lipid levels was observed in any groups. CRP levels decreased significantly
both in insulin plus metformin and insulin plus rosiglitazone groups.
Fibrinogen levels decreased in insulin alone, insulin plus metformin, and
insulin plus rosiglitazone groups. All groups were comparable in hypoglycemic
episodes. No serious adverse event was noted in any group.
Diabetes mellitus type 2 (DM2) is affecting physical and psychological health.
Compare anthropometric data, body composition, lipids levels, emotional state,
quality of life (QoL) of DM2 patients and that of healthy persons of the same age.
39 persons (58.1G9.6 years) with DM2 (18 male, 21 female) and 41 healthy
persons (54.3G9.9 years) (22 male, 19 female). Profile of Mood State (POMS)
used for emotional state evaluation, WHO Brief Quality of Life Questionnair – for
In male weight (107.6G30.1 vs 86.7G23.1 kg, PZ0.008), body mass index
(35.0G9.9 vs 28.1G5.4 kg/m2, PZ0.013), fat mass (37.7G21.0 vs 25.1G
12.3 kg, PZ0.041), lean mass (69.7G10.6 vs 61.6G11.7 kg, PZ0.022), water
mass (52.1G9.1 vs 45.1G7.6 kg, PZ0.007, waist-to-hip ratio (0.97G0.06 vs
0.91G0.05, PZ0.018) were significantly higher in DM2 patients than in controls.
In female weight (90.5G14.6 vs 74.5G18.7 kg, PZ0.002), body mass index
(34.9G6.2 vs 28.0G5.7 kg/m2, PZ0.013), fat mass (42.0G10.4 vs 30.6G
12.2 kg, PZ0.003), lean mass (48.5G6.4 vs 43.5G7.8 kg, PZ0.05), water mass
(38.1G4.8 vs 33.5G4.9 kg, PZ0.004), waist-to-hip ratio (0.90G0.4 vs 0.83G
0.1, PZ0.002) were significantly higher in DM2 patients than in healthy female.
In male and female no significant differences between research and control groups
in high and low density cholesterol were found. In male, but not female QoL
(79.3G8.6 vs 85.3G8.7, PZ0.032), POMS vigor (K11.8G3.8 vs K15.8G4.8,
PZ0.009) were significantly lower in DM2 than in control group. Significant
correlations were found in male between vigor and waist-to-hip ratio (rZ0.347,
PZ0.041), in female between vigor and water mass (rZ0.313, PZ0.049), POMS
total and waist-to-hip ratio (rZ0.362, PZ0.046), depression and low density
cholesterol (rZ0.430, PZ0.028), vigor and lean mass (rZ0.385, PZ0.014).
In conclusion
Weight, body mass index, fat mass, lean mass, water mass, waist-to-hip ratio were
significantly higher in male and female; quality of life and vigor were
significantly lower in DM2 male than in healthy persons of the same age.
Competition between catecholamines and glucose for binding sites on
proteins of erythrocytes
Michael Lepschy, Erich Moestl & Rupert Palme
Veterinary Medicine Vienna, Vienna, Vienna, Austria.
Glucose is slowly linked to haemoglobin in a non-enzymatic reaction and the
determination of a glycated protein (HbA1c) is used for long term monitoring
blood glucose concentrations. Radiometabolism studies in sheep showed that a
haemoglobin-adduct formation also takes place with epinephrine or norepinephrine.
The aim of our study was to elucidate if there is a competition between
catecholamines and glucose for binding sites on proteins of the erythrocytes.
Heparinised canine blood was obtained and centrifuged at 1500 g and the cells
were washed three times with isotonic NaCl-solution. Afterwards, 5 portions of
erythrocytes (0.7 ml each) were re-suspended in 7 ml TCM ‘Eagle’ and incubated
with epinephrine and norepinephrine (1 and 10 ng/ml) for 3 days at 38.6 8C. One
portion served as control.
Afterwards the erythrocyte portions were split into sub-samples of 0.2 ml each.
One half was incubated with 3H-norepinephrine for 1 h (unhaemolysed), the
second half with 14C-glucose for 10 days after haemolysis by freezing. To
determine the uptake of 3H-norepinephrine, samples were centrifuged and the
radioactivity of the supernatant was measured. In total 410G7 Bq of the added
574G16 Bq were measured in the control samples, whereas all groups
preincubated with non-radioactive catecholamines showed significantly (P!
0.05) higher radioactivity. To determine the binding of 14C-glucose, proteins were
precipitated. After centrifugation, 567G24 Bq of the added 1916G80 Bq were
measured in the supernatant of the control samples. As in the experiment using
H-norepinephrine, significant (P!0.05) higher values were measured in the
supernatant of the preincubated erythrocytes, indicating a lower binding of 14Cglucose to the proteins.
Therefore we conclude that catecholamines are blocking binding sites on
proteins of erythrocytes for additional adduct formation with 3H-norepinephrine
or 14C-glucose.
Endocrine Abstracts (2007) Vol 14
Deleterious effects of beta-blockers on arterial stiffness and central
pulse pressure in menopausal women: baseline findings from the
Cashmere trial
S Laurent2, S Christin Maitre1, A Gompel3, P Boutouyrie2, P Jaillon1,
Ch Thuilliez4, F Zannad5, B Pornel7, B Pannier8, H Struijker-Boudier9,
L Van Bortel10, Ch Kuntz11, A Keanry-Schwartz5, I Pithois-Merli6,
D Simonneau6 & T Simon1
Saint Antoine-UMPC-ParisVI university Hospital, Paris, France; 2HEGPParis V-University Hospital, Paris, France; 3Hotel Dieu-Paris V-University
Hospital, Paris, France; 4CHU Rouen, Rouen, France; 5CHU Nancy, Nancy,
France; 6Pfizer, Paris, France; 7Centre de menopause, Bruxelles, Belgium;
Department of cardiology, fleury-merogis, France; 9Department of
cardiology, Maastricht, Netherlands; 10Department of cardiology, Ghent,
Belgium; 11CHU strasbourg, Strasbourg, France.
Beta-blockers (BB) may be less effective than other antihypertensive drugs for
stroke prevention in patients with primary hypertension (ASCOT and LIFE
studies). Our study compares arterial stiffness and central PP between users
(BBC) and non users of BB (BB-), among menopausal women with
hypercholesterolemia and no history of CV disease.
Methods and Results
We used the baseline data of 664 menopausal women, screened for the
Cashmere study, a12-month double-blind randomized trial comparing the
effects of atorvastatin (80 mg/day), vs placebo, Gwith hormone therapy, on
the progression of CCA-IMT and arterial stiffness. Aortic stiffness was
measured by carotid-femoral pulse wave velocity (PWV); central PP and
augmentation index (AI, wave reflection) were determined by applanation
tonometry; carotid stiffness was calculated from relative stroke change in
diameter (echotracking system) and carotid PP. BB were used in 104 women
for treating headache, tachycardia, arrhythmia, and hypertension. 97% BB
used were devoid of vasodilating properties. Age (60G6 vs 58G5 years, P!
0.0001) and mean BP (MBP: 91G12 vs 88G11 mmHg, P!0.0001) were
slightly but significantly higher in BBC than in BB- (nZ560). After
9th European Congress of Endocrinology, Budapest, Hungary, 2007
adjustment to age and MBP, BBC had 10% higher central PP (P!0.0001),
6% higher AI (P!0.001), 4% higher PWV (PZ0.04), and 5% higher carotid
stiffness (P!0.01) than BB-. BBC had 4% higher central SBP (P!0.0001)
than BB-, despite a non significantly higher brachial SBP only (1%, PZNS).
To rule out an influence of hypertension on arterial parameters, we compared
users of anti-hypertensive drugs (nZ110) to non users (nZ554). No
significant difference was observed concerning the above parameters,
excluding or not BB- users.
In menopausal women with hypercholesterolemia and no CV disease, the use of
non-vasodilating BB was associated with higher aortic and carotid stiffness.
These data are consistent with the results of the CAFÉ trial. Whether the
deleterious effects of BB on large arteries increase the risk of CV events in women
remains to be determined.
Prevalence of GADA and IAA in elderly patients with type 2 diabetes
Maria Kurowska1, Jerzy S Tarach1, Helena Jankowska2,
Mariusz Kowalczyk1, Joanna Malicka1 & Andrzej Nowakowski1
Dpt Endocrinology, Skubiszewski Medical University, Lublin, Poland;
Dpt Nuclear Medicine, Skubiszewski Medical University, Lublin, Poland.
Little is known about the prevalence and significance of islet cell immunity in
elderly patients with type 2 diabetes. The low antibody titers against islet-cell
antigens in LADA elderly patients may be a sign of a less aggressive autoimmune
The objective
To establish the changing frequency and titers of GADA and IAA in elderly
83(56F;27M)diabetic patients (60–91 y) divided in age related groups. Group 1:
55 (36F;19M) patients (60–69 y). Group 2: 14 (9F;5M) pts (70–79). Group 3: 14
(11F;3M) pts (80–91). Mean duration of diabetes 5.6G6.4 y.
GADA and IAA determined by RIA (ANTI-INSULIN RIA and GAD-AB kits),
(CIS). IAA estimated in patients not treated with insulin. The positive GADA and
IAA titers were over 1 U/ml and 5.5%B/T.
Group 1: Positive GADA were found in 13(27%) assays, 5(10.2%) patients with
the level 7.1–64.5 U/ml and 8(16.5%) subjects 1.02–2.1 U/ml. In 11(22.9%)
patients GADA titers 0.38–0.98 U/ml were found (method sensitivityO0.3 U/ml).
The positive IAA were in 20(40.8%) assays (5.6–13.2%B/T). Group 2: In
3(21.5%) patients, the GADA were O1 U/ml (1.63; 38.5;68.5 U/ml). 4(28.6%)
patients had GADA 0.93–0.99 U/ml. The positive IAA were obtained in 4(28.6%)
patients (9.1–19.7%B/T). Group 3: There were positive GADA in 4(30.8%)assays
(1.3–12.1 U/ml). In 8(61.5%%) patients GADA ranged 0.61–1.42 U/ml. In
6(42.9%) subjects the positive IAA was obtained (1 patient 36.1%B/T and the rest
The percentage of patients with high GADA titer didn’t significantly change with
the age. In the older patients the frequency of GADA low titers (close to 1 U/ml)
clearly increased. The IAA frequency and titer didn’t significantly change with
the age.
Eldery diabetic patients are characterized by increasing frequency of GADA
sublimited titers as they aged. The autoantibodies low level may signify a less
aggressive beta-cell autoimmunity as well as instability of the immunological
system related to aging or both.
Comparison of plasma homocysteine concentrations (HYC) in patients
with acute coronary syndrome (ACS) and newly or previously
diagnosed type 2 diabetes
Maria Kurowska1, Jerzy S Tarach1, Wojciech Gernand2, Janusz Kudlicki3,
Adam Tarkowski3, Andrzej Nowakowski1, Teresa Czekajska3 &
Janusz Solski2
Dpt Endocrinology, Skubiszewski Medical University, Lublin, Poland;
Dpt Laboratory Medicine, Skubiszewski Medical University, Lublin,
Poland; 3Dpt Cardiology, Skubiszewski Medical University, Lublin, Poland.
The patients with ACS and scheduled for an elective coronary angiography have
high frequency of both newly and previously diagnosed diabetes. The diabetic
patients with acute myocardial infarction have an increased risk of death.
Elevated blood HYC is strongly related to an increased risk for atherosclerosis
and cardiovascular disease. This association is particularly evident in patients
with diabetes.
Aim of the study
An attempt to evaluate whether cardiovascular risk expressed by serum HYC in
ACS patients differs between groups of patients with newly or previously
diagnosed type 2 diabetes.
Group of patients
95 cases (30F and 65M) of which 71 pts (18F; 53M) without previously diagnosed
disorders of carbohydrate metabolism and 24 patients (12F and 12M) with
previously diagnosed type 2 diabetes. Patients aged 41–90 years.
In all patients the following parameters have been measured: 1 The blood glucose
level in the course of acute coronary disorders (admission glucose); 2 Fasting
blood glucose in the next day; 3 Serum HYC applying chemiluminescence
method (IMMULITE, DTC reagents). Diagnosis of type 2 diabetes has been
established according WHO criteria.
Patients with recent diagnosed t. 2 diabetes constituted 13% of group without
previously known symptoms of carbohydrate disorders. The mean admission
glucose level in the group with newly diagnosed diabetes was 151.8G26.9 mg/dl;
in the group with previously known diabetes was 218.8G127.1 mg/dl. Mean
HYC in the former group was 18.4G7.3 mmol/l (F-20.2G9.9; M- 17.5G
6.6 mmol/l) and 15.3G5.2 mmol/l (F-15.3G4.9; M-15.4G5.6 mmol/l) in the
latter, respectively. In the group with normoglycemia the mean serum HYC were
15.02G5.2 mmol/l (M-15.5G5.5 mmol/l, F-13.6G4.6 mmol/l).
The cardiovascular risk estimated according to serum HYC is higher in ACS
patients with newly diagnosed type 2 diabetes.
The association between carotid artery intima-media thickness and
cardiovascular mortality and morbidity in Type 2 diabetes: a retrospective study
Hayriye Esra Ataoglu, Mustafa Yenigun, Tayyibe Saler, Zehra Yigit,
Levent Temiz, Zuhal Saglam, Faik Çetin, Baki Kumbasar, Fuat Sar &
Suleyman Ahbap
Haseki Training and Research Hospital 4th Clinic of Internal Medicine,
Istanbul, Turkey.
Carotid artery intima-media thickness (CCA-IMT) highly correlates with
cardiovascular events in type 2 diabetes (T2DM). We aimed to determine the
cardiovascular mortality and morbidity incidence regarding CCA-IMT and
Framingham Score compared with preceding results of T2DM individuals. Our
aim was to determine whether ultrasonographic evaluation of carotid arteries may
predict cardiovascular mortality, morbidity and diabetic complications in T2DM
Demographic and clinical data of 102 T2DM individuals were registered
including blood pressure, HbA1c, lipid parameters, albumin excretion rate (AER),
ECG and ultrasonographic evaluation of carotid IMT and reevaluated seven years
later (2004). Primary end point was defined as cardiovascular mortality and
morbidity. Student-t test, regression analysis and [chi]2 tests were used. P!0.05
was significant.
The percentage of patients reaching primary end point was 45.10%. Age (PZ
0.043), diastolic blood pressure (DBP) (P!0.0001), systolic blood pressure
(SBP) (PZ0.004), A1c% (PZ0.042), (AER) (PZ0.017), triglyceride levels
(PZ0.038), IMT/CCA (PZ0.001) and percentage of coronary risk assessment
by Framingham Score were significantly high(PZ0.001) in patients presenting
with any of the primary end points. Reevaluation at the end of 7 years
revealed that measuring DBP, SBP and IMT/CCA was statistically important
at assessing the risk of presenting with any primary end points in T2DM
patients (Constant:P!0.0001).
Although Framingham Score predicts 10-year risk for cardiovascular mortality
and morbidity in diabetic patients, we suggest that DBP, hypertriglyceridemia and
microalbuminuria should also be included in risk scoring as well as the
measurement of carotid IMT.
Endocrine Abstracts (2007) Vol 14
9th European Congress of Endocrinology, Budapest, Hungary, 2007
Comparison of the effects of gliclazide and glibenclamide on insulin
resistance and metabolic parameters
Rabia Gokturk, Hayriye Esra Ataoglu, Mustafa Yenigun, Suleyman Ahbap,
Zuhal Saglam, Levent Temiz, Faik Çetin, Fuat Sar & Baki Kumbasar
Haseki Training and Research Hospital 4th Clinic of Internal Medicine,
Istanbul, Turkey.
It has been shown with many studies that sulphonylureas may have a negative effect
on parameters of insulin resistance while improving glucose regulation. However not
all of the sulphonylureas have the same effect. This analysis assessed the different
effects of sulphonylureas on some metabolic parameters of insulin resistance.
Newly diagnosed 25 T2DM individuals who were naive of oral antidiabetic therapy
were recruited and randomized to either long lasting gliclazide (30–90 mg/day;nZ
13) or glibenclamide (1–3 mg/day;nZ12) group. Body-mass index (BMI), waisthip ratio and blood pressure as well as biologic parameters like blood glucose,
A1c(%), BUN, creatinine, uric acid, lipid parameters, microalbuminuria, CRP,
insulin, c-peptide, glucagon, proinsulin and IGF1 levels were recorded at baseline
and at the end of the third month. The ratios of glucose/insulin, proinsulin/insulin,
HOMA-IR were assessed for each patient. Comparisons between groups were
performed by Students t test. [Chi]2 test was used for categorical variables. All
analyses were two sided with a significance level of [alpha]Z0.05.
By the end of three months, gliclazide caused a decrease in c-peptide and insulin
levels whereas glibenclamide resulted with a significant increase. Although insulin
resistance was decreased in both groups it was evident in glibenclamide group.
Creatinine levels were elevated in both groups which was significant with
glibenclamide group. Uric acid levels were decreased in gliclazide group contrary
to glibenclamide group in which uric acid levels were elevated.
Sulphonylureas have different effects on metabolic parameters of insulin resistance.
These data suggest that gliclazide has a lowering effect on hyperinsulinemia. Yet this
study is an observation based on small number of patients, studies with bigger
numbers and longer duration are required for confirmation.
24-hour ambulatory blood pressure and aortic dimensions in women
with Turner syndrome
Britta Hjerrild1, Keld Sorensen2, Erik Morre Pedersen3, Erik Lundorf3,
Arne Horlyck4, Jens Sandahl Christiansen1 & Claus Hojbjerg Gravholt1
Medical Department M (Endocrinology and Diabetes) and Medical
Research Laboratories, Aarhus University Hospital, Aarhus, Denmark;
Department of Cardiology, Skejby Hospital, Aarhus University Hospital,
Aarhus, Denmark; 3The MR Centre, Skejby Hospital, Aarhus University
Hospital, Aarhus, Denmark; 4Department of Radiology, Skejby Hospital,
Aarhus University Hospital, Aarhus, Denmark.
Study objective
To study blood pressure (BP) levels and aortic dimensions in women with Turner
syndrome (TS).
Materials and methods
102 women with TS (mean age 37.7 years; 18–62 years). 24 hour ambulatory BP
measurement and echocardiography was performed on participants.
Mean BP systolic (sys) and diastolic (dia) values were (GSD): sysBPday
128.0G15.3; diaBPday 81.6G11.8; sysBPnight 110.4G14.0 and diaBPnight
68.1G11.5. Heart rate (HR): 77.5G9.7.
Hypertension was found in a large proportion of the women: sysBPday.
36/97 (37%); diaBPday 44/97 (45%); sysBPnight 27/96 (28%) and diaBPnight 49/96
(51%). 34/97 (35%) did not have elevated BP levels, 22/97 (23%) had elevated levels
in all 4 measures. 19 women already received antihypertensive treatment, and sys BP
was significantly higher in this group. Aortic diameters (cm):
Aortic Annulus
Sinotubular level
Brachial trunk
% above cutoff
Endocrine Abstracts (2007) Vol 14
17 individuals had aortic diameters above expected levels. A positive correlation was
found between systolic BP (rZ0.36; PZ0.001) and age, but not weight or BMI. HR
correlated negatively to VO2max (rZ0.22; PZ0.038). We found no correlation
between BP and aortic diameters or age and aortic diameters. There was however a
significant increase in aortic diameters in TS with karyotype 45,X compared to others
(P!0.02) and in TS with bicuspid aortic valves (P!0.02).
Hypertension is common in TS, affecting more than 50% of the study group, and
subjects on antihypertensive treatment were insufficiently treated. Aortic
dimensions are larger in TS (17%), especially with the karyotype 45, X. In this
study we found no correlation between BP and aortic dimensions.
Plasma marker of lipid peroxidation and type 2 diabetes in subject with
coronary artery disease in Iranian subjects
Fariborz Haghparast & Jaffar Nourooz-Zadeh
Islamic Azad University-Larestan Branch, Larestan, Iran.
Abnormal lipid profile is an important risk factor in the development of
macrovascular atherosclerotic complications in patients with type 2 diabetes
mellitus (T2D). The aim of this study was to investigate the relationship between
lipid profile and lipid peroxidation in type 2 diabetics with and without coronary
artery disease (CAD).
Materials and methods
We studied 80 patients with T2D, 40 with CAD and 40 without CAD. We also
studied 50 non-diabetics, 30 with CAD, and 20 without CAD. Lipid profile was
estimated by the total, HDL, LDL cholesterol and triglyceride (TG). To evaluate
the oxidative status we measured circulating malondialdehyde (MDA), plasma
levels of superoxide dismutase (SOD), glutathione (GSH), as well as vitamin E
and C.
No significant difference was found in the lipid profile in patients with T2D and
CAD patients. There was significantly difference in the level of MDA between the
groups. In diabetics, MDA positively correlated with the total cholesterol, LDL
-C, total lipid, and the relations between LDL/HDL and TG/HDL (P!0.001). In
non-diabetic with CAD group, MDA positively correlated with total cholesterol,
(P!0.05). There was significant difference in the SOD, glutathione, vitamin E /
total lipid and vitamin C between the groups of diabetics and were lower in the
diabetes group with CAD (P!0.05). There were significant negative correlations
between MDA and vitamin E and C in groups with T2D, but it was statistically
significant in the non-diabetic with CAD (P!0.05).
Type 2 diabetes is associated with excess risk of CAD and primary therapy should
be directed first at lowering lipid peroxidation. CAD and T2D alone and
combined carry similar atherosclerotic burden concerning lipid profile, enzymatic
and nonenzymatic antioxidative status and lipid peroxidation.
Abstract unavailable
Effect of testosterone replacement therapy on adipocytokines in
hypogonadal men with Type 2 diabetes
D Kapoor1, S Clarke3, R Stanworth1, KS Channer2 & TH Jones3
Centre for Diabetes and Endocrinology, Barnsley NHS Foundation Trust
Hospital, Barnsley, United Kingdom; 2Department of Cardiology, Royal
Hallamshire Hospital, Sheffield, United Kingdom; 3Academic Unit of
Diabetes, Endocrinology and Metabolism, University of Sheffield, Sheffield,
United Kingdom.
Serum testosterone level is known to inversely correlate with insulin sensitivity
and obesity in men. Furthermore, there is evidence to suggest that testosterone
replacement therapy reduces insulin resistance and visceral adiposity in Type 2
diabetic men. Adipocytokines are hormones secreted by adipose tissue and
contribute to insulin resistance. We report a double-blind placebo controlled
crossover study in 20 hypogonadal Type 2 diabetic men examining the effect of
9th European Congress of Endocrinology, Budapest, Hungary, 2007
testosterone replacement therapy on adipocytokines and CRP. Patients were
treated with testosterone (Sustanon 200 mg) IM every 2 weeks or placebo for 3
months in random order followed by a wash-out period of 1 month before the
alternate treatment phase. At baseline, leptin levels significantly correlated
with BMI (rZ0.71; P!0.001) and waist circumference (rZ0.78; P!0.001).
There was also a significant inverse correlation between IL-6 levels and
total testosterone (rZK0.68; PZ0.002) and bioavailable testosterone levels
(rZK0.73; PZ0.007). CRP levels also correlated significantly with total
testosterone levels (rZK0.59; PZ0.01). Testosterone treatment reduced leptin
(K7141.9G1461.8 pg/ml;
(K2075.8G852.3 ng/ml; PZ0.02). There was a significant reduction in waist
circumference (K2.1G0.81 cm; PZ0.02). No significant effects of testosterone
therapy on resistin, TNF alpha, IL-6 or CRP levels were observed.
In conclusion, testosterone replacement treatment decreases leptin and
adiponectin levels in Type 2 diabetic men. Moreover, low levels of testosterone
in men are associated with inflammation, though testosterone treatment over 3
months had no effect on inflammatory markers.
secretory functions that are confirmed by meaningful increase of radionuclide
half-deduction time (T1/2) from the liver (60G4.16 vs 45.2G3.49, P!0.03).
Also a reliable T1/2 delay occurs in patients with type 2 diabetes and metabolic
syndrome comparing to healthy. But in patients with smaller body mass index was
found significant lowering of time of radiopharmaceutical occurrence in intestine
that testifies the hypotonia of Oddi’s sphincter. In patients with decompensation
stage of carbohydrate metabolism comparing to subcompensation occurs
meaningful increase of liver T1/2 that points on excretory function delay.
Nevertheless we have not found any significant relations between delay of liver
excretory function and HOMA, level of C-peptide, triglycerides, cholesterol,
HDL-cholesterol, LDL-cholesterol, WHR, arterial hypertension in patients with
type 2 diabetes and metabolic syndrome. Different impacts of per oral
hypoglycemic drugs displayed significant lowering of excretory function in
patients taking metformin comparing to those who were taking sulfonylurea due
to T1/2 elongation of liver (61.75G5.54 vs 39.75G6.62, P!0.05). The obtained
findings suggest that absorbing and excretory functions of liver slow down at
increase of BMI and decompensation stage in patients with type 2 diabetes and
metabolic syndrome. But other markers of metabolic syndrome are not defining in
early disturbances of liver excretory function in mentioned patients.
A role of the liver in the infringements of lipid metabolism of patients
with diabetes mellitus type 2 and metabolic syndrome
Vadim Korpachev1, Alla Kovalchuk1, Natalija Kushnareva1 &
Volodymyr Kovalchuk2
V.P. Komissarenko Institute of Endocrinology and Metabolism, Kyiv,
Ukraine; 2O.O. Bogomolets National Medical University, Kyiv, Ukraine.
Omega-3 polyunsaturated fatty acids in the treatment of cardiovascular
autonomic neuropathy in Type 2 diabetes mellitus patients
Victoria Serhiyenko, Alexander Serhiyenko & Ludmila Serhiyenko
Medical University, Lviv, Ukraine.
Different interdependences with symptoms of insulin resistance give us the
possibility to consider steatosis as a disorder of the liver with metabolic syndrome
The aim of study is to assess the role cholesterol-HDL in rise of diabetic
40 patients with Diabetes Mellitus type 2 (DM) and signs of MS were examined
to determine spreading of steatohepatosis as one of the factors of insulin
resistance. Only 8 of them didn’t have diabetic hepatopathy, while 32 patients had
adipose infiltration of the liver (according to the results of the ultrasonic
Actual difference between the two groups was revealed in the rate of HDL
decrease. So, if the patients with DM type 2 and symptoms of MS with
steatohepatosis have the rate of cholesterol-HDL decrease which is 34.36G4.2%
from the low norm measure, the patients with the same symptoms, but without
steatohepatosis, had 6.8G0.2% (P!0.05). We distinguished a group of patients
who had prevalent fasting hyperglycemia. Those patients who had prelevant
postprandian hyperglycemia formed the group of comparison. Analyzing the
findings, it is necessary to mention that the group of patients with prevalent
fasting hyperglycemia were effected by more serious disorders with lipid
metabolism, they had a lower level of cholesterol-HDL than those who had rather
high postprandian hyperglycemia (0.89G0.03 vs 1.027G0.05 mmol/l, P!0.05)
and rather high percentage of a waste circle growing that indicates of a greater
aggressiveness of MS factors.
Thus, it was determined that prevalent fasting hyperglycemia which effects
patients with DM type 2 and diabetic hepatopathy in condition of adipose
infiltration confirmed by echographic results is a proof of a major role of the liver
in the infringement of lipid metabolism that contributes to increasing of insulin
resistance due to, so called, ‘lipid toxity’.
Background and aims
The aim of this study was to assess the effects of docosahexaenoic (DHA) and
eicosapentaenoic acid (EPA) on the heart rate variability (HRV), some
biochemical parameters in patients (pts) with Type 2 diabetes mellitus and
cardiovascular aunonomic neuropathy (CAN).
Materials and methods
39 pts with CAN (54G5 yrs) were allocated in two groups: A (nZ26) were
receiving capsules of fish oil every day (2.0 g EPA, 2.0 g DHA and 0.1%
a-tocopherol acetate), B (nZ13) - placebo capsules of olive oil. We investigated the
activities of protein-kinase C (PK-C), NaC, KC-ATPase, Ca2C, Mg2C- ATPase in
the membranes of RBC’s, levels of the 125I-6-ketoprostaglandin F1alpha (6-ketoPGF1alpha), 125I-thromboxane B2 (TXB2) in the blood plasma.
The manifestation of the CAN is accompanied by decrease of the NaC, KCATPase, Ca2C, Mg2C-ATPase activities (P!0.001), 6-ketoPGF1alpha, EPA level
(P!0.001) with increase of TXB2, PK-C activity, stage of platelet’s aggregation,
QTc interval. After four months of treatment there were a decrease of TXB2 level
(141.2G15.4 pg/ml, P!0.001), activity of PK-C (14.46G4.52 pmol 32P/mg
protein per 1 min, P!0.001), degree and speed of an aggregate of thrombocytes
with simultaneous increase activities of NaC, KC-ATPase (0.1G0.004 mMol
Pi/mg protein per 1 hour, P!0.001), Ca2C, Mg2C-ATPase and the level of the
6-ketoPGF1alpha in the group A marked. Also, we observed significant
improvement of HRV parameters, decrease of QTc interval (P!0.01).
DHA and EPA at moderate doses may exert antithrombotic effects and may be used
for prophylaxis and treatment of patients with Type 2 diabetes mellitus and
cardiovascular aunonomic neuropathy.
Radionuclide study of hepatobiliary system function in patients with
type 2 diabetes and metabolic syndrome
Valentin Slavnov, Alla Kovalchuk, Vadim Korpachev &
Natalija Kushnareva
V.P. Institute of Endocrinology and Metabolism, Kyiv, Ukraine.
Nicotinamide and alpha-lipoic acid in the treatment of cardiovascular
autonomic neuropathy in Type 2 diabetic patients
Ludmila Serhiyenko, Alexander Serhiyenko & Victoria Serhiyenko
Medical University, Lviv, Ukraine.
The aim of the research is to study the functional state of liver parenchyma in
patients with type 2 diabetes and to analyze hepatobiliary system disorders
depending on marker of metabolic syndrome (MS).
The study involved 22 patients with type 2 diabetes and MS and 8 healthy
persons. Dynamic hepatoholecystoscintigraphy was performed using RKC 301T
gamma camera after Tc-99m mesida administration and bile-expelling meal.
We established a reliable increase of maximum accumulation time of
radiopharmaceutical in parenchymatous cells of the liver (22.0G3.76 vs 14.6G
0.83, P!0.01) comparing to healthy. Also these patients have infringements of
Background and aims
The present study has examined the effect of a-lipoic acid (ALA) and
nicotinamide (NA) on the heart rate variability (HRV), superoxide dismutase
(SOD), gluthation peroxidase (GPO), catalase activities, reduced gluthatione
(GSH), malondialdegide (MDA) contents in the RBCs’ in Type 2 diabetic patients
(T2DM) with cardiovascular autonomic neuropathy (CAN).
Materials and methods
59 patients with T2DM and CAN (59.3G7.9 years) were allocated to three
treatment group: (1) daily per os dose of ALA 600 mg (nZ29); (2) NA 700 mg
(nZ18); (3) ALA 600 mg and NA 700 mg (nZ12) during 2 months.
Endocrine Abstracts (2007) Vol 14
9th European Congress of Endocrinology, Budapest, Hungary, 2007
The progress of CAN is accompanied by decrease of the activities of SOD
(7.38G0.29, P!0.001), GPO and catalase (P!0001), the content of GSH and
increase of the MDA (P!0.001) in RBC’s. After 2 months of a treatment course
with ALA it the increasing spectral power in the low- and high frequency
(P!0.01), coefficient of variation (P!0.05). Simultaneously, activity of SOD,
GPO (P!0.001) and GSH concentration were authentically augmented, and the
contents of MDA, QTc interval parameters (0.52G0.057, P!0.05) was reduced
(P!0.01). Simultaneously introduction of NA and ALA is conducted with more
significant increasing SOD - 9.14G1.25 IU/ml Rbc’s, P!0.001; GPO 298.14G19.45 mcmol GSH/min Hb, P!0.001) and GSH concentration
(1.97G0.04 mcM/g Hb, P!0.001), TRAC (P!0.001), HRV, decreasing of
MDA concentration (P!0.001) and QTc interval parameters.
Usage of ALA and NA is accompanied by improvement of HRV, QTc interval,
antioxidant defence parameters and may be used for the treatment of CAN.
Plasma measures of oxidative stress and antioxidant status in type 2
diabetes mellitus
Fariborz Haghparast & Jaffar Nourooz-Zadeh
Islamic Azad University-Larestan Branch, Larestan-Fars, Iran.
The aim of this study was to test the hypothesis that type 2 diabetes mellitus is
associated with increased oxidative stress in Iranian subjects.
Materials and methods
The study population consisted of Fifty-nine patients with type 2 diabetes (mean
age 62.5G8.7 years). Type 2 diabetes was diagnosed according to the American
Diabetes Association criteria. 36 patients had diabetes complications and 23
patients had no complications. For the normal control subjects, fifty-five age- and
sex- matched healthy control subjects (mean age 63G5.7 years) were included.
Plasma a-tocopherol (a-ToH) was analyzed with HPLC. Malondialdehyde
(MDA), plasma glutathione (GSH), vitaminC and superoxide dismutase (SOD)
were spectrophotometrically measured. Total cholesterol, triacylglycerol, LDLcholesterol, HDL-cholesterol, HbA1c, uric acid, blood urea nitrogen (BUN) and
creatinine (Cr) were studied.
Plasma a–TOH-to-lipid ratio, glutathione and vitamin C levels were significantly
decreased in type 2 diabetes compared with controls (all P!0.05). Plasma vitamin C
and glutathione levels in diabetic patients with complications were significantly
lower than in those without complications (51.86G2.6 vs. 62.31G2.7 mmol/L, P!
0.001, 64.02G7.6 vs. 125.33G25.6 nmol/L, P!0.05, respectively). MDA
concentration was significantly higher in patients compared with controls (P!
0.005) as well as diabetes with complication compared to without complications
(P!0.05). Plasma levels of a–TOH/ total lipid was similar in diabetic patients with
or without complications. Plasma concentration of uric acid and SOD were
significantly lower in patients with diabetes than in control subjects.
Our results support the oxidative stress hypothesis for type 2 diabetes mellitus. We
therefore suggest that oxidative stress is an early stage in the disease pathology,
which may contribute to the development of complications.
Does screening of primary hyperaldosteronism only lead to diagnosis of
more adrenal hyperplasia?
Helga Sigurjonsdottir1, Mikael Gronowitz2, Ove Anderson3,
Robert Eggertsen4, Hans Herlitz5 & Gudmundur Johannsson1
Dept. of Endocrinology and Metabolism, Sahlgrenska University Hospital,
Gothenburg, Sweden; 2Nödinge Primary Care Center, Nödinge, Sweden;
Hypertension outpatient clinic, Sahlgrenska University Hospital, Gothenburg, Sweden; 4Mölnlycke outpatient clinic, Mölnlycke, Sweden;
Nephrology outpatient clinic, Sahlgrenska University Hospital, Gothenburg,
The prevalence of primary hyperaldosteronism (PA) has recently been reported as
high as 7.5% in patients with hypertension from unselected populations (USP)
and up to 22% in selected populations (SP). Whether increased screening and
Endocrine Abstracts (2007) Vol 14
diagnosis of PA will lead to more findings of curable PA (aldosterone producing
adenoma, APA) is unclear.
Three-hundred fifty-three consecutive patients with hypertension, age 20 to 88
years were included from two primary care centers (230 USP) and specialized
university hypertension outpatient clinics (123 SP) in the same catch-up area.
Plasma renin activity and serum aldosterone levels were sampled. Patients with
criteria for PA did positional and salt-loading test for confirmation. Further
investigation was with CT-adrenals, 131I-chol-scintigraphy and adrenal vein
sampling (AVS), with few exceptions. The local ethical committee approved the
Forty-six patients, 28 SP (22.8%) and 18 USP (7.8%), had criteria for PA. Six
USP and 22 SP were available for further investigation. Confirmation tests found
8 patients to be normal. Nine of eighteen (53%) CT-adrenals had positive
findings. Three of 17 (18%) 131I-chol-scintigraphies had positive findings. Ten of
14 AVS (71%) had positive findings. Four AVS were unsuccessful.
Supplementary information from 131I-chol-scintigraphy and CT-adrenals lead
to clear diagnosis in 3 of them, 1 AH and 2 APA. Further investigation after
screening lead to clear diagnosis in 27 of 28 (96%) patients, 8 AH, 11 APA.
The study confirms high prevalence of PA found in recent studies, higher in SP
than USP as expected. Our results indicate that screening for PA finds more
patients with curable cause of PA. All APA were from the SP group. Our findings
indicate that 131I-chol-scintigraphy is less accurate for diagnosing APA than
CT-adrenals and that the AVS is superior to both of them, further comparison of
the methods are needed.
Liquorice in moderate doses decreases serum levels of vitamin B12 but
does not affect the serum lipid levels
Helga Sigurjonsdottir1, Margret Arnadottir2 & Sven Wallerstedt3
Dept. of Endocrinology and Metabolism, Sahlgrenska University Hospital,
Gothenburg, Sweden; 2Dept. of Nephrology, Landspitali University
Hospital, Reykjavik, Iceland; 3Dept. of Internal Medicine, Sahglrenska
University Hospital, Gothenburg, Sweden.
Liquorice in moderate doses increases blood pressure (BP) in healthy individuals
(NT) as well as patients with hypertension (HT) due to increased cortisol effect.
Glycyrrhetinic acid, the active substance in liquorice, inhibits 11betahydroxysteroid-dehydrogenase type 2 (11betaHSD2) which converts the active
hormone cortisol to the inactive hormone cortisone. Recently it has been reported
that treatment with glucocorticoids decreases serum levels of cobalamin (B12), it
is also known that increased cortisol levels negatively affect different metabolic
risk-factors as serum lipids. Hence, it is possible that liquorice due to its increased
cortisol effect can decrease serum levels of B12 and affect the lipid levels
Thirty-six individuals, 25 NT (13 men and 12 women) and 11 HT (8 men and 3
women), 22–44 years old, consumed 100 g of liquorice (150 mg GA) daily for 4
weeks. Blood tests were taken, 24-hour-urin collected and BP measured before
and after the liquorice consumption. The study was approved by the local ethical
Serum-B12 decreased from 299G78 pmol/L to 284G78 pmol/L in the whole
group (nZ36, PZ0.005), from 322G77 pmol/L to 303G74 pmol/L
(PZ0.005) in the NT group and from 288G82 pmol/L to 270G77 pmol/L
(PZ0.007) in men. Serum levels for total-cholesterol, LDL-cholesterol, HDLcholesterol, triglycerides, apolipoprotein A1 and lipoprotein(a) did not change
after liquorice consumption. Serum levels for apolipoprotein B (ApoB)
decreased from 0.83G0.22 g/L to 0.81G0.22 g/L (PZ0.04) in the whole
group (nZ36). The ratio for urinary free cortisol/cortisone (Q, an indicator of
11betaHSD2-activity) increased significantly in all groups (P!0.001 in all
groups). No statistical difference was found between the genders or between
the NT-and HT-groups.
The glucocorticoid-effect induced by liquorice consumption in moderate doses
for 4 weeks is sufficient to significantly decrease the serum concentration of
B12, which is a novel finding. Even if the decrease is not substantial it can be
of clinical importance. This moderate dose of liquorice does not affect the
serum lipid levels.
9th European Congress of Endocrinology, Budapest, Hungary, 2007
Decreased insulin sensitivity in young lean hypertensive men is not
associated with increased visceral fat and changes in plasma
Adela Penesova1, Zofia Radikova1, Eva Cizmarova2, Vitazoslav Belan3,
Milan Vigas1 & Juraj Koska1
Institute of Experimental Endocrinology SAS, Bratislava, Slovakia; 2Outpatients Clinic of Pediatric Cardiology, Karlova Ves, Bratislava, Slovakia;
Radiological Clinic of Faculty Hospital, Bratislava, Slovakia.
Increased abdominal visceral adipose tissue (VAT) deposition is associated
with insulin resistance in obese and/or hypertensive patients. We investigated
the association of insulin sensitivity with the amount of VAT in young, lean,
non-treated males with recently established high normal blood pressure or
hypertension grade 1 (HT).
Subjects and methods
Twenty-one subjects with HT (age 20.3G0.6 years, BMI 22.4G0.5 kg/m2,
systolic BP 141G2, diastolic BP 73G2 mmHg, mean GSE) and 19 normotensive
controls (NT; age 23.1G1.0, BMI 22.1G1.4 kg/m2, systolic BP 117G3, diastolic
BP 67G2) underwent a 75-g oral glucose tolerance test (OGTT) and magnetic
resonance imaging for measurement of abdominal adipose tissue distribution.
Fasting concentrations of leptin and adiponectin, and fasting and post load
concentrations of glucose and insulin were measured in plasma. Indices of insulin
sensitivity Cederholm (ISICED), Matsuda (ISIMAT) and insulin resistance (IR
HOMA) were also estimated. Abdominal VAT and subcutaneous adipose tissue
depots (SAT) were measured from single transverse MRI scan in the space
between L4 and L5. The study was approved by the Ethics Committee of the IEE.
All subjects had normal fasting glucose levels and normal glucose tolerance.
HT patients had higher IR HOMA (2.4G0.4 vs. 1.2G0.1, PZ0.007) and
lower ISICED and ISIMAT (58G3 vs. 77G4, PZ0.0001 and 5.1G0.6 vs. 9.0G0.8,
PZ0.001, respectively) than NT subjects. The two study groups did not differed
in amount of VAT and SAT (31.80G8.63 vs. 47.35G6.78; 93.58G15.66
vs. 111.05G10.80 cm2, NS), and in plasma levels of leptin and adiponectin
(3.82G0.52 vs. 3.45G0.49 ng/ml; 1.71G0.40 vs. 1.40G0.21 mg/ml NS).
These results demonstrate that even lean subjects with recently established higher
blood pressure and with normal fasting and post-load glucose levels display signs
of insulin resistance. These changes were however not related to abdominal
adipose tissue distribution or circulatory levels of leptin and adiponectin.
Comparison of twice daily NPH insulin versus once daily glargine
insulin in the frequency of nocturnal hypoglycemia in Type2 diabetic
patients with congestive heart failure
Neslihan Kurtulmus1, Fatma Demirdogen2 & Tufan Tukek2
Vakif Gureba Educational Hospital, Department of Endocrinology,
Istanbul, Turkey, 2Vakif Gureba Educational Hospital, Department of
Internal Medicine, Istanbul, Turkey.
We had the aim to determine the insulin treatment strategy that could prevent or
decrease the occurrence of hypoglycaemia while providing better regulation of
blood glucose in Tip 2 diabetic patients with cardiac failure.
The patients demonstrating similar characteristics with respect to the age, body
mass index, the duration of diabetes and heart failure were randomized into two
groups as insulin glargine (n: 19) and NPH (n: 11). The subjects have been
prospectively followed up for 12 weeks.
Basal blood glucose level was detected as 197.21G69.01 in insulin glargine
group(group1), it was 175.45G52.26 in NPH insulin group(group2) (PZ0.339).
Basal postprandial blood glucose in group1 was found to be 191.42G63.42, it
was 186.18G81.82 In group2 (PZ0.857). The nocturnal(3.00 am) blood glucose
was 191.42G63.42 in group1, it was 186.18G81.82 in group2 (PZ0.857). In
group1, basal HbA1c value was 8.11G1.98, which was found to be 7.88G1.49 in
group2 (PZ0.728). At week 12 of insulin therapy, HbA1c value was 6.86G1.59%
in group1, markedly decreased compared to initial HbA1c value (P!0.001). In
NPH group, HbA1c was found to be 7.31G1.36% at week 12, which was also
lower than that at the beginning of the treatment, however this result was not
statistically significant (PZ0.417). The frequency of nocturnal hypoglycaemia in
group1 was detected to be 10.5%, compared to 9.1% in group2. In two groups did
not show any statistical difference related to the frequency of nocturnal
In our study, while the use of insulin glargine provided a better metabolic control
compared to NPH insulin,but it failed to decrease the frequency of nocturnal
hypoglycaemia in diabetic subgroup with cardiac failure.
Intravenous constant ghrelin infusion in healthy young men: sustained
cardiovascular effects of supraphysiological ghrelin levels
Esben Thyssen Vestergaard, Niels Holmark Andersen, Troels
Krarup Hansen, Lars Melholt Rasmussen, Niels Moller, Keld Sorensen,
Erik Sloth, Jens Sandahl Christiansen & Jens Otto Lunde Jorgensen
Aarhus University Hospital, Aarhus, Denmark.
The short-term cardiovascular effects of continuous ghrelin infusion in healthy
humans remain to be studied.
Fifteen healthy, young and normal-weight men volunteered to participate in a
randomized double-blind, placebo-controlled cross-over study. The local ethics
committee approved the study. We used a constant infusion of human ghrelin at a
rate of 5 pmol/kg body weight per minute for 180 minutes and measured peak left
ventricular myocardial systolic velocity Vmax, tissue tracking TT (GE Vivid Seven
with a 2.5 MHz transducer) and endothelium-dependent flow-mediated vasodilatation of the radial artery (Acuson Sequoia C256, 8 MHz linear array vascular
ultrasound transducer).
Ghrelin infusion increased serum ghrelin levels w6-fold (5.2 to 6.5) (P!0.001)
, Vmax increased w9% (PZ0.002), TT increased w10% (PZ0.004), while
endothelium-dependent flow-mediated vasodilation did not change (PZ0.10).
Concomitantly, growth hormone peaked after 60 minutes of infusion
(36.8G4.7 ng/ml, P!0.001), glucose levels increased 0.5G0.1 mmol/l
(P!0.001), free fatty levels increased 1.7-fold (PZ0.002), cortisol levels
increased 1.4-fold (P 0.002), while insulin levels were constant.
Supraphysiological levels of ghrelin persistently improve left ventricular function
in healthy young normal-weight men without changing endothelium-dependent
flow-mediated vasodilation. It remains to be studied whether ghrelin exerts direct
myocardial effects or indirect effects through the concomitant changes in glucose,
growth hormone, free fatty acids and cortisol levels.
Circulating retinol binding protein 4 and protein C inhibitor are not
related to insulin resistance
Miriam Promintzer1, Michael Krebs1, Anton Luger1, Martin
Georg Bischof1, Peter Nowotny1, Christoph Binder2, Harald Esterbauer2 &
Christian Anderwald1
Division of Endocrinology and Metabolism, Department of Internal
Medicine III, Medical University of Vienna, Vienna, Austria; 2Clinical
Institute of Medical and Chemical Laboratory Diagnostics, Medical
University Vienna, Vienna, Austria.
Recent data suggest that circulating retinol binding protein-4 (RBP4) is involved
in the pathogenesis of insulin resistance in rodents and humans. Moreover, protein
C inhibitor (PCI) which specifically binds retinoic acid was found to be increased
in myocardial infarction survivors who are also insulin-resistant.
Therefore, we investigated the association of insulin resistance with plasma
retinol binding factors (RBP4 and PCI active antigen) in nondiabetic humans with
high (IS; nZ20, f/mZ14/6, age: 47.2G1.9 years, BMI: 26G1 kg/m2) and low
(IR; nZ20, f/mZ14/6, age:45.5G1.7 years, BMI:28G1 kg/m2) insulinstimulated glucose-disposal (M), measured by 2-h hyperinsulinemic(40 mU†min-1†m-2)-isoglycemic clamp-tests.
M (80–120 min) was higher in IS (10.9G0.6 mg†min-1†kg-1) than in IR
(4.0G0.2; P!10–12). Fasting plasma RBP4 concentrations were comparable in
IS (4.4G0.3 mg/dl) and IR (4.6G0.3). Fasting plasma PCI active antigen was
similar in both groups (IS: 106.6G15.6%; IR: 95.3G4.0%). Plasma RBP4 and
PCI were not significantly related to M.
In conclusion, our data demonstrate that healthy, nondiabetic, insulin-resistant
humans do not show altered plasma retinol binding factors, such as RBP4 and
PCI. Both do not significantly correlate with insulin sensitivity. Thus, our findings
do not support the hypothesis of insulin sensitivity modulation by proteins
involved in retinol transport.
Endocrine Abstracts (2007) Vol 14
9th European Congress of Endocrinology, Budapest, Hungary, 2007
KCNJ11 and ABCC8 promotor variants in congenital hyperinsulinism
Klaus Brusgaard1, Khalid Hussain2, Lone Svargo1, Bendt Brock-Jacobsen1
& Henrik Christesen1
Odense University Hospital, Odense, Denmark; 2Great Ormond Street
Hospital, London, United Kingdom.
Congenital hypoglycemic hyperinsulinemia (CHI) is a clinical and genetic
heterogeneous entity. Clinical manifestations can vary from serious life
threatening to milder difficultly identifiable cases. Children who don’t react
adequate to medical treatment are subject to pancreatic recession. The molecular
ethiology are from recessive mutations of the ABCC8 (SUR1) and KCNJ11
(Kir6.2) to dominant mutations of the GCK or GDH genes. Focal dysplasia
characterised by loos of maternal Chromosome 11 and hereby ABCC8 and
KCNJ11 is a common cause of CHI. In some studies mutations in the ABCC8
promotor have been shown to cause CHI. In approximately 50% of the
incidences the disease is still genetically unexplained necessitating the search for
other genetic factors.
The purpose of the present study was to identify new genetic causes of CHI in
patients with a hitherto unexplained manifestation.
46 children and there parents was tested for mutations in the ABCC8 and
KCNJ11 promotors by D-HPLC and sequencing. Samples with deviating
chromatographic patterns were sequenced.
The a region covering 1063 bp including the minimal KCNJ11 promoter and
a region covering 930 pb including the ABCC8 minimal promoter was
analysed. In 13 samples a c.-507 del T mutation was found in the KCNJ11
gene. This variant has not previously been described. Using SIGSCAN and
TRANSFAC software possible transcription factor binding sites was predicted
in this region site. No other variants were found in either of the two genes. If
the c.-507 delT variant is a common cause of CHI in Denmark has to be
further investigated.
Polycystic ovary syndrome (PCOS) is associated with insulin resistance (IR)
and obesity, both predisposing factors to type 2 diabetes. A very recently
described adipokine, retinol-binding protein 4 (RBP-4), has been shown to
modulate insulin signalling and possibly lead to IR. At present, there is no data
that depict the relative expression of RBP-4 in either serum or adipose tissue of
PCOS women.
In women with PCOS compared to matched control women, we studied the
mRNA expression of RBP-4 from subcutaneous (sc) and omental (om) adipose
tissue and sc adipocytes. Furthermore, RBP4 protein levels were assessed in
adipose tissue; serum RBP4 was also determined.
Real-time RT-PCR and western blotting were used to assess the relative mRNA
and protein expression of RBP4. Biochemical measurements were also
conducted. The Local Research Ethics Committee approved the study and all
patients involved gave their informed consent, in accordance with the guidelines
in The Declaration of Helsinki 2000.
There was significant upregulation of RBP4 mRNA in both sc (P!0.05)
and om (P!0.01) adipose tissue of PCOS women, when compared to normal
controls; these findings were also reflected in isolated sc adipocytes (PCOS O
controls; P !0.01). In addition to elevated serum RBP4 levels in women with
PCOS (P!0.05), when compared to normal controls, RBP4 protein levels were
significantly greater in both sc and om adipose tissue of PCOS women
(P!0.05 and P!0.05, respectively).
RBP4, a new adipokine, is elevated in PCOS women. Our findings potentially
introduce a novel concept into the aetiopathogenesis of insulin resistance in these
Effect of L- carnitine supplementation on glycemic profile in patients
with type 2 diabetes mellitus
Rahebeh Sakerhosseini, Alireza Rahbar, Avid Saadat, Amir hamzeh Pordal,
Feroug azam Taleban & Banefsheh Golestan
National Nutrition and Food Technology Research Institute, Tehran, Iran.
It has been thought that L-carnitine is effective in improving insulin-mediated
glucose disposal either in healthy subjects or in type 2 diabetic patients,and
carnitine plays an important role in diabetes mellitus omplications (cardiovascular disease).
We designed this study to investigate the effects of oral L-carnitin administration
on fasting plasma glucose (FPG) and glycosylated hemoglob (HbA1c), in patients
with diabetes mellitus type II.
Materials and methods
The effect of L-carnitine on FPG and lipid parameters was investigated in 22 male
and 14 female type II diabetic patients, mean ageGSD was 51.3G3.7 years. The
patients were randomly divided into 2 groups (i.e. test and control groups). One
gram of L-carnitine or placebo was given orally three times a day to the test and
control groups respectively for a period of 12 weeks.
Fasting plasma glucose in the test group decreased significantly from 143G
35 mg/dl to 130G35 mg/dl (PZ0.03. There were no significant changes in
HbA1c, between the two groups.
L-carnitine significantly lowers fasting plasma glucose in type II diabetic patients
Raised serum, adipocyte and adipose tissue retinol binding protein 4
(RBP4) in women with polycystic ovary syndrome
Bee Kang Tan1, Jing Chen1, Sheryl Pua1, C Richard Kennedy2 & Harpal
S Randeva1
Warwick Medical School, University of Warwick, Coventry, West
Midlands, United Kingdom; 2University Hospitals Coventry & Warwickshire NHS Trust, Coventry, West Midlands, United Kingdom.
Endocrine Abstracts (2007) Vol 14
Polymorphisms of von Willebrand factor gene promoter modulate the
corticosteroid-mediated increase of VWF levels in Cushing’s syndrome.
Viviana Daidone1, Francesca Sartorello2, Nora Albiger1, Franco Mantero1,
Antonio Pagnan2, Alessandra Casonato2 & Carla Scaroni1
Division of Endocrinology, Department of Medical and Surgical Sciences,
University of Padova, Padova, Italy; 2Division of Intenal Medicine,
Department of Medical and Surgical Sciences, University of Padova,
Padova, Italy.
Cushing’s syndrome (CS) is associated with hypercoagulable state, mainly
dependent on corticosteroid-induced increase of von Willebrand factor (VWF)
levels, even though this does not affects all patients. In normals plasma VWF
levels are genetically determined by ABO blood groups and polymorphisms
G/C K1793, C/T K1234, A/G K1185, G/A K1050 of VWF promoter.
These SNPs segregate as haplotype 1 (G/C/A/G) and haplotype 2 (C/T/G/A)
with genotype 1/1 (GG/CC/AA/GG) associated with higher VWF:Ag levels
than genotype 2/2 (CC/TT/GG/AA), and intermediate VWF values in
heterozygote subjects (genotype 1/2). In this study we aim to investigate
the relationship between SNPs of VWF promoter and VWF levels in CS
patients, in order to evaluate whether glucocorticoid effects may be influenced
by VWF promoter genotypes.
50 patients with Cushing’s syndrome and 200 normal subjects were
Patients were divided by ABO blood group into groups A (increased VWF)
and B (normal VWF). While a significant difference in VWF levels was
observed between the two groups (P!0.001), cortisol values were similar
(PZ0.44). A direct correlation between cortisol and plasma VWF levels was
observed in group A (P! 0.001), while no correlation was found in group B
(PO0.1).Genotype distribution differed significantly between the two groups
being 25.8% genotype 1/1, 22.6% type 2/2 and 38.7% type 1/2 in group A, as
opposed to 0% type 1/1, 57.9% type 2/2 and 31.6% type 1/2 in group B
(PZ0.03) and their genotypes also differed from the controls (PZ0.003 for
group A, PZ0.03 for group B). Our findings suggest that corticosteroidmediated increases of VWF, and its associated prothrombotic state, are
dependent on peculiar haplotypes of VWF gene promoter. CS patients
presenting genotype 1/1 have a higher risk of developing thrombosis than
patients with genotype 2/2.
9th European Congress of Endocrinology, Budapest, Hungary, 2007
Circulating pro- and anti-inflammatory cytokines in women with
gestational diabetes
Mariusz Kuzmicki1, Beata Telejko2, Anna Zonenberg2,
Jacek Szamatowicz3, Adam Kretowski2, Agnieszka Nikolajuk2 &
Maria Gorska2
Department of Pathophysiology of Pregnancy, Medical University,
Bialystok, Poland; 2Department of Endocrinology, Diabetology and Internal
Medicine, Medical University, Bialystok, Poland; 3Department of Gynecology, Medical University, Bialystok, Poland.
Gestational diabetes mellitus (GDM) identifies a population of women at high risk
of subsequent type 2 diabetes mellitus, representing an early stage in the natural
history of the disease. Systemic inflammation is associated with the development
of type 2 diabetes but the data concerning pro- and anti-inflammatory cytokines in
patients with GDM are limited. The aim of our study was to investigate serum
concentrations of interleukin-8 (IL-8), IL-18 and IL-10 in pregnant women with
various degree of glucose intolerance. The group studied consisted of 58 patients
with GDM, 31 pregnant women with normal glucose tolerance (NGT) and 32
women with an abnormal result of a 50 g glucose challenge test (GCT) but a
normal result of 75 g oral glucose tolerance test (OGTT). Serum IL-8, IL-10,
IL-18 and CRP concentrations were measured by immunoenzymatic assays.
Patients with GDM had markedly higher IL-8 and IL-18 levels than women with
NGT (3.86G5.44 vs 0.8G0.57 pg/ml, PZ0.00001 and 264.4G111.98 vs
203.57G108.14 pg/ml, PZ0.0005, respectively), as well as significantly lower
IL-10 concentrations (1.37G2.04 vs 2.86G1.53 pg/ml, PZ0.00001). There were
no significant differences in interleukin levels between patients with NGT and
abnormal GCT. There were significant correlations between IL-8 concentration
and prepregnancy BMI (RZ0.2093, PZ0.031), insulin (RZ0.42075,
PZ0.00004), HOMA-IR (RZ0.45857, PZ0.000001), and glucose (RZ0.2030,
PZ0.03), as well as between IL-18 level and insulin (RZ0.20055, PZ0.0301)
and HOMA-IR (RZ0.20385, PZ0.028). IL-10 correlated inversely with insulin
(RZK0.26822, PZ0.0036) and HOMA-IR (RZK0.29127 PZ0.0016). CRP
correlated with insulin (RZ0.28875 PZ0.0017) and HOMA-IR (RZ0.28836,
PZ0.0019). Our results suggest that GDM is associated with elevated
concentrations of pro-inflammatory cytokines IL-8 and IL-18, as well as with
low level of anti-inflammatory IL-10. This association seems to be mediated in
part by the indices of insulin resistance.
Abstract unavailable
Metabolic improvement in diabetic patients with glucose continuous
monitoritation in real time
Cristobal Morales Portillo, Isabel Serrano Olmedo, Silvia Maraver,
Amaya Fernandez Arguelles, Juan Manuel Garcia-Quiros Muñoz,
Guillermo Martinez De Pinillos, Carmen De La Cuesta Mayor &
Angel Sendon Perez
Virgen Macarena Hospital, Seville, Spain.
To study if the use of continuous glucose monitoritation systems in real time
(GUARDIAN REAL TIMEw) in the diabetic patients could improve the
metabolic control.
Material and method
15 type 1diabetic patients studied (age: 33.8G13.40, years of evolution: 17.06G
11.32) in intensive treatment (5 multidoses, 10 insulin pump) which were made
one first blind 4 days long monitoritation to them, PERIOD 1 (P. BLIND) with
sensor CGMS Goldw. Next it was made another monitoritation with a real time
system with glycemia and alarms of hyperglycemia and hypoglycemia,
GUARDIAN RTw, PERIOD 2 (P. Real time). These 2 monitoritations were
consecutive in each patient, establishing in the second period the levels of alarm
of hypoglycemia in 50 mg/dl and hyperglycemia in 200 mg/dl. We studied in both
periods: Average glycemia Glycemia Variability, Percentage of time in
hiperglycemia (O180), normoglycemia and hipoglycemia (!70). A nonparametric test for matched up data was made (Wilcoxon)
% High
% Euglucemia
% Low
157.17G34.30 (110–224)
137.49G21.99 (115–203)
48.23G13.20 (25–75)
19.90G13.87 (1.23–56.03)
74.98G14.22 (43.97–98.77)
5.10G5.16 (0–17.00)
In our patients we observed during the monitoritation in real time: – longer time in
normoglycemia with decrease of the frecuency in hipoglycemia and hiperglycemia. – smaller glycemia variability.The monitoritation in real time could be a
useful tool at the time of assuring a better metabolic control and to diminish the
exhibition to hipoglycemias.
The role of stress related aldosterone secretion in essential hypertension
Athina Markou1, Ioannis Androulakis1, Aggeliki Gouli1,
Kostantina Dimitriou1, Achilleas Zacharoulis2, Kostantinos Papadopoulos2,
Theodoros Barlogiannis2, Evangelos Chariatis2, Antony Halapas2,
Eleni Kourlaba2, Despoina Ragkou1, Georgia Kondyli1 & George Piaditis1
General Hospital of Athens “G. Gennimatas”, Department of
Endocrinology & Diabetes Center, Athens, Greece; 2General Hospital of
Athens “G. Gennimatas”, Cardiology Department, Athens, Greece.
Approximately 90% of the hypertensive population is characterized as having
essential hypertension. Apart from renin and KC, ACTH plays an important role
in aldosterone secretion, being a potent stimulant under situations of stress. Up to
date, the association between stress and aldosterone-related hypertension has not
been studied and that is the aim of our study.
36 hypertensive patients and 14 matched for age and sex controls (BP !
140/90 mmHg), had baseline biochemical profile, TSH, cortisol, ACTH,
aldosterone, active renin and 24 hr urine NaC/KC measurements, followed by
a Bruce protocol exercise test aiming at the 80% of maximal effort according to
Froelicher normograms and repeated the hormonal profile at peak exercise. 17
hypertensines and 7 controls had a 0.03 mcg ACTH stimulation test.
Hypertensive patients on treatment were switched to a calcium channel blocker
for at least 3 weeks before. Exclusion criteria were any cause of secondary
hypertension, renal, hepatic or heart failure, ischemic heart disease and diabetes
mellitus. CT scan of the adrenals was performed in both groups.
Exercise test: baseline ACTH and aldosterone to renin ratio (ARR) did not differ but
at peak exercise hypertensives had statistically higher ACTH and ARR levels
compared to controls [35.97G5.59 (meanGS.E.M.) vs 23.24G4.25 pg/ml, PZ0.046
and 138.83G34.22 vs 55.22G34.45 pmols/L/pg/ml, PZ0.015].
0.03 mcg ACTH test: there was a trend towards higher values in ARR at peak in
hypertensives that did not reach statistical significance probably due to the low
number of patients.
Using an exercise test at sub maximal effort in order to mimic every day’s life
physical stress, we observed a higher response of aldosterone to stress in patients
with hypertension. Therefore, stress related aldosterone hyper secretion may play a
causative role in essential hypertension with major implications in its treatment.
Dialysis therapy and its complications
Evgeniya Bublik, Gagik Galstyan, Galina Melnichenko, Victor Safonov,
Euginy Shutov, Pavel Filipcev & Oleg Udovichenko
National Research Centre of Endocrinology, Moscow, Russia; 2Moscow
Sechenov Medical Academy, Moscow, Russia.
To study prevalence of foot complications in patients on dialysis therapy and
evaluate the role the haemodynamic changes during dialysis procedure in
development of foot problems.
Endocrine Abstracts (2007) Vol 14
9th European Congress of Endocrinology, Budapest, Hungary, 2007
109 dialysis patients, mean age 49 years. 60 of them had diabetes mellitus (DM):
29 on haemodialysis (HD), 31 on peritoneal dialysis (PD). Non-diabetic patients
(NDM): 24 HD, 25 PD.
Vascular status: doppler, photoplethysmography. Polyneuropathy: NDS. Monitoring of BP: during and after dialysis (follow-up period 14 months).
Peripheral vascular disease (PVD) was associated with DM (16 DM vs. 1 NDM).
Polyneuropathy: 51 DM, and in 7 NDM.
Ulcers were diagnosed only in DM patients (prevalence 25%). The number of
patients with diabetic ulcers was increased after starting dialysis therapy (from 4
to 12) and it was due to increasing neuroischemic ulcers (from 0 to 8, PZ0,016).
Transient intra- and postdialysis hypotension (TH) was determined in 15 HD, 5
PD. This group had significant fall of pressure in toe arteries during TH.
Neuroischemic ulcers were frequently diagnosed in the group with PVD and HD,
than with PVD and without HD; PZ0,001.
Diabetic patients on dialysis therapy have high risk of neuroischemic ulcers. TH
can intensify PVD and provoke neuroischemic ulcers.
The effect of interferon treatment on glucose metabolism in patients
with chronic hepatitis
Atilla Alev1, Ayse Kubat Uzum2, Ali Murat Tatli1, Fatih Oner Kaya1,
Iskender Dik1 & Burhan Bedir1
Istanbul Training and Research Hospital, Istanbul, Turkey; 2Istanbul
University, Istanbul Faculty of Medicine, Department of Internal Medicine,
Division of Endocrinology and Metabolism, Istanbul, Turkey.
In recent years, interferon (IFN) is used in treatment of chronic hepatitis and the
studies about the side effects of IFN therapy are increasing.
We aimed to investigate the effects of IFN therapy on glucose metabolism.
Materials and methods
Study group was consisted with 30 patients who were diagnosed as chronic
hepatitis. Sixteen of 30 were chronic hepatitis B and 14 were chronic hepatitis C.
Diagnose was confirmed by serology and liver biopsy. Patients with chronic
hepatitis B were prescribed alpha-IFN, 9–10 MU/three times/week and chronic
hepatitis C were given alpha-IFN, 3 MU/three times/week, subcutaneously. All
patients were evaluated by fasting plasma glucose concentrations (FPG) and oral
glucose tolerance test (OGTT) at the beginning and and at the 4th week of IFN
treatment. Diagnose of impaired fasting glucose (IFG), impaired glucose
tolerance (IGT) and diabetes mellitus (DM) was approved by American Diabetes
Association (ADA) criteria.
The study group was consisted of 16 (53.3%) female and 14 (46.7%) male
patients. Mean age was 42G13.67 years. Twenty eight patients had normal
FPG concentrations, whereas two had IFG. No patient had DM. Mean FPG
concentrations of chronic hepatitis B and C was 91.13G8.25 and 96.5G
97.07 mg/dl, respectively. At the 4th week of the therapy, we reevaluated
the patients for glucose metabolism. Difference between FPG levels before
and after treatment were not statistically significant (93.63G10.54 and
94.33G16.01 mg/dl; PO0.05). However OGTT results were affected by the
therapy. Nineteen patients (63.3%) had normal, six had IGT anf 5 had DM.
Mean glucose concentrations during initial and second OGTT were 106G
26.53 and 132G17 mg/dl respectively (P!0.001).
IFN treatment alteres glucose metabolism. Therefore, patients who had chronic
hepatitis and treated with IFN should be followed-up closely for diabetes
mellitus during and after the therapy.
Unacylated ghrelin (UAG) enhances the early insulin response to meal,
improves glucose metabolism and decreases free fatty acids levels in
healthy volunteers
Flavia Prodam1, Fabrizio Riganti1, Elena Gramaglia1, Andrea Benso1,
Barbara Lucatello1, Fabio Broglio1, Thierry Abribat2, Aart Jan van der Lely3
& Ezio Ghigo1
Dept. Internal Medicine – University of Turin, Turin, Italy; 2Alizé Pharma,
Lyon, France; 3Dept. Internal Medicine – Erasmus University, Rotterdam,
Endocrine Abstracts (2007) Vol 14
Ghrelin circulates in two different forms. Acylated ghrelin (AG), a natural
ligand of the GH Secretagogue receptor (GHS-R) type 1a, exerts several
biologic central and peripheral actions including stimulation of GH
secretion, but also modulation of insulin secretion, glucose and lipid
metabolism. Unacylated ghrelin (UAG), despite unable to bind the GHSR1a, is biologically active showing some influence in vitro and in vivo on
glucose and lipid metabolism likely mediated by still unknown receptors.
Based on these data, the aim of our study was to investigate the endocrine
and metabolic effects of prolonged UAG administration in humans in
physiological conditions. To this goal, the effects of UAG (1.0 mcg/kg/h
infused iv over 16 hours from 21.00 to 13.00 h) or saline were studied in 8
normal subjects who had isocaloric balanced standardized meals at h21.20
and h09.00. Blood samples were collected every 20 min. Compared to
saline, UAG infusion significantly modified the profile of all parameters,
except glucagon. Compared to saline, UAG decreased glucose (P!0.01) and
FFA AUCs (P!0.01). The glucose decrease during UAG was particularly
relevant at fasting during nighttime (P!0.01) while FFA profile was
reduced both post-prandially and at fasting(P!0.01). UAG did not modify
total insulin AUC; however, the early insulin response to both dinner (P!
0.01) and breakfast (P!0.05) was enhanced by UAG infusion that was
associated to decrease in the nighttime HOMA index (P!0.01). During
UAG, cortisol (P!0.01) and GH (P!0.05) AUCs were lower than those
during saline, but cortisol levels remained within physiological values. Thus,
the intravenous infusion of UAG in normal subjects enhances the early
insulin response to meals, improves glucose metabolism and insulin
sensitivity, and inhibits lipolysis. Thus, UAG displays a remarkable
metabolic impact suggesting a promising anti-diabetogenic action through
an original mechanism of action.
Weight-related concentrations of steroid hormones in patients of both
sexes with preserved gonadal function suffering from coronary artery
Zbigniew Sablik1, Anna Samborska-Sablik2, Jan Henryk Goch1 &
Krzysztof Kula3
Department of Cardiology and Cardiac Surgery, Medical University of
Lodz, Lodz, Poland; 2Department of Emergency Medicine and Disaster
Medicine, Medical University of Lodz, Lodz, Poland; 3Department of
Andrology and Endocrynology of Fertility, Medical University of Lodz,
Lodz, Poland.
To define concentrations (conc) of steroid hormones in patients (pts) with
preserved gonadal function, suffering from coronary artery disease (CAD), and to
assess their relations to patients’ weight.
Pts with coronarographically proved CAD: C-W group (gr)-52 women (W) in the
age 43G3 years, with stable menstrual rhythm, C-M gr-46 men (M) in the age
52G6 years. Healthy volunteers: H-W gr-15 W (H-W) in the age 41G4 years,
H-M gr-13 M in the age 51G6 years.
In all pts occurrences of common risk factors of CAD including values of body
mass index (BMI) and waist-hip-ratio (WHR) were defined. To assess
concentrations of hormones in pts of all grs blood samples from cubital vein
were taken at 8.00 a.m., in W in 4-7 day of sexual cycle. Using immunological
methods conc of estradiol (E2), testosterone (T), dehydroepiandrosterone
sulphate (DHEAS), follicle-stimulating hormone (FSH), luteinizing hormone
(LH), progesterone (P) and cortisol (Cort) were measured.
Only conc of T was significantly higher in C-W than in H-W (3.5G1.7 vs 2.4G
1.0 nmol/l, P!0.02). In C-W a negative correlation between BMI or WHR and
conc of T and DHEAS was found.
In C-M, comparing to H-M, conc of P and conc of Cort were higher (3.5G1.6 vs
1.4G1.0, P!0.001, and 345G97 vs 246G96 nmol/l, P!0.01, respectively) and a
there was a trend towards lower conc of T (10.3G3.8 vs 12.2G3.3 nmol/l, P!0.1).
In C-M we found a negative correlation of BMI or WHR with conc of P and DHEAS
and positive correlation with conc of E2. Because in C-M a positive correlation
between conc of P and T, and conc of P and Cort was present, there was an indirect
negative relationship between BMI or WHR and conc of T and Cort.
T is involved in pathogenesis of CAD and plays proatherogenic role in young
women and probably antiatherogenic role in men. In both sexes excessive weight is
a potent risk factor of CAD, because it influences conc of steroid hormones of
gonadal and adrenal origin including changing conc of T in unfavourable manner.
9th European Congress of Endocrinology, Budapest, Hungary, 2007
Diabetic patient’s evaluation of continuous glucose monitoring sensors
versus capillary glucose measurements
Guilermo Martı́nez De Pinillos Gordillo, Amaya Fernández-Argüelles &
Juan Manuel Garcı́-Quirós Jm
Hospital Virgen Macarena, Sevilla, Spain.
To evaluate the monitoritation systems acceptance: capillary glucose measurements and continuous glucose sensors (CGSM and GUARDIAN).
Research design and methods
15 diabetics patients were monitoritatied in two diferents periods of time. (Period 1:
Guardian, 86 hours long. Period 2: CGSM 72 hours long). Later, they had to fill a
satisfaction questionnaire concerning several aspects which were valued from 0–6.
Administration of DHEA was associated with 4.5-fold increase in DHEA-S
levels. Estrogen levels significantly increased after DHEA from 22.1G0.7 pg/mL
to 27.4G1.6 pg/L (meanGS.E.M.; P!0.05), while testosterone levels did not
changed. Fibrynogen concentrations significantly decreased in DHEA group from
4.5G0.3 g/L to 3.83G0.2 g/L (P!0.05 vs placebo). Changes of tissue
plasminogen activator (tPA) and plasminogen activator inhibitor-1 (PAI-1)
were not statistical significant (respectively: 8.37G0.4 ng/mL vs 8.93G
0.5 ng/mL and 82.3G6.3 ng/mL vs 92.7G9.1 ng/mL (meanGSEM; NS vs
placebo). Mean testosterone levels did change. Tolerance of the treatment was
good and no adverse effects were observed.
DHEA therapy in dose of 150 mg daily during 40 days in men with DHEAS levels
!2000 mg/l and angiographically verified coronary heart disease (CHD) was
connected with significant decreasing of fibrinogen concentration and increasing
of estradiol levels, and did not influence on plasminogen activator inhibitor-1
(PAI-1) and tissue plasminogen activator (tPA) plasma concentrations.
Table 1
Recomendable system
Wish to
with: work
social life
Insulin resistance and insulin secretion in non-diabetic acromegalic
Dan Niculescu1, Mariana Purice2, Radu Lichiardopol1 & Mihail Coculescu1
Carol Davila University, Bucharest, Romania; 2C. I. Parhon Institutute of
Endocrinology, Bucharest, Romania.
P! 0.05
The information given both by capillary mesearuments and continous clucose
sensors was valued positively by our patients without significative differences
between them but with a bigger acceptance with the Guardian. Real time
monitorization did not generate greater anxiety than the blind registry. Glucemia
sensors interfere in the daily life of the patients in most of the studied aspects but
less with the Guardian than the CGSM sensor.
Dehydroepiandrosterone therapy in men with verified coronary heart
disease: the effects on fibrinogen, plasminogen activator inhibitor-1
(PAI-1) and tissue plasminogen activator (tPA)
Michal Rabijewski, Lucyna Papierska & Wojciech Zgliczynski
Department of Endocrinology; Medical Center for Postgraduate Education,
Warsaw, Poland.
The aim of this study was to analyze the influence of DHEA therapy on
fibrinogen, plasminogen activator inhibitor-1 (PAI-1) and tissue plasminogen
activator (tPA) plasma concentrations in men with decreased serum DHEAS
levels and angiographically verified coronary heart disease (CHD).
Material and methods
The study included thirty men aged 41–60 years (mean age 52G0.90 yr) with
serum DHEAS concentration !2000 mg/l, who were randomized into a doubleblind, placebo-controlled, cross-over trial. Subjects completed the 80 days study
of 40 days of 150 mg oral DHEA daily or placebo, and next groups were changed
after 30 days of wash-out. Fasting early morning blood samples were obtained at
baseline and after each treatment to determine serum hormones levels
(testosterone, DHEA-S, LH, FSH and estradiol) and also fibrinogen, plasminogen
activator inhibitor-1 (PAI-1) and tissue plasminogen activator (tPA) plasma
To set up, in acromegaly without diabetes mellitus, a correlation between the
disease activity in GH-secreting adenoma (AA) - assessed by minimum GH
serum level during an oral glucose tolerance test (OGTT) - and severity of insulin
resistance (IR), assessed by HOMA-IR index.
75 out of 88 consecutive patients with acromegaly hospitalized in our department
were included in this study. 13 patients proved to have diabetes mellitus and were
excluded. Serum glucose, GH and insulin levels were measured by immunoradiometricassay basal and at 30, 60 and 120 minutes after a 75 g OGTT in 88
patients with active or cured acromegaly. IR was assessed using HOMA-IR index.
A value over 2.5 was considered indicating IR. An Ethical Committee approval
has been obtained for this study.
Out of 75 patients without diabetes mellitus, 36 subjects (48%) were presenting
with IR (34 with active disease, 2 cured). We found a significant positive
correlation (rZ0.56, P!0.001) between AA and HOMA-IR. The GH minimal
level corresponding to the intersection of the exponential regression curve with
the HOMA-IR level of 2.5 was 8.8 ng/mL, a cut-off point indicating IR with 82%
specificity and 78% sensitivity. The odds ratio for developing IR becomes
significant at a minimum GH level during OGTT of 2 ng/mL (odds ratio 7.6, 95%
confidence interval 2–29).
The severity of IR revealed by acromegaly correlates with GH production. A GH
serum level higher than 2 ng/mL during OGTT indicates an increased risk for
developing IR. This cut-off level of GH can be used as one of criteria of cured
disease, regarding the lack of metabolic effects.
Response to metformin treatment in adolescent siblings with familial
partial lipodystrophy of the dunnigan variety (FPLD) due to the R482W
LMNA gene mutation
James Ryan1, Patrick Kiely2, Vivion Crowley3, Michael Maher4,
Rosemary O’Connor2 & Domhnaill O’Halloran1
Department of Endocrinology, Cork University Hospital, Cork, Ireland;
Department of Biochemistry, University College Cork, Cork, Ireland;
Department of Clinical Chemistry, Trinity College, Dublin, Ireland;
Deparment of Radiology, Cork University Hospital, Cork, Ireland.
FPLD is a rare monogenic cause of insulin resistance. We document responses to
treatment with metformin in 2 adolescent sisters with FPLD due to heterozygosity
for R482W LMNA gene mutation.
The probands, aged 14 and 16 years, presented with secondary amenorrhoea,
hirsutism and progressive acanthosis nigricans. Phenotypically they showed central
obesity, nuchal enlargement, and thin muscular arms. These changes occurred postpubertally. Anthrpometric and metabolic parameters of the probands, their R482W
Endocrine Abstracts (2007) Vol 14
9th European Congress of Endocrinology, Budapest, Hungary, 2007
mutation positive father and three R482W negative sisters are shown in Table 1.
Proband B had impaired glucose tolerance at diagnosis. Limb MRI of the probands
Table 1
Baseline OGIS
Proband A
Proband B
Father C
Sibling D
Sibling E
Sibling F
showed almost complete absence of subcutaneous fat; neck MRI showed
lipohypertrophy. Liver ultrasound of the probands and father showed diffuse fatty
infiltrate. Both probands had cystic ovaries. A therapeutic trial with metformin in
both probands showed a modest improvement in insulin resistance scores(Table 1).
Proband A had regression of acanthosis nigricans, Proband B regained normal
glucose tolerance. Both regained menses.
This kindred demonstrate the classical phenotype associated with FPLD,
including marked insulin resistance. While FPLD may be rare, it is nonetheless
vital to recognise this condition, as it is associated with significant morbidity and
mortality. Furthermore, while lamin mutations are associated with different diseases
this particular mutation is not well studied. We document a modest decrease in
insulin resistance and regression of secondary amenorrhoea in response to
metformin. Further longitudinal studies are required to fully evaluate metformin
as a treatment modality for FPLD.
Insulin sensitivity and lipid levels in pateints with primary
Goran Cvijovic, Dragan Micic, Aleksandra Kendereski, Svetlana Zoric,
Mirjana Sumarac-Dumanovic, Danica Pejkovic & Maja Georgiev
Institute of endocrinology, diabetes and diseases of metabolism, Belgrade,
United States.
Patients with primary hyperparathyroidism (PHPT) are insulin resistant. The
effect of PHPT on lipid levels and low-grade inflammation leves is unknown. The
aim of our study was to estimate the cardiovascular risk profile in patients with
PHPT. Methods: In patients with PHPT (NZ19; age: 58.15G8.38 years; PTH
180.83G104.15 ng/l, calcium 2.97G0.19 mmol/l) insulin sensitivity (measured
using euglycemic hyperinsulinemic clamp - M value), lipids (total cholesterol,
HDL-C, LDL-C, triglycerides, ApoA1 and ApoB) and CRP levels were
measured. Results: There were low-normal level of insulin sensitivity (M
value: 4.29G0.52), slightly elevated levels of total cholesterol (6.07G
1.39 mmol/l) and LDL-C (3.72G1.04 mmol/l) and normal levels of HDL
(1.28G0.08 mmol/l), triglycerides (1.80G0.19 mmol/l), ApoA1 (1.54G
0.09 g/l), ApoB (1.19G0.09 g/l) and CRP (1.58G0.52 mg/dl) levels. There
were negative correlations between M index and total cholesterol (rZK0.56,
P!0.05) and Apo B (rZK0.77, P!0.05) levels, while there was positive
correlation between PTH and CRP levels (rZ0.55, P!0.05). In conclusion, lownormal insulin sensitivity and elevated levels of total holesterol and LDL-C were
observed in our group of patients with PHPT. Further evaluation of low-grade
inflammation is necessery in this group of patients.
of patients. The aim of our study was to evaluate the effect of surgical treatment
on insulin sensitivity in patients with PHPT. Methods: In patients with PHPT
(NZ19; age: 58.15G8.38 years) insulin sensitivity was estimated using
euglycemic hyperinsulinemic clamp (M value) before and 3 months after surgical
treatment. Results: There was significant reduction of PTH (180.83G104.15 vs
46.11G19.45, P!0.05) and calcium serum levels (2.96G0.19 vs 2.29G
0.17 mmol/l, P!0.05) after surgical treatment. We have observed low-normal
insulin sensitivity before operation with significant improvement after surgical
treatment (M value: 4.29G0.52 vs 8.21G1.44, P!0.01). There was no change in
BMI (25.72G3.70 vs 24.93G3.33 kg/m2, PO0.05) and waist/hip ratio (0.82G
0.11 vs 0.85G0.13, PO0.05) before and after operation (when the tests were
performed). There were no correlations between chages (%D) of M index and
PTH (rZ0.32, PO0.05) and calcium (rZ0.05, PO0.05) levels. In conclusion,
surgical treatment improves insulin sensitivity in patients with PHPT. The
mechanism of insulin resistance and its improvement after surgical treatment
remains unclear in patients with PHPT.
Insulin-sensitivity and glycaemic control improve on rosuvastatin
(RSV) treatment in hypertriglyceridaemic type-2 diabetes (T2DM)
Giorgio Silvani, Andreas Tartaglia, Silvia Acquati, Anna Laura Vacirca,
Antonella Bondi, Lorenza Gagliardi & Maurizio Nizzoli
Unit of Endocrinology, GB Morgagni-L Pierantoni Hospital, Forlı̀, Italy.
Studies on statins and insulin-sensitivity in T2DM are highly controversial. We
aimed to evaluate the effect of RSV in type-2 diabetic people and whether its
action may be phenotype-dependent, i.e. triglyceride (TG)-related (study
approved by the local Ethical Committee).
48 type-2 diabetic pts (22 M:26 F), in a poor glycaemic control with oral agents,
insulin or a combination therapy (unchanged over the study), were given RSV
10 mg for 12 weeks and stratified in 2 groups (23:25) by fasting TG-levels (!150
and 150–400 mg/dl), matched for age (59.7G9.8 vs 60.0G10.2 years), BMI
(29.8G4.9 vs 29.9G5.5 kg/mq), waist (103.9G10.8 vs 105.7G11.1 cm), HbA1c
(8.3G1.0 vs 8.5G1.2%), total cholesterol (TC) (245.8G33.6 vs 264.7G
26.1 mg/dl), LDL-C (167.2G31.2 vs 176.6G35.0), HDL-C (45.7G11.6 vs
44.0G14.4), and Apo-B (152.4G34.8 vs 170.2G28.1). Baseline- and 12-wk
samples were taken for TC, LDL-C, HDL-C, TG, Apo-B, HbA1c, fasting plasma
glucose and insulin. Homeostasis Model Assessment for Insulin-Resistance
(HOMA-IR) was calculated, baseline score being higher in the 2nd group (4.68G
1.0 vs 6.32G1.5 P!0.05).
In both groups RSV lowered LDL-C (K47.2 vs K45.8%) and Apo-B (K40.7 vs
K39.6%) significantly and to a similar extent. HDL-C was significantly increased
(C5.3 vs C4.4%) irrespective of changes in TG levels, mostly affected by RSV
in the 2nd group: 133.5G47.9 (K17.2%) vs 250.5G60.1 (K25.9%) P!0.001.
HOMA-IR correlated with TG (rZ0.21) and was significantly decreased by RSVtreatment in hyper-TG-group (3.35G0.9 vs 6.32G1.5 P!0.001), as far as
HbA1c showed a slight but significant improvement (K0.7% P!0.05), while no
change was detected in HOMA-score or in HbA1c level in normo-TG-one, BMI
and waist being not modified in both.
Perturbations in large-VLDL- and TG-metabolism generate an atherogenic lipid
profile in T2DM and are closely linked with insulin-resistance. So in our data
RSV improves HOMA-IR and HbA1c in hyper-TG type-2 diabetic pts by
lowering TG-levels and seems to have both phenotype-independent and –
dependent (TG-related) actions.
The effect of surgical treatment on insulin sensitivity in pateints with
primary hyperparathyroidism
Aleksandra Kendereski, Dragan Micic, Goran Cvijovic, Svetlana Zoric,
Mirjana Sumarac-Dumanovic, Danica Pejkovic & Maja Georgiev
Institute of endocrinology, diabetes and diseases of metabolism, Belgrade,
United States.
It was reported that patients with primary hyperparathyroidism (PHPT) are insulin
resistant, and that surgical treatment may improve insulin sensitivity in this group
Endocrine Abstracts (2007) Vol 14
Gestational diabetes mellitus and adiponectin levels
Cavit Culha, Suheyla Gorar, Rustu Serter, Yavuz Demir, Pinar Karakaya &
Yalcin Aral
Ankara Education and Research Hospital, Department of Endocrinology,
Ankara, Turkey.
Hypoadiponectinemia is known to be associated with insulin resistance, diabetes
and obesity. Since gestational diabetes is together with increased body mass index
(BMI) and decreased insulin sensitivity, the evaluation of adiponectin levels in
these patients is interesting. We investigated the relationship between adiponectin
and glucose tolerance during pregnancy and after delivery.
9th European Congress of Endocrinology, Budapest, Hungary, 2007
Materials and methods
We evaluated plasma adiponectin levels, insulin resistance and glucose tolerance
in women with gestational diabetes mellitus (GDM, nZ16) and in normal
pregnancies (controls, nZ18). Measurements were performed two times as in
28–31 weeks of pregnancy and at 3 months after delivery. Insulin resistance was
calculated by the homeostasis model assessment (HOMA-IR).
Four of the GDM patients remained as impaired glucose tolerance after delivery.
Adiponectin levels during pregnancy were significantly lower in women with GDM
compared to normal pregnancies (7.68G6.26 mg/ml vs 12.72G3.72 mg/ml;
P!0.01). Adiponectin levels increased significantly after delivery both in GDM
and control groups. Despite the increment after delivery, adiponectin remained
significantly lower in women with GDM compared to controls (11.75G6.11 mg/ml
vs 16.55G3.05 mg/ml; P!0.01). In HOMA-IR, the differences between two groups
before and after delivery, and also the changes with delivery within the groups, were
not found statistically significant. Adiponectin was correlated negatively with
HOMA-IR (rZK0.39, P!0.05), third-trimester BMI (rZK0.37, P!0.05) and
one-hour plasma glucose (rZK0.33, P!0.05); and positively with HDLcholesterol (rZ0.34, P!0.05) in women with GDM. These correlations including
the adiponectin-HOMA-IR one disappeared following the delivery.
Decreased adiponectin levels in GDM do not normalise instantaneously following
the delivery. The difference is more apparent in adiponectin levels than in HOMAIR. There is a moderate correlation between adiponectin and one-hour plasma
glucose in GDM.
Lipoprotein Lp(a) in patients with systemic lupus erythematosus.
Relationship with disease activity and anticardiolipin antibodies
Panagiotis Athanassiou1, Ifigenia Kostoglou-Athanassiou2,
Despina Papadopoulou1, Chrysoula Galanaki1, Thomais Kalogirou3,
Athanasios Kordalis3, Christodoulos Antoniadis1 & Philippos Kaldrymidis2
Department of Rheumatology, Asclepeion Hospital, Athens, Greece;
Department of Endocrinology, Metaxa Hospital, Piraeus, Greece; 31st
Department of Internal Medicine, Asclepeion Hospital, Athens, Greece.
Systemic lupus erythematosus (SLE) is a multisystem multifactorial autoimmune
disorder. The survival of SLE patients has been improved by the administration of
immunomodulatory therapy. Patients, however, are affected by late onset
complications of the disease such as atherosclerosis. Lipoprotein Lp(a) is a
known risk factor for the development of atherosclerosis.
The aim was to study Lp(a) levels and their relationship with disease activity in
SLE patients.
Patients with SLE, nZ74, aged 21–64 years, and normal controls, nZ74, of the
same age and sex were studied. In patients and controls the levels of hematocrit,
hemoglobin, erythrocyte sedimentation rate, C-reactive protein, antinuclear
antibodies, complement, anti-dsDNA antibodies, cholesterol, triglycerides, HDL,
LDL and lipoprotein Lp(a) were measured.
Lp(a) levels (normal values !30 mg/dl) were found increased in 23 of 74
(31.1%) patients with SLE and in 9 of 74 (12.2%) controls. Within the group of 23
SLE patients with increased Lp(a) levels 17 (73.9%) had active disease. In 11 of
23 (47.8%) SLE patients with increased Lp(a) levels anticardiolipin antibodies
were detected, while anticardiolipin antibodies were found in 12 of 51 (23.5%)
patients with Lp(a) levels within the normal range. All patients with active disease
and increased Lp(a) levels had renal and/or central nervous system involvement.
A strong relationship was observed between Lp(a) levels and anti-dsDNA
Lp(a) levels were higher in SLE patients. Increased Lp(a) levels were found to
be related to disease activity in SLE, specifically with renal and central nervous
system involvement and anticardiolipin antibodies. Increased Lp(a) levels may
contribute to the development of atherosclerosis and cardiovascular disease in
SLE patients.
Epidemiological studies indicate that rheumatoid arthritis (RA) patients have
increased mortality. Cardiovascular disease seems to be one of the major causes
of death in patients with RA. Lipoprotein disorders are observed in patients with
systemic autoimmune disorders as well as in patients with RA. Lipoprotein Lp(a)
is an independent risk factor for the development of cardiovascular disease.
The aim of the study was estimate lipoprotein Lp(a) levels and their
relationship with disease activity in RA patients.
Patients with RA, nZ92, aged 22–71 years and normal controls, nZ92, of the
same age and sex were studied. All the patients fulfilled the American College of
Rheumatology criteria for the diagnosis of RA. In patients and controls the levels
of hematocrit, hemoglobin, erythrocyte sedimentation rate, C-reactive protein,
cholesterol, triglycerides, HDL, LDL and lipoprotein Lp(a) were measured.
DAS28 disease activity index was calculated in all RA patients.
Lipoprotein Lp(a) levels (normal values !30 mg/dl) were found increased in
24 of 92 RA patients (26.1%) and in 11 of 92 controls (12%). Within the group of
24 RA patients with increased Lp(a) levels 18 (75%) had increased inflammation
markers and increased DAS28. A strong relationship was observed between Lp(a)
levels, erythrocyte sedimentation rate (P!0.01) and C-reactive protein
Lipoprotein Lp(a) levels were found increased in RA patients. RA patients
are at an increased risk for the development of atherosclerosis. The increase in
Lp(a) levels seems to be observed specifically in patients with active RA.
Inflammation may be the factor responsible for the increase in Lp(a) levels in
RA patients.
Impaired proinsulin secretion before and during oral glucose
stimulation in HIV-infected patients, who display fat redistribution
Steen B Haugaard2, Ove Andersen2, Ian Halsall4, Johan Iversen1,
Charles Nicholas Hales4 & Sten Madsbad3
Dept. Infectious Diseases, Hvidovre University Hospital, Copenhagen,
Denmark; 2Clinical Research Unit, Hvidovre University Hospital,
Copenhagen, Denmark; 3Dept. of Endocrinology, Hvidovre University
Hospital, Copenhagen, Denmark; 4Dept. of Clinical Biochemistry,
University of Cambridge, Cambridge, United Kingdom.
Beta-cell function of HIV-infected patients on highly active antiretroviral therapy
(HAART), who display lipodystrophy, may be impaired. An early defect in betacell function may be characterized by an increased secretion of 32–33 split
proinsulin (SP) and intact proinsulin (IP).
To address this issue the secretion pattern of SP and IP of 16 HIV-infected men
with lipodystrophy (LIPO) and 15 HIV-infected men without lipodystrophy
(NONLIPO) were studied during an oral glucose tolerance test (OGTT). All
patients received HAART. Insulin secretion rates were determined by
deconvolution of plasma C-peptide concentrations.
More LIPO than NONLIPO patients displayed diabetes mellitus and impaired
glucose tolerance than a normal glucose tolerance (LIPO 2/8/6 vs NONLIPO
1/2/12, PZ0.05). LIPO had increased fasting SP, IP, ratio of SP/IP, area under the
curve (AUC) of SP and IP during early phase of the OGTT (0, 10, 20 minutes),
and AUC-SP and AUC-IP during the late phase of the OGTT (45, 75,
105 minutes), respectively, compared to NONLIPO (Ps!0.05). LIPO exhibited
significantly increased fasting SP/IP ratio, fasting SP/insulin ratio and ratios of
total proinsulin to C-peptide during the OGTT. LIPO displayed increased
incremental secretion of IP during the first 10 minutes of the OGTT (P!0.05),
despite the fact that the incremental insulin secretion during this period did not
differ between LIPO and NONLIPO.
These data suggest that HIV-infected patients with lipodystrophy display major
perturbations of proinsulin secretion in the fasting state and during an OGTT,
which is compatible with the notion of a beta-cell dysfunction of such patients.
Lipoprotein Lp(a) in patients with rheumatoid arthritis and its
relationship with disease activity
Panagiotis Athanassiou1, Ifigenia Kostoglou-Athanassiou2,
Despina Papadopoulou1, Chrysoula Galanaki1, Thomais Kalogirou3,
Athanasios Kordalis3, Christodoulos Antoniadis1 & Philippos Kaldrymidis2
Department of Rheumatology, Asclepeion Hospital, Athens, Greece;
Department of Endocrinology, Metaxa Hospital, Piraeus, Greece; 31st
Department of Internal Medicine, Asclepeion Hospital, Athens, Greece.
Concentration of vasopressin and of N- terminated naturetic
propeptyde type B – potent predictors of survival of patients after
cardiac arrest
Anna Samborska-Sablik1, Zbigniew Sablik2, Wojciech Gaszynski3,
Jan Henryk Goch2 & Krzysztof Kula4
Department of Emergency Medicine and Disaster Medicine, Medical
University of Lodz, Lodz, Poland; 2Department of Cardiology and Cardiac
Surgery, Medical University of Lodz, lodz, Poland; 3Department of
Anaesthesiology and Intensive Therapy, Medical University of Lodz, Lodz,
Poland; 4Department of Andrology and Endocrynology of Fertility, Medical
University of Lodz, Lodz, Poland.
Endocrine Abstracts (2007) Vol 14
9th European Congress of Endocrinology, Budapest, Hungary, 2007
To assess concentration (conc) of arginine vasopressin (AVP) and conc of Nterminated naturetic propeptyde type B (NTpBNP) in patients (pts) after cardiac
arrest (CA) and their role for clinical state of pts after CA.
52 pts after CA, 36 men and 16 women, in the age 62G13 years. CA was caused
by ventricular fibrillation in 31 cases, by asystolia in 15 and by pulseless electrical
activity in 6. 28 pts died after CA (P-CA-D), 24 survived and were discharged
from hospital (P-CA-S).
Clinical state of pts after CA was assessed by common scales used in critical care:
Glasgow Coma Scale (GCS) and Acute Physiology and Chronic Health
Evaluation II (APACHE II). Venous blood samples to measure conc of AVP
and NTpBNP were taken from each patient just after admission to hospital and in
2 consecutive days at 8.00.
Just after CA mean conc of AVP was higher in P-CA-D than in P-CA-S (87G58
vs 60G46 pmol/l, but P!0.1). Mean conc of NTpBNP was higher in P-CA-D in
3 consecutive days, significantly in 1 day after CA (11,4000G112000 vs 45000G
58,000 pmol/l, P!0.027).
In logistic regression analysis as well in Kaplan-Meyer survival analysis
an important relation between conc of AVP just after CA and survival after CA,
and between levels of NTpBNP just after CA and in first day after CA and survival
was revealed.
We proved negative correlations among blood conc of AVP, conc of NTpBNP and
values of GCS and positive correlations among levels of them and values of
1-Mechanisms involving biological function of AVP and of brain naturetic peptide
play an important role for covalescence in early stage after CA.
2- Conc of AVP and NTpBNP are important predictors of survival after CA.
Power spectral analysis (PSA) of heart rate variability (HRV) in the
detection of cardiac autonomic neuropathy (CAN) in subjects with
diabetes mellitus
Amjed Khamis, SR Rizvi, Shu Hoashi, Marie Byrne, RG Firth &
Brendan Kinsley
Diabetes and Endocrine department, Mater Misercorea University Hospital,
Dublin, Ireland.
Standard Autonomic Function tests AFT may not detect subclinical CAN.
Modalities exist (Frequency Domain) using PSA of HRV, which may detect
subclinical CAN.
We performed standard AFTs (HR response to deep breathing, Valsalva, Tilt at
1 min and 6 min) and PSA of HRV on these tests in 46 subjects (29 DM and 17
Controls) matched for age and sex. We sought to establish if those DM subjects
considered normal by AFT would exhibit abnormalities in PSA of HRV. We
measured mean spectrum RR interval and LF/HF ratio (measures of
sympathovagal tone).
Diabetic Subjects were divided into group A (normal AFT), group B (any
abnormal AFT), and to subgroup B1–3 by number of abnormal AFTs.
We then sought to identify if subjects in Group A would demonstrate
differences in results of PSA of HRV tests compared to controls, which might
suggest subclinical CAN.
In standard AFT, HRV in deep breathing was 22G10 beats/min in Group A
and 20G6 beats/min in Control, PZNS. In contrast results of PSA of HRV
show that LF/HF ratio in deep breathing was 7.1G3.3 (Control), 3.3G1.6
(Group A) and 1.8G1.5 (Group B), 1.2G0.6 (GroupB2), 2.3G1.6 (Group B3),
P!0.01 Control vs Group A and Group B. P!0.001 Control vs Groups B1,
B2, B3.
LF/HF ratio to deep breathing is a useful parameter to detect presence of
subclinical CAN and to stratify severity of CAN. It may be useful as a
screening test for the presence of subclinical CAN in subjects with diabetes
Changes in plasma adiponectin during the treatment of diabetic
A Emre Yildirim1, Yavuz Selim Demir2, Abidin Ozturk1, A Ozden Barazi3,
Hacer Cetiner1, Gokcen Kilic1, Tugrul Ozcan1, Yasar Acar1,
Berrin Demirbas1 & Gul Gursoy1
Ankara Education and Training Hospital Department of Internal Medicine,
Ankara, Turkey; 2Ankara Education and Training Hospital Department of
Endocrinology and Metabolism, Ankara, Turkey; 3Ankara Numune
Education and Training Hospital Department of Biochemistry, Ankara,
Low plasma adiponectin concentrations are associated with diabetes mellitus.
Resuts from animal studies suggest that adiponectin plays an important role in
regulating insulin action. Leptin levels found to be low in patients with diabetic
ketoacidosis (DKA). The recent studies showed that insulin replacement during
DKA increased leptin concentrations. In our study, we aimed to determine the
effect of insulin replacement on serum leptin and adiponectin concentrations in
patients with DKA.
Our study included 31 patients (F/M) with DKA. 18 of 31 patients have been
treated with oral anti diabetic agents and 13 of 31 patients have been treated with
insulin treatment before admission. Leptin and adiponectin concentrations are
analyzed in samples which are collected on admission and at resolution of
ketoacidosis in 24–48 hours.
Mean age of the the patients was 46.7G17.3 years, mean period of diabetes was 7.1G
7.3 years, and body mass index was 26.5G4.3 kg/m2. There was a signifcant negative
correlation between plasma adiponectin levels and blood ketone concentrations on
admission (rZK0.66). Significant positive corelation between age and body masss
index was also determined (rZ0.477). While plasma adiponectin levels didn’t change
after DKA treatment (PZ0.095), leptin levels increased significantly (P!0.001). In
patients using oral antidiabetic agents adiponectin levels didn’t change (PZ0.103) but
leptin levels increased significiantly (PZ0.002) at the end of treatment. In the patients
using insulin therapy, adiponectin levels didn’t change (PZ0.56), however leptin
levels increased significantly (P!0.001).
In our study leptin levels are increased after the treatment of DKA. This result can be
described with the increase of calori intake and the regulation of glucose utilization in
adipocytes caused by insulin. Adiponectin levels found to be still low in DKA after
the treatment. These results could be explained by early period of treatment.
The aim of study was to evaluate glucose control in obese diabetics during six
months of treatment with glargin insulin in combination with metformin and
In beginning of study excluded patients who had coronary heart and kidneys
disease before. In study included 43 obese diabetics with type 2 diabetes [23 male
and 20 female, BMIZ29.82G1.91 kg/m2, aged 42–65 yr], who had previously
been treated with different orally antidiabetics. Previous treatment was without
results, because all treated patients had bed glicoregulation. Patients divided in
two groups. Both groups were without significant difference in BMI, age and sex.
Twenty five patients (14 male and 11 female) received glargin s.c. once a day and
metformin orally at the dose of 3!850 mg/d. Eighteen diabetics (10 male and 8
female) received glargin s.c. once a day and glimepirid orally at the dose of
2–4 mg/d. Glicoregulation evaluated by measuring fast blood glucose (FBG),
postprandial blood glucose (PBG) and HbA1c. Duration of study was six months.
Percentile, average and correlation analysis have been utilized in statistical
The results of study, after six months treatment with glargin and metformin, show
statistical significantly decreasing of FBG (6,7C/K1.4 mmol/l, vs 9.9C/K
2.9 mmol/l, P!0.05), PBG and HbA1c (7.0C/K1.3% vs 9.1C/K1.3%, P!
0.05). BMI decreased for 10% (27.1C/K0.9 kg/m2 vs 29.82G1.91 kg/m2). In
group treated with glargin and glimepirid FBG, PBG and HbA1c (7.7C/K1.2%
vs 9.3C/K1.1%, P!0.05) as well decreased but no more then group treated with
glargin and metformin.
Glargin in combination with metformin is more effective in treatment of obese
diabetics then glargin in combination with glimepirid.
Endocrine Abstracts (2007) Vol 14
Glicoregulation in obese diabetics treated with glargin insulin in
combination with metformin and with glargin in combination with
Zelija Velija-Asimi
University Clinical Centre of Sarajevo, Sarajevo, Bosnia and Herzegovina.
9th European Congress of Endocrinology, Budapest, Hungary, 2007
High-sensitivity C-reactive protein in diabetes mellitus type II
according to micral test findings
Zarida Hambali
University Putra, Malaysia.
Adrenocortical carcinosarcoma: first european case report
Frédéric Somda1, Julie Leger1, Laurent Guy2, Olivier Norha3,
Françoise Desbiez1, Jean-Paul Boiteux2, Jean-Louis Kemeny3,
Philippe Thieblot1 & Igor Tauveron1
CHU Gabriel Montpied, Endocrinology, Clermont-Ferrand, France; 2CHU
Gabriel Montpied, Urology, Clermont-Ferrand, France; 3CHU Gabriel
Montpied, Pathology, Clermont-Ferrand, France.
Cardiac complications account for three quarter of deaths among diabetic
patients. Many studies have shown that high-sensitivity C-reactive protein (hsCRP) correlated with the inflammatory process of atherosclerosis in the
coronary artery. This study is designed to determine the levels of plasma
hs-CRP in Type II diabetic patients with microalbuminuria and its association
with other biochemical markers used for diabetic monitoring. All biochemical
parameters were analyzed using HITACHI 919 Analyzer. Microalbuminuria
levels were assessed using Micral Test in 120 diabetics and 100 normal
subjects (control). hs-CRP is significantly higher among diabetics (P!0.05)
as compared to the control group. The concentrations of hs-CRP increases
significantly with increasing levels of microalbuminuria which are classified
into 0 mg/dL, 20 mg/dL and more than 50 mg/dL (P!0.01). Among
diabetics, hs-CRP is significantly higher in those with miroalbuminuria
compared to those without microalbuminuria (P!0.001). In contrast, hs-CRP
is not significantly correlated with fasting blood glucose, LDL-chol, total
cholesterol and triglyceride (PO0.05). This case-control study confirms the
findings of higher concentration of hs-CRP among diabetic patients and may
suggest the ongoing inflammation associated with atherosclerosis. This study
suggests that by measuring the concentration of plasma hs-CRP in addition to
other biochemical parameters as recommended by the Malaysian Clinical
Practice Guideline, a proper planning to monitor complications of coronary
artherosclerosis among diabetic patients with or without microalbuminuria can
be done.
Endocrine tumors and neoplasia – presented on Sunday
Localization of an ectopic adrenocorticotropin-secreting tumour using
F- Dopa PET/CT
Séverine Dubois1, Olivier Morel2, Patrice Rodien1,
Christian Jeanguillaume2, Bernard Enon3, Frédéric Illouz1, Jean-Paul SaintAndré4, Sylvie Girault2 & Vincent Rohmer1
Pôle d’Endocrinologie, Diabètes et Nutrition, Centre Hospitalier et
Universitaire, Angers, France; 2Pôle de Médecine Nucléaire et Cancérologie, Centre Hospitalier et Universitaire, Angers, France; 3Pôle de
chirurgie thoracique et cardiaque, Centre Hospitalier et Universitaire,
Angers, France; 4Département d’anatomo-pathologie et de cytologie, Centre
Hospitalier et Universitaire, Angers, France.
Ectopic adrenocorticotropin secretion (EAS) accounts for 10–15% of cases of
Cushing’s syndrome and comprises a spectrum of lesions from highly malignant
tumours to a variety of less aggressive neuroendocrine tumours. Selective
removal of the primary lesion is the optimal management. It is therefore
mandatory to localize the source of ectopic ACTH.
As no single test is accurate enough to distinguish the ectopic from the pituitary
sources of ACTH, no single imaging technique can itself identify every tumour
responsible for EAS.
We report on the use of Photon Emission Tomography (PET) scanning using
F-fluoro-Dopa in the localization of an occult ACTH-secreting carcinoid
An 18-yr-old man was referred for evaluation of EAS. Evidence for EAS
included: plasma ACTH and ß LPH levels above the normal reference range, no
serum cortisol suppression after high-dose dexamethasone suppression test,
normal pituitary MRI and lack of central to peripheral gradient on bilateral
inferior petrosal sinus sampling. The patient had a history of post-infectious
bronchiectasis since 6 years. The chest computed tomographic (CT) scan showed
a widespread lobar disease already known and compatible with bronchiectasis.
In-111 pentreotide scintigraphy was interpreted as normal. A low-intensity uptake
was seen on 18FDG PET scanning located in the middle right pulmonary lobe. As
the patient suffered from a respiratory infection, interpretation of this image was
difficult. An 18F-fluoro-dopa PET scanning revealed a pathologic uptake localized
in the right lung middle lobe.
The pulmonary lesion was surgically treated after adrenolytic medication.
Histology revealed a bronchial carcinoid tumor. Hypercortisolism was replaced
by prolonged corticotropic insufficiency. Until now, hypercortisolims did not
In conclusion, no imaging technique should be neglected in the localization of
an occult EAS.
Adrenocortical sarcoma is an extremly rare tumour associated with a quite
pejorative evolution.We report the case of a fifty-eight years old woman
presenting a chronic asthenia and acute flank pain. She had no hypertension, no
clinical sign of virilization or hypercorticism. Abdominal ultrasonography
revealed an 8 centimeters mass above the right kidney. CT scan aspect evoked
an adrenal carcinoma embolizing vena cava. Hormonal assays did not reveale any
inappropriate secretion (17 alpha hydroxyprogesterone, 11 desoxy-cortisol,
cortisol, dehydroepiandrosterone-sulfate, delta-4 androstenedione, testosterone,
aldosterone, renin, 24-hour urine metanephrine and normetanephrine). A radical
adrenalectomy associated with a nephrectomy was performed. Tumour measured
13!7.5!5 centimeters, weighed 760 grams. Histological study confirmed the
diagnosis of adrenal carcinoma, but described a sarcomatous component
occupying nearly twenty percent of the total mass. Immunohistochimical
labelling was positive for anti-vimentin, anti-desmin and anti-actin antibodies.
In addition to surgical resection, the patient received mitotane as adjuvant
treatment (6 g per day, mitotanaemia: 20.6 mg/l). After a 16 month evolution,
physical exmination, CT scan, PET scan and hormonal monitoring don’t show
any evidence of local reccurence or metastasis. In the last twenty years, only four
cases of adrenocortical carcinosarcoma have been reported in literature. One was
a non secreting tumor, the three others were revealed by aldosterone, androgen or
catecholamine secretion. Considering pathology, one had an osteogenic and
chondroid differenciation, the two others a rhabdomyosarcomatous differenciation. To our knowledge, this is the first observation of an adrenal carcinosarcoma
expressing a smooth muscle phenotype. The strikingly good evolution in our
patient is also particularly unusual. Indeed adrenocortical sarcoma is a cancer
with a very poor prognosis since in all other cases, life expectancy after diagnosis
has never exceeded 8 months.
The genetic association of medullary thyroid carcinoma with Hirschsprung’s disease
Sarka Dvorakova1, Eliska Vaclavikova1, Richard Skaba2, Petr Vlcek3 &
Bela Bendlova1
Dept. of Molecular Endocrinology, Institute of Endocrinology, Prague,
Czech Republic; 2Dept. of Pediatric Surgery of the 2nd Faculty of Medicine,
Charles University and Hospital, Prague, Czech Republic; 3Dept. of Nuclear
Medicine and Endocrinology of the 2nd Faculty of Medicine, Charles
University and Hospital, Prague, Czech Republic.
Medullary Thyroid Carcinoma (MTC) can be associated with Hirschsprung’s
disease (HSCR). Mutations in exon 10 of the RET proto-oncogene were found in
patients with co-occurrence of HSCR and MTC. The aim of the study was to
screen the MTC risk exons in patients with HSCR. The genetic analysis
comprised 73 HSCR patients (53 males, 20 females) who were operated on and
followed-up during 2001-2006. The cohort consisted of 48 patients with classical
HSCR, 11 with long colonic aganglionosis and 14 with total colonic
aganglionosis (TCA). DNAs were isolated from blood after signing informed
consent approved by ethical committee. HSCR patients and 10 available family
members were tested for RET mutations in exons 10,11,13,14,15 and 16. Direct
sequencing revealed RET mutations in 7 (9.6%) HSCR patients. Three groups of
mutations were detected. Typical MTC risk mutations were found in 2 HSCR
patients with TCA: Cys609Tyr and Cys620Arg (both exon 10). Atypical mutation
Tyr791Phe (exon 13) was detected in 2 classical HSCR patients. This mutation is
causative for MTC only and has not been associated with HSCR till now.
Novel mutations with unknown function for HSCR and MTC were found in
3 patients – del603(A) (exon 10), Gly798Ser (exon 13) and Ser649Leu (exon 11).
Two of these patients had TCA and the third one had classical HSCR. MTC
developed in 2 patients and 2 family members with typical mutations for HSCRMTC. These mutation carriers underwent total thyroidectomy (TTE), the other
RET positive patients are screened for calcitonin level and they are without TTE
till now. Results showed the benefit of systematic RET mutation screening in
HSCR families in order to identify the risk of MTC. We recommend to investigate
not only exon 10 but also other MTC risk exons in all HSCR patients. This work
was supported by grant GACR 301/06/P425.
Endocrine Abstracts (2007) Vol 14
9th European Congress of Endocrinology, Budapest, Hungary, 2007
Inhibition of C17,20-lyase activity by new 17b-exo-heterocyclic androsterone derivatives
Mihály Szécsi1, István Tóth1, János Wölfling2, Gyula Schneider2 &
János Julesz1
Endocrine Unit and Research Laboratory, University of Szeged, Szeged,
Hungary; 2Department of Organic Chemistry, University of Szeged, Szeged,
17a-Hydroxylase-C17,20-lyase (P45017a) is a key regulator enzyme of the steroid
hormone biosynthesis in both the adrenals and the testes. Inhibition of this
enzyme can block androgen synthesis in an early step, and may thereby be useful
in the treatment of prostatic carcinoma, which is androgen-dependent in the
majority of cases. Abiraterone and its analogues have been found strong inhibitors
of P45017a suggesting that steroid derivatives with heterocyclic substituent on the
C-17 position may bear such potential.
We investigated inhibitory effect on C17,20-lyase exhibited by newly
synthesised androsterone derivatives with heterocyclic 17b substituents. C17,20lyase inhibition was tested via conversion of 17a-hydroxy-progesterone to
androst-4-en-3,17-dione in the homogenate of rat testis in vitro. Incubation was
carried out with 14C labeled substrate at 37 8C for 20 min. Following an
extraction procedure and isolation by thin layer chromatography, the enzyme
product and the residual substrate were quantified by their radioactivities.
Ketokonazole, a P45017a inhibitor applied in medical practice was used as a
reference compound. Among test compounds the non-substituted tetrahydrooxazolone and tetrahydrooxazinone derivatives were found to be the best C17,20lyase inhibitors; IC50 values were 4.2 and 6.0 mM, respectively. The N-phenyltetrahydrooxazinones did not show substantial inhibition (IC50 O50 mM).
The 17b-exo-heterocyclic androsterone derivatives which proved to be
potential C17,20-lyase inhibitors in the present study, also exhibited marked
inhibition against prostatic 5a-reductase activity in our previous investigations.
This dual effect might be particularly beneficial in the therapy of prostate cancer.
Milanese, Italy; 3Institute of General Pathology, Laboratory of Clinical
Pathology, University of Milan, Milan, Italy.
An increased cardiovascular risk has been described in patients (pts) with
adrenal incidentaloma (AI), similarly to pts with overt Cushing’s syndrome
(CS). Some echocardiographic abnormalities and alterations in adipokine
secretion involved in insulin resistance, inflammation and atherosclerosis have
been reported in pts with CS. In this study the possible correlation between
echocardiographic parameters and adipokine levels in pts with AI was
Subjects and methods
Morphological and functional echocardiographic characteristics and plasma IL-6,
TNF-a, MCP-1 and resistin levels (ELISA methods) were studied in 7 pts (60.0G
2.5 yrs, BMI 31.1G2.1) with AI and subclinical Cushing’s syndrome (SCS) and
in 17 pts (58.8G2.3 yrs, BMI 29.5G1.2) with non functioning masses. All
adrenal masses were identified as cortical adenoma. In all pts plasma ACTH,
serum cortisol and urinary free cortisol (UFC) were measured.
In pts with SCS the interventricular (IV) septum thickness was significantly
greater than in pts with non functioning masses (13.2G0.1 vs 10.7G0.03 mm,
P!0.05) and in 8 obese normotensive subjects (10.5G0.5 mm, P!0.001).
Plasma IL-6, TNF-a, MCP-1, and resistin levels were higher in pts than in 20
normal subjects (60.3G2.5 vs 5.5G0.6 pg/ml, 27.2G1.3 vs 22.1G1.4 pg/ml,
164.3G17.0 vs 104.3G19.4 pg/ml, 12.9G2.4 vs 5.1G0.2 ng/ml, respectively,
P!0.05). The other echocardiographic parameters and adipokine values were not
different in pts with SCS and with non functioning AI. In all patients, UFC
excretion positively correlated with left ventricular (LV) diameter end-systole
(rZ0.549, PZ0.01) and with LV mass (rZ0.479, P!0.05). Significant
correlations were found between early wave diastolic filling velocity and IL-6
and TNF-a levels (rZK0.633, PZ0.01 and rZK0.547, P!0.05, respectively),
and between late wave diastolic filling velocity and TNF-a levels (rZK0.520,
P!0.05), in all pts.
In AI a long-lasting exposure to an even slight cortisol excess and inflammatory
stimuli might be responsible for a gradual impairment of both diastolic function
and cardiac morphology.
Cigarette smoking increases high calcitonin levels
Michele d’Herbomez1, Catherine Bauters2, Laurence Leclerc2,
Emmanuelle Leteurtre3, Bruno Carnaille4, Jean-Louis Schlienger5,
Philippe Caron6 & Jean-Louis Wémeau2
Nuclear Medicine, Lille, France; 2Endocrinology, Lille, France; 3Pathology, Lille, France; 4Endocrine Surgery, Lille, France; 5Internal Medicine,
Strasbourg, France; 6Endocrinology, Toulouse, France.
Increased basal or pentagastrin-stimulated calcitonin level is the cornerstone for the
biological diagnosis of medullary thyroid carcinoma, but is also observed in patients
with C-cell hyperplasia (CCH) of the thyroid. In a prospective multicenter study we
re-evaluated the reference ranges of basal calcitonin (bCT) in 287 euthyroid controls
without thyroid disease (142 men-45 smokers, 3 deprived, 145 women-27 smokers).
The CT levels were measured using 2 different assays (Cis-Bio International,
Advantage Nichols). After exclusion of the main causes of increased CT levels, 11
(8%) male controls had bCT concentrations O10 pg/mL within the two assays. All,
except one, were active or deprived smokers. Then, we evaluated preoperative bCT
and pentagastrin-stimulated CT levels in patients with CCH of the thyroid (more than
50 C cells per field at 3 low-power magnification microscopic fields). In 27 smokers or
deprived patients (23 men and 4 women, median age 53 years) total thyroidectomy
was performed for nodular pathology. CCH was diffuse and bilateral (nZ17), diffuse
and unilateral (nZ4), nodular (nZ1) or diffuse and nodular (nZ5). Preoperative bCT
was normal (!10 pg/mL), between 10 and 20 pg/mL or O20 pg/mL in 8, 13, and 6
patients, respectively. Pentagastrin- stimulated CT level was normal (!50 pg/mL),
between 50 and 100 pg/mL, and O100 pg/mL in 2, 3, and 15 patients respectively.
In conclusion, there are evidences that cigarette smoking induces: 1) diffuse and
bilateral CCH of thyroid, 2) increased bCT level, 3) abnormal pentagastrin-simulated
test, particularly in men.
Cortisol excess, inflammatory markers and echocardiographic alterations in adrenal incidentalomas
Federica Ermetici1, Alexis Malavazos1, Calin Coman2, Lelio Morricone1,
Massimiliano Corsi3 & Bruno Ambrosi1
Endocrinology Unit, Department of Medical and Surgical Sciences, IRCCS
Policlinico San Donato, University of Milan, San Donato Milanese, Italy;
Echocardiographic Unit, IRCCS Policlinico San Donato, San Donato
Endocrine Abstracts (2007) Vol 14
Prognostic value of anti-thyroperoxidase antibodies in high malignancy
degree breast cancer
Emilio Fiore1, Claudio Giani1, Elisa Giustarini1, Ilaria Muller1,
Claudia Mammoli1, Daniela Campani3, Manuela Roncella2,
Loredana Fustaino2 & Aldo Pinchera1
Department of Endocrinology and Metabolism, Pisa, Italy; 2Department of
Surgery, Unit of Senology, Pisa, Italy; 3Department Pathology, Pisa, Italy.
A high incidence of serum anti thyro-peroxidase antibodies (TPOAb) has been
found in breast cancer (BC). Aim of this study was to evaluate the predictive
value of TPOAb in BC. The study group included 47 women submitted to
mastectomy for high malignancy degree BC (tumor size O5 cm and/or n8
lymph-nodes O3), followed for 5 years. No patient had distant metastases. All
were evaluated for thyroid disorders after breast surgery and before any antitumoral adjuvant therapy. Thirty-one out of 47 (65.9%) patients were alive 5
years after BC diagnosis (survivors group: SG), 16/47 (34.1%) were dead
during follow-up (deaths group: DG), (mean age 53.1G10.9 yrs and 53.3G
8.5 yrs, respectively) (p NS).
Estrogen Receptor (ER) was measured in 43/47 (91.5%) BC speciments.
ER was detected (ERC) in 19/30 (63.0%) patients in SG and 3/13 (23.1%)
in DG (PZ0.01, x2 5.9). Five year mortality in ER- BC was 10/21 (47.6%),
and in ERCBC was 3/22 (13.6%) (PZ0.008). The overall prevalence of
TPOAb was 15/47 (31.9%); 14/31 (45.1%) patients in SG and 1/16 (6.2%) in
DG were TPOAbC (PZ0.008). Five years mortality was 15/32 (46.9%) in
TPOAb- and 1/15 (6.7%) in TPOAb C (PZ0.01). TPOAb were detected in
8/21 (38.1%) ER- patients and in 7/22 (31.8%) ERC; no relation was found
between ER expression and TPOAb positivity (x2 0.2; p 0.7). Age at
diagnosis was not significantly related to five years survival (O.R. 0.98;
95%C.I. 0.92–1.04; PZ0.6). Absence of ER expression (O.R. 6.54; 95%C.I.
1.70–25.21; PZ0.006) and absence of TPOAb (O.R. 9.37; 95%C.I. 1.21–
72.67; PZ0.03) were related to a higher mortality rate. REC and TPOAbC
are positive prognostic parameters in BC and the absence of any relationship
between them seems to propose an independent role on the prognosis of BC
9th European Congress of Endocrinology, Budapest, Hungary, 2007
Bone density in patients with non-functioning pituitary adenomas
Stefan Fischli, Christoph Stettler, Rahel Sahli, Silvia Schwab,
Bernard Chappuis, Stefan Jenni, Peter Diem & Emanuel Christ
Department of Endocrinology, Diabetology and Clinical Nutrition,
University Hospital of Bern, Inselspital, Bern, Switzerland.
Surgically treated patients with NFA often present with secondary hypogonadism.
Hypogonadism is a well known risk factor for osteopenia or osteoporosis. The
aim of this study was to assess (a) the frequency of osteopenia/osteoporosis in a
single centre Swiss cohort of patients with operated NFA and (b) whether gender
or hypogonadism impacts on bone density at follow up.
Data of patients with NFAs diagnosed between 1967 and 2005 were analysed.
Clinical and endocrinological parameters were recorded before, immediately
after surgery and at last follow-up. Bone densitometry (DEXA) was performed
during follow up. Data were analyzed using Fisher’s Exact Test for calculating
relative risks (RR) and p-values.
121 patients with NFA were included (71% male and 29% female). Mean age at
diagnosis was 55.2G14.7 years. 74% of male and 25% of female patients had
secondary hypogonadism at follow up, 57% (20) of female were menopausal prior
to surgery. DEXA was performed in 68% (nZ82) of all patients. Overall, DEXA
showed a normal bone density (T-score SK1) in 26%, in 30% signs of
osteopenia (T-score between K1 and K2.5) and in 12% signs of osteoporosis (Tscore %K2.5). The relative risk (RR) for osteopenia/osteoporosis in all patients
with secondary hypogonadism at follow up compared to patients with normal
gonadale function at follow up was 0.84 (95% CI 0.61–1.16; PZ0.36) [men: 1.19
(0.59–2.40; 0.74), women: 1.50 (0.67–3.34;PZ0.37)]. The RR for osteopenia/osteoporosis in female patients with hypogonadism (incl. menopausal
females) compared to men with hypogonadism at follow up was 1.57 (95% CI
1.16–2.14; PZ0.013).
(1) Osteopenia and Osteoporosis is a common problem in patients with NFA. (2)
A diminished bone density is not only related to impaired gonadale axis in
patients with NFA. (3) The influence of gender on bone density appears to be
Echo-enhanced ultrasound has a higher sensitivity than high-resolution
CT in the detection of hepatic metastasis of adrenocortical carcinoma
Jürgen Bauditz1, Wolfram Wermke1, Dirk Beyersdorff2, Herbert Lochs1,
Christian J. Strasburger1 & Marcus Quinkler1
Medicine, Center for Gastroenterology, Hepatology and Endocrinology,
Charite Campus Mitte, Charite Universitaetsmedizin Berlin, Berlin,
Germany, 2Institute for Radiology, Charite Campus Mitte, Charite
Universitaetsmedizin Berlin, Berlin, Germany.
Adrenocortical carcinoma (ACC) is a rare and heterogeneous malignancy with
incompletely understood pathogenesis and poor prognosis. Computerized
tomography (CT) and magnetic resonance imaging (MRI) are routinely
performed for imaging of the adrenal mass and for standard staging of chest
and abdomen as lung and liver are the primary organs for metastatic spread in
ACC. Contrast ultrasound is a non-invasive procedure which has been shown to
have a high sensitivity and specifity for differentiation of hepatic and
neuroendocrine tumours.
patients (7 women, 5 men; aged 24 to 77 years) with ACC were treated in our
centre from 2004 to 2006. Patients received staging with HR-CT as well as with
contrast ultrasound (Sonovue/Bracco, Acuson Sequoia/Siemens, CPS) of the
Contrast ultrasound demonstrated liver metastases in 8 of 12 patients (67%),
HR-CT showed liver metastases in 6 of 12 patients (50%). In 2 of 8 patients
(25%) HR-CT missed detection of liver metastases. Even retrospectively and
with knowledge of the ultrasound results, the hepatic lesions were not
recognized by HR-CT, but were detectable by HR-CT at a later time point. All
hepatic lesions diagnosed by HR-CT were also seen by ultrasound. The
detection of liver metastases by ultrasound resulted in a change of therapy in
the 2 patients.
Contrast ultrasound has a higher sensitivity than HR-CT in detecting highly
vascularized liver metastases of ACC and should be included in the staging
algorithm of ACC.
Characteristics of metabolic syndrome in patients with adrenal
Miomira Ivovic, Svetlana Vujovic, Milos Stojanovic, Milina Tancic-Gajic,
Ljiljana Marina, Marija Barac & Milka Drezgic
Institute of Endocrinology, Belgrade, Serbia.
Several studies show that characteristics of metabolic syndrome are often seen in
patients with adrenal incidentaloma. The aim of our study was to evaluate
metabolic factors in these patients. 208 patients (148 female and 60 male, age
55.08G11.02 y’s and BMI 27.91G4.6 kg/m2) were admitted and biochemical,
endocrine testing were performed. Lipid status: cholesterol 5.77G1.26 mmol/L,
triglyceride 1.92G0.98 mmol/L. 113(55%) patients were hypertensive (mean
systolic pressure was 150.3G30.12 mmHg, diastolic 92.93G16.48 mmHg). 34
(16.35%) patients had type 2 diabetes. According to OGTT (performed in 131
patients) more than 50% were diabetic or showed glucose intolerance. Insulin
sensitivity was calculated by HOMA, QUIQI formula and 56,86% of patients had
insulin resistance. After endocrine evaluation we divided them in two groups: first
with subclinical hypercorticism and second without hypercorticism. First group:
46 patients (38 woman and 8 man mean age 56.6G9.25 y’s and BMI 27.83G
4.37 kg/m2). Second group: 162 patients (110 women and 52 men, age 54.66G
11.45 years and BMI 27.93G4.67 kg/m2). No statistically significant difference
was found for cholesterol (5.68G1.24 vs. 6.09G1.29 mmol/L; PO 0.05) and
triglyceride (1.88G0.9 vs. 2.08G1.22 mmol/L; PO0.05) between these
subgroups. We also find no statistically significant difference in insulin resistance
between groups (QUIQI: 0.34G0.05 vs. 0.33G0.03; PO 0.05). Mean systolic
and diastolic blood pressure was not significantly higher in subgroup with
sublinical hypercorticism (149.6G29.92 vs. 152.7G31.02 mmHg; pO 0.05 and
92.38G16.42 vs. 94.89G16.74 mmHg; PO0.05).
Significant number of patients with adrenal incidentaloma had characteristics
of metabolic syndrome even without proved endocrine hypersecretion. These
patients are at high risk for cardiovascular events. Well-defined international
study protocols should include screening for metabolic syndrome.
The role of radio-guided surgery (RGS) with the use of 99mTc-EDDA/HYNIC-octreotate in detection of unknown primary and secondary
sites of neuroendocrine tumours of the gastrointestinal tract (GEPNET) and improving the final outcome of patients
Alicja Hubalewska-Dydejczyk1, Jan Kulig2, Piotr Szybinski2,
Renata Mikolajczak3, Anna Sowa-Staszczak1, Katarzyna Fröss-Baron1 &
Bohdan Huszno1
Department of Endocrinology, Medical College at Jagiellonian University,
Cracow, Poland, 2Gastrointestinal and General Surgery Department,
Medical College at Jagiellonian University, Cracow, Poland, 3Radioisotope
Centre POLATOM, Otwock-Swierk, Poland.
Despite a wide spectrum of imaging diagnostics, GEP-NETs often stay
undetectable until the time of dissemination. Removing of a primary tumour
together with disseminated lymph nodes even with the presence of liver
metastases is the most appropriate treatment to delay progression of the disease.
SRS followed by RGS gives a possibility to detect occult GEP-NET intraopratively. 99mTc-HYNIC/EDDA-octreotate, a somatostatin analogue with high
affinity to sst2 was applied in the study. The aim of the study was to determine
whether intra-operative radio-detection with the use of 99mTc-EDDA/HYNICoctreotate, is able to reveal unknown primary tu and metastases of GEP-NET
thereby improving surgical treatment and final prognosis.
Materials and methods
There were ten patients under examination with GEP-NET (with positive SRS
and negative different pre-operative imaging tests). Insulinoma was suspected in 5
pts, non-functioning pancreatic NET - 1, and carcinoid in 5 cases. At surgery,
suspected lesions were measured in vivo and ex vivo (Navigator-GPS) and the
exact exploration of the abdominal cavity was performed.
Amongst patients with pancreatic NET, 99mTc-EDDA/HYNIC-octreotate SRS
followed by RGS detected 4 insulinomas, 1 glucagonoma and in one patient false
Endocrine Abstracts (2007) Vol 14
9th European Congress of Endocrinology, Budapest, Hungary, 2007
positive result appeared to be a cyst but nesidoblastosis was finally recognised. Three
carcinoids with metastases were detected; in two cases the use of hand-held gamma
probe extended the surgical procedure resulting in the successful excision of the
metastatic lymph nodes. In one case the liver metastases were confirmed previously
revealed by SRS only. Another false positive result was caused by ileitis.
In our study 99mTc-EDDA/HYNIC-octreotate SRS followed by RGS localized all
primary GEP-NETs undetected with other imaging diagnostics. The main
advantage of RGS in comparison to SRS is high sensitivity in detection of
metastatic lymph nodes. The imaging properties of the 99mTc-EDDA/HYNICoctreotate creates abilities for more common application of this tracer followed by
RGS in oncology.
Ascl1 is abundantly expressed in endocrine pancreatic tumors
Téresè Johansson1, Margareta Halin Lejonklou1, Sara Ekeblad1,
Peter Stålberg2 & Britt Skogseid1
Institution of Medical Sciences, Uppsala, Sweden, 2Institution os Surgical
Sciences, Uppsala, Sweden.
Apart from inactivation of the MEN1 gene, molecular events essential for
tumorigenesis of the endocrine pancreas are poorly characterized. A potentially
useful approach for understanding tumor progression is to study transcription
factors operating in fetal pancreatic development. The Notch signaling cascade
with expression of the transcription factors Hes1, Hey1, and Ascl1 plays a vital
role in sustaining the balance between cell proliferation, differentiation and
apoptosis during the pancreatic development. They may play a similar role in the
development of endocrine pancreatic tumors (EPT).
To study the expression of Notch1, Hes1, Hey1 and Ascl1 in EPT, by quantitative
PCR (qPCR) and Immunohistochemistry (IHC)
Material and methods
Notch1, Hes1, Hey1, and Ascl1 mRNA and protein expression were investigated
in 26 EPT (ten were MEN1 associated). Immunohistochemistry was also
performed on 11 normal pancreatic tissues adjacent to the tumor (five MEN1 and
six sporadic). The immunoreactivity was graded (negative, weak, moderate or
strong), and sublocalization of expression as nuclear and/or cytoplasmatic was
The statistical analysis of the qPCR data revealed a correlation between the
Notch1-Hes1 expressions in EPT. All tumors displayed Ascl1 immunoreactivity,
which was graded as strong in 85%. Hes1 expression in EPT was graded as
invariably weak, or completely absent (30%). In normal islets a weak nuclear
Hes1 staining was observed. Hey1 and Notch1 were expressed in the cytoplasm
and nucleus of tumor cells and normal endocrine tissue.
Ascl1 is invariably and abundantly expressed in EPT. Hes1 is either lacking or
weakly expressed and confined to the cytoplasm of EPT. The lack of Hes1 in
tumor cell nuclei could contribute to the prominent Ascl1 expression in EPT.
These results show that Notch1, Hes1, Hey1 and Ascl1 are variable expressed in
EPT and normal pancreatic tissues; and that they may be involved in endocrine
pancreatic tumorigenesis.
Histopathological and molecular studies in patients with goiter and
hypercalcitoninemia: reactive or neoplastic C-cell hyperplasia?
Uberta Verga1, Stefano Ferrero3, Leonardo Vicentini2, Tatiana Brambilla3,
Valentina Cirello1, Marina Muzza1, Paolo Beck-Peccoz1 &
Laura Fugazzola1
Endocrine Unit, Dept. of Medical Sciences, University of Milan and
Fondazione Policlinico IRCCS, Milan, Italy, 2Endocrine Surgery Unit,
Fondazione Policlinico IRCCS, Milan, Italy, 3Pathology Unit, Dept. of
Medicine, Surgery and Dentistry, University of Milan, Ospedale S. Paolo,
Milan, Italy.
The cut-off values able to differentiate between reactive or neoplastic C cell
hyperplasia (CCH) or to predict sporadic medullary thyroid cancer (MTC) are still
debated both for basal and stimulated calcitonin (bCT and sCT). Aim of the present
study was to define the prevalence and the histological patterns of CCH in 15
patients with multinodular goiter (MNG), bCTO10 pg/ml and sCT levels O
Endocrine Abstracts (2007) Vol 14
50 pg/ml. These data were compared with those from 16 patients with MNG and
bCT levels !10 pg/ml, and with those from 4 patients with familial medullary
thyroid cancer (FMTC). For each case, 6 paraffin blocks were selected, CT
immunoreactive cells were counted in sixty consecutive high power fields (400x)
and classified as focal, diffuse, nodular or neoplastic. RET genetic analyses were
performed at the germline and tissue level in MTC and, for the first time, in CCH
cases. In patients with MNG, sCT levels O50 pg/ml were associated with CCH or
with MTC, being the total number of C cells/60 fields significantly higher than that
found in MNG with normal bCT (PZ0.0008), and comparable to that detected in
FMTCs. Interestingly, in the group with sCTO50 pg/ml, the C cells displayed a
neoplastic phenotype, concerning morphology, distribution and localization. No
RET mutations were found neither at the germline nor at the somatic level.
In conclusion, sCT levels O50 pg/ml were associated with CCH in all cases and
with MTC in 4 patients, without correlation between CT levels and the number of C
cells or the final diagnosis. After serial blocking and high power field
magnification, an elevated number of C cells were counted, often showing a
morphology and a distribution pattern consistent with neoplastic CCH, thus
strengthening the hypothesis that CCH might be the precursor also of sporadic
MTC in the absence of RET mutations. Hence, sCT levels O50 pg/ml indicate the
presence of CCH with a possible preneoplastic potential, suggesting the
opportunity to perform a “prophylactic” surgical treatment.
Thyroid cancer and pregnancy: clinical outcome and time of diagnosis
in a series of 94 women
Perrino Michela1, Vannucchi Guia1, Vicentini Leonardo2,
Deborah Mannavola1, Paolo Beck-Peccoz1 & Laura Fugazzola1
Endocrine Unit, Dept. of Medical Sciences, University of Milan and
Fondazione Policlinico IRCCS, Milan, Italy, 2Endocrine Surgery Unit,
Fondazione Policlinico IRCCS, Milan, Italy.
Thyroid cancer represents the second more frequent tumor among those
diagnosed during pregnancy. Indeed, during pregnancy thyroid volume increases
by 20–30% and new nodules can appear, due to the effect of choriogonadotropin
which stimulates thyroid growth. Hence, it has been proposed that thyroid
cancer diagnosed during pregnancy could harbour a poorer prognosis. Aim of
the present study was to compare the clinical outcome in the following 3 groups
of patients affected with thyroid cancer: group 1 (Gr.1): 12 women with tumor
diagnosed during pregnancy and submitted to thyroidectomy during the second
trimester or in the first year after delivery; group 2 (Gr.2): 33 women with
diagnosis of tumor at least 1 year after the delivery; group 3 (Gr.3): 49 women
with diagnosis and treatment of the tumor before pregnancy or nulliparous. The
3 groups were matched for age, treatment, histology and follow-up. In particular,
all patients of group 1 were treated with total thyroidectomy and radiometabolic
treatment. Remission or persistence of disease were defined on the bases of basal
thyroglobulin (Tg) levels before and after rhTSH, in the absence of anti-Tg
antibodies, and of Total Body Scan. No significant differences in tumor size,
capsular invasion and local/distant metastases were observed between the 3
groups. As far as the outcome is concerned, patients with the tumor diagnosed
during pregnancy showed more frequently persistence or relapse of the disease
with respect to the patients of the other groups (Gr. 1 vs Gr. 2: PZ0.0035; Gr.1
vs Gr. 3: PZ0.0057; Gr1 vs Gr. 2C3, PZ0.018; Gr.2 vs Gr.3: PZNS). In
particular, 9/12 patients of Group1 showed persistence of disease, with lymphnode metastases in 2 cases, distant metastases in 2 cases and elevated Tg levels
in 5 cases.
In conclusion, the present data show that thyroid cancer diagnosed during
pregnancy is associated with a poorer prognosis with respect to tumors
developed in a non gravidic period, thus suggesting the need for an aggressive
treatment by thyroidectomy during the second trimester and radiometabolic
therapy soon after delivery.
RET genotypes comprising specific haplotypes of polymorphic variants
are associated with sporadic medullary thyroid cancer
Laura Fugazzola1, Marina Muzza1, Caterina Mian3, Daniela Cordella2,
Susi Barollo3, Valentina Cirello1, Maria Elisa Girelli3, Giuseppe Opocher3,
Paolo Beck-Peccoz1 & Luca Persani2
Endocrine Unit, Dept. of Medical Sciences, University of Milan and
Fondazione Policlinico IRCCS, Milan, Italy, 2Dept. of Medical Sciences,
University of Milan and Istituto Auxologico Italiano IRCCS, Milan, Italy,
Endocrinology Unit, Dept. of Medical and Surgical Sciences, University of
Padova, Padova, Italy.
9th European Congress of Endocrinology, Budapest, Hungary, 2007
Many single nucleotide polymorphisms (SNPs) of the RET gene have been described
both in the general population and in patients with sporadic medullary thyroid cancer
(sMTC), MEN2 or Hirschsprung disease. Some association studies reported a higher
prevalence of these variants in the affected patients, suggesting a possible role in
modifying the risk of occurrence of the disease. However, data from different cohorts
of sMTC are discrepant and the aim of the present study was to determine if a variant
per se or a combination of variants predispose to sMTC. Thus, a possible association
of RET haplotype(s) and disease was looked for in 82 patients affected with sMTC
and 49 age matched controls. Six RET SNPs were studied by PCR and direct
sequencing. The most frequent SNPs were those in intron 1 (30 and 32% in sMTC
and controls, respectively), exon 2 (22 and 24%) and exon 13 (24 and 26%). No
significant differences were observed in the prevalence of single SNPs between
patients and controls, including G691S, which is the only non-synonymous variant.
Accordingly, functional analyses did not reveal an increased autophosphorylation for
G691S. Twelve unique haplotypes, labelled A-N, were obtained. The distribution of
haplotypes between cases and controls were significantly different (P!0.05). The
study of the association of these different haplotypes in cases and controls lead to the
identification of 30 different genotypes. Inspection of the genotypes in the two groups
showed that the genotype distribution between cases and controls was different (P!
0.05). In particular, there were 7 genotypes unique to controls, 13 unique to sMTC
and 11 shared by the 2 groups. For example, AA, AC, AD and AH, all of which
containing one allele without polymorphisms, are prominently or uniquely
represented in sMTC. These data suggest that genotypes comprising specific pairs
of RET haplotypes are associated with predisposition to sMTC. In this series, the
absence on both alleles of the 6 SNPs analyzed was recorded only for MTC cases,
indicating that the presence of RET variants could be protective against cancer
Isolation of the Side population (SP) from murine adrenal glands
renders cells with adrenocortical stem cell properties
Urs Lichtenauer1, Igor Shapiro1, Klaus Geiger2, Anne-Marie Pulichino3,
Jaques Drouin3 & Felix Beuschlein1
Institute of Molecular Medicine and Cell Research, Albert-LudwigsUniversity Freiburg, Freiburg, Germany, 2Department of Internal Medicine
I, Albert-Ludwigs-University Freiburg, Freiburg, Germany, 3Laboratoire de
Genetique Moleculaire, Institut de Recherches Cliniques de Montreal,
Montral, Canada.
Radioactive and transgenic tracing experiments indicate that in the adult adrenal stem
cells persist in the periphery of the cortex, which migrate centripetally and populate the
inner cortical zones upon differentiation. However, investigation of these cells has
been hampered by the lack of known marker genes. Vital Hoechst dye exclusion has
been described as a method for isolating a side population (SP) from mouse bone
marrow, which was enriched with stem cells. Utilizing this technique, we demonstrate
the presence of SP cells in a variety of adrenal derived cell populations including
normal mouse (0.71–0.83%) and human (0.01%) adrenals. After FACS sorting,
isolation of SP and non SP (NSP) cells from murine adrenal glands revealed selfrenewal and long-term culture capacities only for the SP fraction, which grew in a
fibroblast-like manner, whereas the NSP cells did not proliferate. In addition, adrenal
SP cells expressed adrenocortical markers such as MC2 receptor, StAR, and P450scc
by means of RT-PCR and IHC. Interestingly, in a mouse model of ACTH deficiency
(Tpit knock out animals, TpitK/K), the proportion of SP cells was significant higher
in comparison to heterozygous animals (TpitK/K 0.45G0.16% vs. TpitC/K 0.13G
0.04%;P!0.004). This higher SP cell proportion was associated with an increased
width of the subcapsular cell compartment (TpitK/K 100G12.3% vs. TpitC/K
259G10.7%; P!0.0001), which was characterized by the lack of expression of
steroidogenic enzymes such as 3ßHSD. Short term ACTH treatment of TpitK/K
animals resulted in a decrease of SP proportion (0.09%) and a shrinkage of the subcapsular zone similar to that of untreated TpitC/K controls (130G10.2%;PZ0.33).
In summary, the adrenal Side Population displays certain stem cell properties.
Moreover, we present indirect evidence that ACTH might be required for
adrenocortical stem cell differentiation thus affecting adrenal zonation in vivo. Current
studies including in vitro stimulation and in vivo transplantation experiments aim at the
further characterization of this cell population.
Selective intra-arterial calcium stimulation with hepatic venous
sampling in investigation of hyperinsulinemic hypoglycemia
Mohd Shazli Yusof, Tomas Ahern, Thomas P Smith & Donal O’Shea
Department of Endocrinology and Diabetes Mellitus, Elm Park, Dublin 4,
A retrospective analysis of the results of all intra-arterial calcium stimulations
performed at St. Vincent’s Hospital, Dublin, in the years 2001-2006. All patients
with symptoms suggestive of hypoglycemia had 72 hour fasting test with
evidence of inappropriately elevated insulin and c-peptide at the time of
hypoglycemia. These patients were investigated further with pancreatic imaging
and selective intra-arterial calcium stimulation with hepatic venous sampling
(ASVS). Analysis of the results was performed using the Wilcoxon signed rank
test. Results were available in 9 patients. The overall catherisation success rate
was: minimum four arteries in 7/9, three arteries 1/9 and two arteries in 1/9. CT
was positive in 2/7 patients, MRI 0/2, octreotide scan 0/2 and endoscopic
ultrasound 0/2. Mean insulin increment was 11.91 fold (95% CI 6.51–17.30) in
tumour area versus 1.61 fold (95% CI 1.21–2.01) PZ0.002. ASVS was positive
in 8 patients. 7 patients were found to have insulinoma and 2 patients were
diagnosed with adult nesidioblastosis by means of histological diagnosis. One of
nesidioblastosis patient had negative calcium stimulation test but had diffuse
hyperinsulinemic picture on ASVS. Our results suggest that selective intraarterial calcium stimulation with hepatic venous sampling remains a powerful
tool for diagnosis of insulinoma. CT pancreas alone combined with ASVS should
be the standard of investigation in biochemically proven insulinoma. Three fold
insulin levels increment should be used as the cut-off point for positive test after
calcium stimulation. We reported a case of failure ASVS. ASVS use should be
restricted to units with expertise in this area.
Somatostatin and dopamine receptor regulation and effects of a new
somatostatin/dopamine chimeric compound on cell proliferation of the
human androgen-dependent prostate cancer cell line LNCaP
Marica Arvigo1, Massimiliano Ruscica2, Elena Dozio2, Michael D Culler3,
Francesco Minuto1, Marcella Motta2, Paolo Magni2 & Diego Ferone1
Department of Endocrinological & Metabolic Sciences and Center of
Excellence for Biomedical Research, Genoa, Italy, 2Center for Endocrinological Oncology, Istituto di Endocrinologia,, Milan, Italy, 3Biomeasure
Incorporate/IPSEN, Milford, United States.
The increasing use of somatostatin (SRIF) analogues prompted extensive
investigations on SRIF receptor (SSR) in human tumours. Human prostate
cancer (PCa) may differentially express SSRs from the normal tissue. Moreover,
SSR and dopamine (D) receptors (DR) may interact to form homo- and
heterodimers with enhanced functional activity. In the present study, using the
human androgen-dependent PCa cell line LNCaP, we investigated: 1) SSR and
DR subtype expression in different culture conditions (10% and 2% FBS); 2) the
effects of SRIF and of a new SRIF/D chimeric molecules, BIM-23A760, able to
bind with high affinity both sst2A and D2R on cell proliferation. LNCaP expressed
sst1, sst2A, sst3, sst5, and D1R and D2R subtypes at gene (RT-PCR) and protein
(Western blot) level. SSRs and D2R expression was differentially regulated by the
culture conditions: sst2A, sst5 and D2R expression was not modified by serum
concentration, whereas sst1 and sst3 were inversely correlated to serum
concentration. Dose-response studies were performed at 24 and 48 h with a
dose range from 10K11 to 10K7 M. SRIF inhibited cell proliferation
([3H]thymidine incorporation) after 24 and 48 h at all doses. The clinically
available analogue lanreotide inhibited cell proliferation after 24 and 48 h with a
maximum effect at 10K11 M. However, the chimeric BIM-23A760 resulted more
potent than lanreotide and significantly inhibited cell proliferation after 24 h at
10K9 M and after 48 h in a dose range from 10K7 to 10K11 M. These data indicate
a heterogeneous expression of SSRs and DRs in PCa, depending on the culture
conditions and show an enhanced potency of the chimeric BIM-23A760 in
inhibiting cell proliferation, suggesting an important role of the dopaminergic
pathway in PCa. Hence, LNCaP provides a model to study the interaction
between membrane receptors and to further investigate chimeric SRIF/D
compounds in human cancer.
Somatostatin receptor regulation and effects of somatostatin and
somatostatin analogues on cell proliferation of the human androgendependent prostate cancer cell line LNCaP
Massimiliano Ruscica1, Marica Arvigo2, Elena Dozio1, Michael D Culler3,
Francesco Minuto2, Marcella Motta1, Diego Ferone2 & Paolo Magni1
Center for Endocrinological Oncology, Istituto di Endocrinologia,
Università degli Studi di Milano, Milan, Italy, 2Department of Endocrinological & Metabolic Sciences and Center of Excellence for Biomedical
Research, University of Genoa, Genoa, Italy, 3Biomeasure Incorporate/IPSEN, Milford, Massachusetts, United States.
Endocrine Abstracts (2007) Vol 14
9th European Congress of Endocrinology, Budapest, Hungary, 2007
Somatostatin (SRIF) has been demonstrated to inhibit in vitro proliferation of normal
and transformed cells via SRIF receptors (SSRs). Moreover, like other
neuroendocrine molecules, SRIF and SSRs may play a significant role in the
progression and neuroendocrine differentiation of human prostate cancer (PCa).
However, conflicting results have been reported in the literature on SSR
heterogeneity and specific cell localization in PCa. In the present study, using the
human androgen-dependent PCa cell line LNCaP, we investigated: 1) SSR subtypes
expression in different culture conditions (10% and 2% FBS); 2) the effects of SRIF
and of new agonists on cell proliferation. LNCaP expressed sst1, sst2A, sst3, sst5, at
gene (RT-PCR) and protein (Western blot) level. SSR level of expression was
differentially regulated by the culture conditions: sst2A and sst5 expression was not
modified by serum concentration, whereas sst1 and sst3 expression was inversely
correlated to serum concentration. Dose-response studies were performed at 24 and
48 h with a dose range from 10K11 to 10K7 M. SRIF inhibited cell proliferation
([3H]thymidine incorporation) after 24 and 48 h at all doses. The sst1 (BIM-23926),
sst2 (BIM-23120) and sst5 (BIM-23206) preferential compounds did not affected cell
proliferation. Conversely, lanreotide, inhibited cell proliferation after both 24 and
48 h with a maximum effect at 10K11 M, whereas, the bispecific sst2/sst5-preferential
ligand BIM-23244 inhibited cell proliferation after 24 h at the dose of 10K9 M. The
bi-specific sst1/sst2-preferential ligand BIM-23704 inhibited LNCaP proliferation
after 48 h treatment, (dose range 10K10 M to 10K11 M). SSR subtype expression in
PCa can be actively regulated by culture conditions, suggesting that receptor profile
in PCa may depend from the tumor microenvironment. Finally, LNCaP represents a
useful model for studying SSR regulation in PCa, intracellular subtype-linked
signalling, and validate new analogues with different receptor affinities in PCa
Germline mutations in the RET gene cause MEN2, an inherited cancer syndrome
associated with medullary thyroid carcinoma (MTC). We performed genetic
analysis on DNA from whole blood of a 58 yr old female affected by a multifocal
MTC. Exons 10, 11, 13, 15 and 16 of RET gene were amplified by PCR using
specific primers and characterised by direct automatic sequencing. Here, we
report a new RET point mutation: a heterozigous missense mutation Y606C, a G
to A nucleotide substitution leading to a Tyrosine (Y) to Cysteine (C) amino acid
change in exon 10. We approached the functional effects of such a mutation in an
in vitro system by cloning the wild-type RET, the Y606C mutation as well as the
C620Y mutation, previously described as less strong RET oncogene associated
with MTC, in an expression vector and transiently transfecting NIH3T3
fibroblasts. All mutations were obtained by site-directed mutagenesis. We first
demonstrated by western blot analysis using a specific antibody an increased
tyrosine phosphorylation in the Y905 residue in the RET/Y606C, corresponding
to receptor activation. Since RET activation results in an intracellular signalling
cascade leading to extracellular signal regulated kinases (ERKs), we investigated
ERK activity in our transfected cells. Results demonstrate a significant increase in
ERK2 phosphorylation/activation in the RET/Y606C versus the wild type and
RET/C620Y. We finally showed by gel electrophoresis of transfected cell lysates
in non reducing conditions that the introduction of a C due to the Y606C mutation
results in an increased dimerization of the receptor. All these findings suggest that
the Y606C mutation confers constitutive activation of RET signalling.
Conjugated and unconjugated serum steroid hormone concentrations
in relation to tumour receptor status in postmenopausal breast cancer
Borbála Vincze, Ferenc Pommersheim, Nora Udvarhelyi, Zsolt Horváth,
Bence Kapuvári, Mariann Boldizsár, István Köves, Zsolt Orosz &
István Láng
National Institute of Oncology, Budapest, Hungary.
Human breast cancer tissue is able to concentrate estrogens. 17-beta-estradiol (E2)
and estrone (E1) are produced locally through several mechanisms, e.g. from
conjugated and unconjugated steroid hormones uptaken from the circulation. This
study was aimed to investigate the correlation between endogenous serum sex steroid
concentrations and tumour receptor status in postmenopausal breast cancer patients
undergoing surgical intervention. The study involved 740 postmenopausal patients
with primary breast cancer of Stage I-II prior to surgical intervention. None of them
took hormone preparations and received chemo or radiotherapy. Serum levels of
sexual hormones and precursors, sex hormone-binding globulin (SHBG), insulinlike growth factor-1 (IGF-1) and IGF binding protein-3 (IGFBP-3) were measured by
fully automated equipment using RIA and IRMA methods. Estrogen (ER) and
progesterone receptors (PR), HER2/neu expression in tumour tissues were
determined using immunohistochemical methods (NCL-ER-6F, 11/2; NCL-LPgR-312; CB11-RTU, Novocastra; Hercep Test, DAKO). In the ICH 2C/3C cases
HER2/neu gene amplification was confirmed by fluorescence in-situ hybridization.
MedCalc Software was used for statistical analysis. Our investigation revealed
significant correlations among steroid receptor status of tumour tissue and the serum
E1 and androstenedione (AD) levels. Close relationship was observed among serum
value of E1-sulfate, IGF-1, testosterone (TE), dehydroepiandrosterone sulphate
(DHEA-S) and HER2/ER status of tumour tissue. Results demonstrate that the
positivity of tumour tissue receptor status can be predicted on the basis of increased
serum unconjugated (E1, DHEA, AD, TE) and conjugated (E1-S, DHEA-S) sexual
hormone concentrations. It is suggested that circulating E1-S and DHEA-S might
play a major role in the intratumoral estrogen synthesis. Our study supports the
hypothesis that the serum E1, AD, E1-S, DHEA-S, TE and IGF-1 levels might also be
useful for predicting the magnitude of response to postoperative chemotherapy.
This research was supported by the Hungarian Research Fund (OTKA No.T
A novel activating germline mutation in the RET gene (Y606C) in a
patient with medullary thyroid carcinoma
Michaela Luconi, Tonino Ercolino, Adriana Lombardi, Lucia Becherini,
Elisabetta Piscitelli, Maria Sole Gaglianò, Mario Serio & Massimo Mannelli
University of Florence, Dept. Clinical Physiopathology, Florence, Italy.
Endocrine Abstracts (2007) Vol 14
Novel germline VHL mutations associated to uncommon clinical
Tonino Ercolino1, Lucia Becherini1, Lisa Simi1, Maria Sole Gaglianò1,
Gabriella Nesi2, Andrea Valeri3 & Massimo Mannelli1
University of Florence, Dept. Clinical Physiopathology, Florence, Italy,
University of Florence, Dept. Human Pathology, Florence, Italy, 3AOUC,
General and Vascular Surgical Unit, Florence, Italy.
The von Hippel-Lindau (VHL) syndrome is an inherited multi-tumor disorder
characterized by clinical heterogeneity and high penetrance. Pheochromocytoma
(Pheo) is present in 10-15% of cases. It can be isolated or associated with other
lesions such as hemangioblastomas, kidney cysts or cancer, and pancreatic
lesions. Pheos secrete norepinephrine and are generally located in the adrenals.
While performing genetic testing in patients affected by apparently sporadic
pheos or PGLs, we found two novel different VHL germline mutations in two
patients presenting two uncommon clinical pictures (an adrenal incidentaloma
and a neck tumor, respectively).
Coding regions and exon-intron boundaries of RET (exons 10, 11, 13, 14, 15),
VHL, SDHD, SDHB and SDHC genes were amplified and sequenced. We
identified two novel point mutations: a L198V missense mutation in a 32 yr old
female affected by a right adrenal compound and mixed tumor constituted by an
epinephrine secreting Pheo, a ganglioneuroma and an adrenocortical adenoma
and a T152I missense mutation in a 24 yr old female affected by a left carotid
body tumor. An extensive clinical, laboratory and radiological examination of the
patients and the mutated relatives did not show any other lesion.
We also analyzed the three-dimensional structure of the wild-type and the
mutated VHL protein showing that the mutations are located in functionally
relevant sites.
These cases enlarge the list of VHL mutations and add new insights in the
clinical variability of VHL disease, thus confirming the importance of genetic
testing in patients affected by apparently sporadic Pheos or PGLs.
The expression of alternatively spliced forms of type 1 deiodinase is
changed in clear cell renal cell carcinoma
Agnieszka Piekielko-Witkowska1, Adam Master1, Tanski Zbigniew2 &
Nauman Alicja1
Medical Center of Postgraduate Education, Warsaw, Poland, 2Specialistic
Hospital, Ostroleka, Poland.
Type 1 deiodinase (D1) catalyses deiodination of tyroxine (T4), which leads
either to synthesis of triiodothyronine or reverse triiodothyronine (rT3). T3 can
influence the process of neoplasia through its receptors which act as transcription
factors and regulate the expression of many tumor suppressor genes and
oncogenes. The aim of the study was to analyze the changes in expression of
alternatively spliced variants of D1 mRNA in clear cell Renal Cell Carcinoma
(ccRCC), which is the most common type of renal cancers (75% of primary renal
9th European Congress of Endocrinology, Budapest, Hungary, 2007
malignancies). Tissue samples were obtained with the permission of the local
Ethical Committee of Human Studies. Using quantitive real-time PCR we have
analyzed: 33 samples of ccRCC with their controls (the contralateral pole of the
same kidney not infiltrated by cancer, assigned C) as well as control samples from
patients suffering from other, nonneoplastic kidney abnormalities (6 samples,
assigned N). The expression of the whole pool of D1 transcript variants was
dramatically lowered in ccRCC tissues. The separately performed expression
analysis of alternatively spliced D1 transcript variants, which differ in the
presence or absence of subexon 1b, also exhibited about 90% decrease of mRNA
in both transcript variants of cancer tissues. Simultaneously, the comparison of
these alternatively spliced mRNA groups revealed that ratio: (whole pool of D1
transcripts)/(transcripts containing the1b exon) as well as relation: (whole pool of
D1 transcripts)/(transcripts devoid of the1b exon) were increased several times in
the ccRCC in comparison with controls. This observation suggests the existence
of at least one another alternatively spliced variant, which extends the whole poll
of D1 transcripts and possibly is overexpressed in ccRCC. Our results indicated
that the alternative splicing process of deiodinase type I can be disturbed in
tissues and 9 wash-out material from fine-needle aspiration biopsies (FNAB) after
signing informed consent approved by ethical committee. For assessment of
influence of Chernobyl nuclear accident we devided samples into 5 periods - one
period before and four periods after the accident. DNAs from paraffin-embedded
samples were extracted using the QIAamp DNA Blood Mini Kit and frozen
samples using Trizol reagent. BRAF gene was screened using the single strand
conformation polymorphism method (SSCP) and verified by direct sequencing.
The V600E mutation was detected in 56 samples (38,6%). All BRAF mutations
except one were heterozygous. Surprisingly, in the period before Chernobyl
nuclear accident no BRAF mutation was found, in other periods 56 mutations
were detected (41,2%). The female to male ratio was 3,7:1, mutation was found in
48,4% of male and in 36% of female patients. In our series difference between age
at diagnosis in patients with and without mutation was not significant. Our study
confirms a high rate of BRAF V600E mutation in Czech PTC patients. Results
indicate that the mutation is the most frequent genetic alteration found in PTC and
it could be used as a reliable genetic marker of PTC and applied for FNAB before
This study was supported by IGA MZ CR NR/7806-3.
Ret expression reduces estrogen-induced lactotrope hyperplasia
Carmen Cañibano, Noela Rodrı́guez, Sulay Tovar, Marı́a Jesús Vázquez,
Montserrat Lavandeira, Carlos Dı́eguez & Clara Álvarez
Department of Physiology, School of Medicine, University of Santiago de
Compostela, santiago de Compostela, Spain.
Effect of surgery on carotid vascular remodeling in patients with
Giampaolo Bernini, Fabio Galetta, Michele Bardini, Ferdinando Franzoni,
Chiara Taurino, Angelica Moretti, Matteo Bernini & Antonio Salvetti
Department of Internal Medicine, Universiyt of Pisa, Pisa, Italy.
RET is a tyrosine kinase receptor activated by GDNF, NTN, ART and PSPN
through GFRa1,2, 3 and 4 respectively. Activation of the receptor elicits
intracellular pathways such us Ras/MAPK and PI3K/AKT leading to
differentiation and proliferation. Our group has previously shown that RET is
expressed specifically in the somatotroph cell population within the pituitary
gland, both in rats and in humans. We have also shown that, in absence of its
ligand GDNF, RET induces activation of caspase 3 PKCd/JNK/c/EBPa and
CREB, causing apoptosis in cell cultures. Cell death is dependent on Pit-1 and p53
induction. This findings confirm previous hypothesis and strongly indicate that
RET acts as a dependence receptor. Now we provide evidence that the same
biological and biochemical mechanisms work in vivo.
For doing so, we have used a model of lactotroph hyperplasia induced by
estrogen administration in rat. Hyperplasic pituitary glands were infected with
purified high-titer retroviruses encoding RET or the corresponding empty virus as
control. Viral delivery was achieved by estereotaxia, injecting the retrovirus
directly into the pituitary of living anesthetized rats. Following treatment and
infection rats were sacrificed and pituitary weights recorded. As expected,
estrogen treatment induced a marked increase in pituitary size. Interestingly,
viral-mediated RET expression caused a significant reduction compared to mockinfected pituitaries (26.6C/K 1.8 mg vs 18.0C/K 1.0 mg), restoring pituitary
weight to values similar to pituitaries not treated with estrogens. We were able to
detect RET expression in lactotrophs, suggesting that ectopic expression of the
dependence receptor caused lactotroph cell death and hyperplasia reversal.
Moreover, we show activation of the caspase 3-PKCd-JNK-c/EBPa-CREB
apoptotic pathway, indicating that the same molecular events are elicited by RET
in cell culture models and in vivo.
In vitro and in vivo studies suggest that catecholamines, in addition to their
hemodynamic effect, exert a direct influence on the vascular wall, leading to
eutrophic and hypertrophic remodeling. This finding is in agreement with that
recently reported by our group on patients with pheochromocytoma (PHEO)
who show carotid intima media thickness (IMT) and vascular fibrosis higher
than essential hypertensives matched for classic cardiovascular risk factors,
including blood pressure. To further confirm the direct vascular influence of
catecholamines in humans, we compared carotid IMT, by ultrasound imaging,
and vascular fibrosis, by imaging backscatter signal (IBS) analysis, in a group
of patients with PHEO and high-normal blood pressure (nZ10; meanGSD age
51G13.2 yr, range 28–70 yr) before and after surgical cure (meanGSD 20.5G
5.98 months, range 12–29 months). After removal of the tumor, no significant
variation in systolic (126.5G6.5 vs 138.3G5.6 mmHg, meanGSE) and diastolic
(83.6G3.1 vs 87.0G4.1 mmHg) blood pressure and in total cholesterol
(207.0G9.6 vs 198.8G12.6 mg/dl), HDL-cholesterol (62.8G4.5 vs 61.3G
4 mg/dl), and LDL-cholesterol (118.3G8.5 vs 117.9G13.1 mg/dl) was
observed, while a reduction in urinary metanephrines (normetanephrine:
480.0G51.2 vs 2264.8G681.4 mg/24 h, P!0.003; metanephrine: 178.7G23.5
vs 879.2G290.8 mg/24 h, P!0.03) and in catecholamines (plasma noradrenaline: 442.9G54.7 vs 623.9G115.0 pg/ml, N.S.; plasma adrenaline:
36.1G7.2 vs 183.8G99.3 pg/ml, P!0.02; urinary noradrenaline: 49.4G8 vs
86G27.4 mg/24 h, N.S.; urinary adrenaline:8.6G0.7 vs 18.0G7.7 mg/24 h, NS)
was shown. After surgery, IBS values significantly decreased (K22.82G0.40 vs
–21.17G0.61 dB, P!0.005) and a similar pattern was observed for carotid
IMT (0.86G0.06 vs 0.88G0.06 mm, P!0.06), though at not significant extent.
A direct and significant correlation was found between the absolute reduction in
IBS values and the absolute decrement in urinary normetanephrines levels (rZ
0.54, P!0.03). In conclusion, our results confirm that high catecholamine
levels directly affect the vascular wall structure, indipendently of the
hemodynamic discharge.
Analysis of BRAF point mutation in papillary thyroid carcinoma
Vlasta Sykorova1, Sarka Dvorakova1, Jan Laco2, Ales Ryska2,
Daniela Kodetova3, Jaromir Astl4, David Vesely4 & Bela Bendlova1
Institute of Endocrinology, Prague, Czech Republic, 2Fingerland’s Institute
of Pathology, Hradec Kralove, Czech Republic, 3Institute of Pathology and
Institute for Pathological Anatomy and Molecular Medicine FN Motol,
Prague, Czech Republic, 4Department of ENT and Head and Neck Surgery
FN Motol, Prague, Czech Republic.
BRAF point mutations are found in 29-69% of papillary thyroid carcinoma
(PTC). BRAF is a serine-threonine kinase involved in the phoshorylation of
MAPK signaling pathway. The mutation is located in the exon 15 of BRAF,
resulting in the substitution of valine to glutamate at codon 600 (V600E).
Mutation generates unregulated B-Raf activity that leads to increased cellular
proliferation. The aim of this study was to determine the frequency of BRAF
mutation in the Czech population and its changes in 1960-2006. We examined
145 of PTC: 92 paraffin-embedded formalin-fixed tissue samples, 44 fresh frozen
A case report of ectopic Cushing’s disease presented with
Demet Ozgil Yetkin1, Sayid S Zuhur1, Ekrem Kara1, Ayla Gurel Sayin2,
Buge Oz3 & Ertugrul Tasan1
Istanbul University Cerrahpasa Medical faculty Endocrinology and
Metabolism Department, Istanbul, Turkey, 2Istanbul University Cerrahpasa
Medical faculty Cardiovascular Surgery Department, Istanbul, Turkey,
Istanbul University Cerrahpasa Medical faculty Pathology Department,
Istanbul, Turkey.
To report a case of Cushing’s syndome caused by ectopic ACTH secretion related
to a thymic carcinoid presented with trombositopenia.
Endocrine Abstracts (2007) Vol 14
9th European Congress of Endocrinology, Budapest, Hungary, 2007
years old male presented with fatigue, skin rash. At presentation, physical findings
showed Cushingoid appearance, with moon face, hyperpigmentation, easy
bruising and buffalo hump. His laboratory findings showed platelet: 90.000
(150.000–450.000), ACTH: 609 pg/ml (0–46 pg/ml), baseline cortisol level
60.8 mgr/dl (6.2–19 mgr/dl), potassium: 2.4 mEq/l (3.5–5 mEq/l), midnight
cortisol level: 57.17 mgr/dl, urine cortisol level: O1000 mgr/24 hour. Serum
cortisol levels failed to supress after low and high dose dexamethasone (DST)
(1 mg: O60 mgr/dl, 8 mg: 42 mgr/dl), therefore confirming the diagnosis of
ectopic ACTH production. Laboratory evaluation for trombositopenia showed,
normal eritrocyte series, deficient trombocyte. PT, aPTT and FDP were normal,
fibrinojen: 606 mg/dl (!350). Megacaryocyte level was elevated and platelet
count was normal in bone marrow aspiration. His sella MRI was normal, thorax
CT showed 2!1.5 cm lesion at anterior mediastinum, and surrenal hyperplasia
on his abdomen CT. His octreoscan was normal. There was a hypermetabolic
focus in anterior mediastinum and bilaterally adrenal gland on his 5FDG PET/CT.
Under the diagnosis of ectopic ACTH production in anterior mediasten, he
underwent mediastinotomy and thymectomy. Pathological examination showed
ACTH, chromogranin and synaptophsin positive thymic benign carcinoid. After
the operation his cortisol levels returned to normal (corisol:11 mgr/dl, ACTH:
54 pg/ml) and low dose DST was 1.6 mgr/dl. Three weeks after the operation his
platelet count was 411.000, with exclusions of other causes of tromposytopenia
and reversal of platelet counts to normal after the operation we concluded that his
trombosytopenia was due to a paraneoplastic immune trombocytopenic purpura
Thymic ACTH secreting carcinoid tumors are rare phenomenon of ectopic
Cushing’s syndome. To our knowledge this is the first case of ectopic Cushing’s
disease with paraneoplastic ITP.
Influence of Lanreotide Autogel on insulin sensitivity among patients
with acromegaly
Melek Eda Ertorer1, Okan Bakiner1, Inan Anaforoglu1, Emre Bozkirli1,
Neslihan Bascil Tutuncu2 & Nilgun Guvener Demirag2
Baskent University Faculty of Medicine, Endocrinology and Metabolism,
Adana, Turkey, 2Baskent University Faculty of Medicine, Endocrinology
and Metabolism, Ankara, Turkey.
There are limited data inquiring the relationship between somatostatin
analogues and insulin sensitivity among acromegalic cases. This study was
conducted to evaluate short-term effects of lanreotide autogel (LA),
administered every 28 days by deep subcutaneous injection, on insulin
sensitivity among acromegalic patients with pituitary tumors. Before and
following six months of LA treatment, insulin resistance and beta-cell function
were calculated by using homeostasis model assessment of insulin resistance
(HOMA-IR) and beta-cell function (HOMA-beta) formula, and euglycemic
hyperinsulinemic clamp test was performed for evaluating the whole insulin
sensitivity. Naı̈ve acromegalic patients (Case 1, Case 3) and cases who
experienced any prior unsuccessful treatment modality and approved to
consume LA (Case 2, Case 4, Case 5) were included. The study was approved
by the local ethics committee. Euglycemic hyperinsulinemic clamp defined by
De Fronzo was used and insulin sensitivity was derived from glucose disposal
rate expressed as mg/kg/min and indicated as ‘M’ index. The characteristics of
the cases regarding serum growth hormone (GH) levels and insulin sensitivity
markers during follow-up are shown in Table. Although there were statistically
insignificant difference between baseline and final GH, HOMA-IR, HOMAbeta% and M values (PZ0.150, PZ0.447, PZ0.158, PZ0.151, respectively),
remarkable M value improvement was observed in Case 1, Case 2 and Case 3.
This finding might be explained by the prominent decrease in their GH levels
following LA treatment.
GH (ng/ml)*
HOMAIbeta (%)*
M value*
Case 1
Case 2
Case 3
Case 4
Case 5
2.32 / 2.25
95/ 58.48
2.31 / 0.41
289.15 / 83.63
4.29/ 5.59
152.25/ 98.06
3.23 / 2.59
76.87 /67.14
1.03 / 8.22
2.98 / 4.70
5.72 /5.53
*Baseline/ following 6 months of treatment.
Endocrine Abstracts (2007) Vol 14
5.09 / 13.09
A newly detected mutation of the RET proto-oncogene in exon 8 as a
cause of multiple endocrine neoplasia Type 2A
S. Bethanis1, Th. Palouka1, Ch. Avgoustis1, G. Koutsodontis2, T. Bei2,
D. Yannoukakos2 & S. Tsagarakis1
Department of Endocrinology, Athens’ Polyclinic, Athens, Greece,
BioGenomica, Centre for Genetic Research and Analysis, Athens, Greece.
Multiple endocrine neoplasia type2A (MEN 2A) is a syndrome of familial cancers
characterized by medullary thyroid carcinoma (MTC), pheochromocytoma and
hyperplasia of the parathyroid glands. RET protooncogene is the responsible gene for
MEN 2A; in more than 96% of MEN 2A families mutations in RET exon 10 or exon
11 are identified. Herein we report a MEN 2A case affected by a mutation
(Gly533Cys) in exon 8. A 66-yr-old male patient was referred to our Department due
to bilateral adrenal nodules, revealed incidentally on a computed tomography of the
abdomen. Patient’s family history was remarkable for pheochromocytoma in his
mother. On physical examination there were no features of von Hippel-Lindau
disease (VHL) or neurofibromatosis type 1(NF1). Biochemical evaluation (elevated
normetanephrines and metanephrines excretion) and findings of the adrenals’
magnetic resonance imaging (hyperintense adrenal nodules on T2-weighted image)
were compatible with the diagnosis of bilateral pheochromocytomas. The patient
underwent laparoscopic bilateral adrenalectomy and histological examination
confirmed the preoperative diagnosis of pheochromocytoma. Absence of phenotypic
characteristics of VHL or NF1 and elevated basal and stimulated by pentagastrin
serum calcitonin levels raised the possibility of MEN 2A syndrome. Total
thyroidectomy was performed and histological examination showed the presence
of MTC. Genetic testing for the presence of a RET mutation was also recommended.
Direct sequencing of exon 8 from patient’s genomic DNA revealed the mutation
c.1597G–OT (Gly533Cys). So far, the above missense point mutation has been
associated with familial MTC (FMTC) but, to the best of our knowledge, mutations
in exon 8 have never been identified in a MEN 2A case. In conclusion, in patients with
clinical suspicion of MEN 2A syndrome the analysis of RET exon 8 should be
considered when routine evaluation of mutations in exons 10, 11 and 13 is negative.
Clinical and biochemical effects of adjuvant mitotane treatment in
patients with adrenocortical cancer (ACC)
Fulvia Daffara1, Silvia De Francia2, Giuseppe Reimondo1, Barbara Zaggia1,
Paola Sperone3, Francesco Di Carlo2, Alberto Angeli1, Alfredo Berruti3 &
Massimo Terzolo1
Dipartimento di Scienze Cliniche e Biologiche - Medicina Interna I, ASO
San Luigi, Orbassano, Italy, 2Dipartimento di Scienze Cliniche e Biologiche
- Laboratorio di Farmacologia, ASO San Luigi, Orbassano, Italy,
Dipartimento di Scienze Cliniche e Biologiche - Oncologia Medica, ASO
San Luigi, Orbassano, Italy.
Seventeen patients (9 women, 8 men aged 36 years, 22–58) radically resected for
ACC were treated with adjuvant mitotane and prospectically followed from 2000
to 2006.
Stage of ACC: was: 1 stage I,; 12 stage II, 4 stage III; Weiss score 6, 3–9; Ki67% 20,
4–67. Eleven patients had functional tumors. Median duration of treatment was 15
months (range:4–84) and 14 patients are currently on mitotane, 2 died, 1 discontinued
treatment after 5 years. All patients were treated with a low-dose regimen (till to 3–
4 g/die) and underwent monitoring of plasma mitotane level every 3 months. None of
the patients discontinued mitotane definitively for side effects and 16/17 patients
reached the therapeutic levels after a median time of 3 months. At the last follow up,
6/17 (35%) patients have relapsed, 15 patients are still alive.
Hyperprolactinemia was observed in 50% of men and 40% of women, 62% of
men become partially hypogonadic: reduction of free testosterone was greater
than total testosterone. Central hypothyroidism developed in 9 patients who were
treated, while 4 patients already on thyroxine required dose increment. Fifteen
patients developed overt hypoadrenalism, while 1 patient showed normal cortisol
and elevated ACTH, 11 patients developed hypoaldosteronism. Total cholesterol
level were slightly enhanced with increase of HDL and reduction of LDL,
triglicerides were normal. Reduction of folate level and consequent increase of
homocysteine was also observed. Mitotane levels were inversely correlated with
cortisol (PZ0.007), aldosterone (PZ0.01) and FT4 levels (PZ0.03), while they
were positively correlated with PRA (PZ0.004) and HDL levels (PZ0.005).
In conclusion, a low-dose regimen of adjuvant mitotane is well tolerated and able to
reach the therapeutic interval. Adequate supplementation of adrenal and sex steroid
and thyroid hormones is necessary. Some effects of mitotane may be ascribed to
either adrenolytic or estrogen-like actions of the drug.
9th European Congress of Endocrinology, Budapest, Hungary, 2007
Effectiveness of retinoic acid treatment for redifferentiation of thyroid
cancer in relation to recovery of radioiodine uptake
Cristián A. Fernández Fernández1, Manel Puig-Domingo1,
Francisco Lomeña1, Montserrat Estorch2, Angel L Bittini3,
Mónica Marazuela5, Javier Santamarı́a4, Tomás Martı́n7,
Purificación Martı́nez de Icaya6, Immaculada Moraga5, Marı́a Cuesta7,
Ana Mejı́as8, Manel Porta9, Dı́dac Mauricio2 & Irene Halperin1
Hospital Clinic i Provincial de Barcelona, Barcelona, Spain; 2Hospital de
Sant Pau, Barcelona, Spain; 3Hospital Gregorio Marañon, Madrid, Spain;
Hospital de Cruces, Barakaldo, Spain; 5Hospital de la Princesa, Madrid,
Spain; 6Hospital de Leganés, Madrid, Spain; 7Hospital Virgen Macarena,
Sevilla, Spain; 8Hospital Juan XXIII, Tarragona, Spain; 9Hospital de Vic,
Vic, Spain.
In the present study we demonstrated that CST mRNA is widely expressed in
samples of patients with leukemic disease and in malignant NHL. On the other
hand, expression of SS is absent in most cases. These findings suggest that, in line
with our findings in normal human immune cells, CST might play a regulatory
role, potentially with respect to control of proliferation or cytokine secretion, in
these diseases, rather than SS. Further studies will be necessary to evaluate the
role of CST and the potential therapeutical implications of CST or CST-like
Retinoic acid (RA) treatment has been used in the last decade for redifferentiation
of metastatic thyroid cancer that have lost radioiodine uptake (RIup) with
heterogeneous results.
To evaluate the improvement of RIup after a course of RA treatment.
Retrospective analysis of 29 patients with radioiodine negative metastatic disease
(17 men /12 women; 22 papillary, 4 follicular and 3 oncocytic tumours). RA was
given at a dose of 0.66–1.5 mg/kg for 5–12 weeks, followed by a therapeutic 131I
dose (3700–7400 MBq). Thyroglobulin levels and CT imaging control after 3
months of RA were performed.
In 44.8% of the patients (14 out of 29 cases, 11 papillary/3 follicular) a positive
radioiodine scan was observed; in 7 additional cases (5 papillary, 2 oncocytic) a
weak RIup was also apparent (total responders 21/29, 72.4%), and in the
remaining 8 the RIup persisted negative (6 papillary, 1 follicular and one
oncocytic). No correlation was observed between changes in thyroglobulin levels
and recovery of RIup. In 11 RA positive treatments a stabilization of mestastasic
growth was observed in 5, while in 6 tumoural mass increased at short term. No
major side effects were detected.
A relatively high rate of reinduction of RIup after RA treatment may be possible
in advanced stage papillary and follicular thyroid cancer patients, with
uncertainty in relation to a potential modification of the natural course of the
disease. Further studies, aiming to identify potential responders to RA treatment
by a better characterization of the biological nature of these tumours, will be
required for an improved indication of RA coadjuvant treatment of thyroid cancer
in the future.
A loss-of-function polymorphic mutation in the P2X7 receptor gene in
patients with papillary thyroid cancer
Angela Dardano1, Simonetta Falzoni2, Antonio Polini1, Alessia Bemi1,
Anna Solini1, Nadia Caraccio1, Francesco Di Virgilio2 & Fabio Monzani1
University of Pisa, Pisa, Italy; 2University of Ferrara, Ferrara, Italy.
Extracellular nucleotides, via specific plasma membrane receptors (P2Rs) of the
X and Y subtype, modulate several cell functions, including cell-to-cell cross talk.
We have previously demonstrated the expression of several functional P2XRs
subtypes, including P2X7, in primary human thyrocytes. P2X7 is the main player
in inflammation and immunomodulation; a strong expression of this receptor has
been shown in several human solid tumors. Polymorphisms of the gene encoding
for P2X7 have been described; among these, 1513AOC induces loss-of-function
while 489 COT gain-of-function of the receptor.
We evaluated the presence of 1513AOC and 489COT polymorphisms in
patients with papillary thyroid carcinoma (PTC).
P2X7R genotypic analysis was performed in 83 patients with PTC (70 women;
mean age 43G13 yrs; 29 with diameter !1 cm; 33 with follicular and 50 with
classical variant) and 100 healthy subjects (Bone Marrow Bank donors, Ferrara).
The single nucleotide polymorphisms were analyzed in genomic DNA samples by
the TaqMan MGB probe technique. Results are summarized in the table.
Table 1
Polymorphism Minor Allele
Frequency Genotype (%)
Expression of the neuropeptide cortistatin in haematological
Virgil Dalm, Frank Staal, Leo Hofland, Aart-Jan van der Lely & Martin van
Erasmus MC, Rotterdam, Netherlands.
Cortistatin (CST) is a 17 amino-acid neuropeptide involved in sleep regulation.
Due to its structural resemblance to somatostatin (SS), CST binds with high
affinity to the 5 known SS receptors. CST also binds to the putative MrgX2
receptor. Previously we demonstrated that various types of human immune cells
and tissues as well as lymphoid cell lines express CST mRNA. We suggested that
CST plays a regulatory role in immune cell function both in physiological and
pathophysiological conditions.
In the present study we investigated CST expression in human haematological
malignancies, in order to gain more insight in the potential significance of CST in
these diseases.
Patients and methods
Bone marrow and peripheral blood samples of 38 patients with T-ALL
and B-ALL were studied using micro-array technique (Affymetrix) and 5
lymph node biopsies from patients with non-Hodgkin’s lymphoma (NHL)
using Q-PCR. Expression of both SS and CST mRNA was investigated in
all samples.
In 11 out of 22 patients with B-ALL CST expression was found, whereas in only 1
patient SS expression could be detected. Moreover, in 14 out of 16 patients with
T-ALL CST expression was detected, while SS expression was present in only 1
patient. In all 5 NHL biopsies low expression of CST mRNA was detected, while
no SS mRNA was found.
Increased homozygous substitution 1513AOC was detected only in patients
with the follicular variant (22%). A significant correlation with PTC dimension
was also observed (PZ0.02). No differences were detected in the allelic
frequencies for 489COT.
Overall, our data demonstrate an increased prevalence of 1513AOC
polymorphism in patients with PTC. This loss-of-function polymorphism
characterized the follicular variant and correlated with cancer dimension. Further
studies are needed to evaluate the role of 1513AOC polymorphism as a novel
clinical marker of differentiated thyroid carcinoma.
Enhanced expression of functional P2X7 receptor in human papillary
thyroid cancer
Angela Dardano1, Davide Ferrari2, Sabina Cuccato1, Eleonora Santini1,
Nadia Caraccio1, Sara Gulinelli2, Giulia Callegari2, Pinuccia Faviana1,
Anna Solini1, Francesco Di Virgilio2 & Fabio Monzani1
University of Pisa, Pisa, Italy; 2University of Ferrara, Ferrara, Italy.
Extracellular ATP modulates several biological processes via activation of
plasma membrane receptors (P2Rs) in normal human thyrocytes (NT). We
characterized P2Rs expression and function in two thyroid cancer cell lines: FB1
(anaplastic cancer) and FB2 [papillary cancer (PTC)]. P2Rs expression was
evaluated by RT-PCR and WB, intracellular Ca2Cchanges by fluorimetric
technique (Fura2-AM), IL-6 release by ELISA, intracellular [i(ATP)] and
extracellular ATP [e(ATP)] concentration by luminometry.
Endocrine Abstracts (2007) Vol 14
9th European Congress of Endocrinology, Budapest, Hungary, 2007
FB1 and FB2 showed significantly higher e(ATP) and i(ATP) concentration than
NT (P!0.001 for both). [Ca2C] fluxes induced by e(ATP) (1 mM, in the presence of
external Ca2C) were higher in both FB1 and FB2 than NT cells, (P!0.01).
Moreover, the addition of ATP (0.25 and 1 mM) induced a significantly higher IL-6
release respect to NT (P!0.001at both ATP concentrations) in both cell lines. The
P2X7 agonist BzATP, almost ineffective in NT, induced a huge IL-6 release in FB2
(from 6315G328 to 11764G1652 and to 25661G2815 pg/ml/1.5x105 cells with
BzATP 0.25 and 1 mM, respectively) and FB1, although at a lesser extent (from
7388G170 to 8721G1332 and to 10620G2216, respectively). Moreover, IL-6
release was prevented either by oxidized-ATP or KN-62, selective blockers of
human P2X7. Accordingly, FB2 cells showed a strong expression of P2X7, less
evident in FB1 cells. These findings demonstrated an enhanced expression of
functional P2X7 receptors in thyroid cancer cell lines. Therefore, we checked P2X7
expression in 33 human PTC histological samples, confirming an increased P2X7
expression in cancer than in normal thyroid tissue both by RT-PCR (P!0.0001) and
immunostaining (avidin-biotin method) (72G15% Vs 8G3% of cells, respectively).
In conclusion, human thyroid cancer is characterized by an enhanced P2XRs
function; specifically, PTC shows a strong P2X7 expression in comparison to normal
thyroid tissue. The increased P2X7R function may play a role in the modulation of the
inflammatory response to neoplasia.
Results 90Y-DOTATATE therapy in patients with neuroendocrine
tumours (NETs) - own experience
Jolanta Kunikowska1, Alicja Hubalewska-Dydejczyk2, Anna Sowa-Staszczak2, Leszek Krolicki1, Pawel Ochman1, Renata Mikolajczak3,
Dariusz Pawlak3, Malgorzata Kobylecka1, Joanna Maczewska1 &
Bohdan Huszno2
Nuclear Medicine Department, Medical Academy, Warsaw, Poland;
Department of Endocrinology, Medical College at Jagiellonian University,
Cracow, Poland; 3Radioisotope Centre POLATOM, Otwock-Swierk,
In the 1980 s the discovery of expression of somatostatin receptors on NET cells
made the use of somatostatin analogues in diagnosis and therapy possible.
The aim
Of the study was to assess response of targeted radio-nuclide therapy with
radio-labelled somatostatin analogue 90Y-[DOTA0,D-Phe1,Tyr3]-octreotate
(DOTATATE) in treatment of disseminated NETs.
Material and methods
12 patients (aged 56.7C/K11.2): carcinoid-5 pts, insulinoma-1pt, gastrinoma2 pts, pancreatic NET-2 pts, ca neauroendocrinale without primary tumor-1,
stomach NET-1 pt) were enrolled in the study. Before the therapy, blood tests for
hematology, kidney and liver function and CgA were performed. All patients
underwent CT scans and 99mTc-HYNIC/EDDA-octreotate SRS. Treatment with
Y-DOTATATE) was repeated every 4–6 weeks up to the total of 200 mCi/m2.
Amino acids infusion was used for kidney protection.
One year observation: regression of disease (PR -decrease of size and number
of metastases, YCgA level, good clinical response) was observed in 6 pts,
stable disease (SD-stable size and number of metastases, YCgA) in 3 pts. 3
patients died. No nephrotoxicity was observed. WBC and PLT levels were
stable during therapy in 3 pts (without chemotherapy). In 1 pt with previous
chemotherapy (last course a month before radiotherapy), PLT level decreased
(220!103/mm3 w 47!103/mm3after the first course); the patient died 2
months after the beginning of the therapy. In 8 pts leucopoenia was observed
(! 4!103/mm3) but serious neutropenia (!2!103/mm3) was found in 3 pts
with previous chemotherapy. Thrombocytopenia (PLT!100!103/mm3) was
observed in 2 patients with previous chemotherapy.
Two-year observation: prolonged PR – 4 pts; SD – 3 pts, progression of disease
in 2 pts: with gastrinoma and stomach NET without hormonal activity (4 and 9
months after radiotherapy). Blood tests stable.
PR and SD were observed in 9/12 patients with disseminated NET. Severe
haematologic toxicity was mainly observed in patients after prior chemotherapy –the
question of optimising the time between chemotherapy and radiotherapy is still open.
In ESC for the period since October 2004 till October 2006 were operated 69
patients with acromegaly. Men were 22 (32%), women – 47 (68%). Age of
patients changed from 24 till 68 (middle – 47).
All patients were separated into 2 groups: surgery (group 1) and combination
treatment (group 2), which consist of surgery and somatostatin analogues therapy
before and after surgery.
In most cases were macroadenomas, only 5 patients (7%) had microadenomas.
Suprasellar invasion had 21 patients (30%), infrasellar – 28 (41%) and 32%
patients had invasion to one or both cavernous sinuses.
50 patients operated by transnasal approach and 19 with endoscopic
techniques. In 47 cases (69%) tumor was total removal, in 17 – subtotal (not
less 90% tumor mass was removal), and in 5 cases (7%) – partial removal.
Significant clinical improvement is seen in most patients – 66 (97%). Reduce
diabetes mellitus we observed at 43% patients (6 from 14), visual improvement
had 78% patients (14 from 18).
Nobody had CSF leak after operation. Diabetes insipidus had 6 patients (9%).
Pulmonary embolus had 3 patients (1 patient died).
After 6–12 months were examination 14 patients from group 1 and group 2. GR was
normalized in 79% of patients of each group. IGF-1 was normalized in 75% of each
group. And postglucose GH level was normalized in 46% into group 1 and 58% into
group 2.
Transsphenoidal surgery for acromegaly is safe and effective treatment with
minimal mortality and morbidity.
Obvious distinctions in postoperative dynamics IGF-1 and postglucose GH in both groups
it is not revealed. There is a tendency in greater efficiency of the combined treatment.
Adrenal incidentaloma, an oncological or endocrinological enigma?
Clinical analysis of 1300 cases observed at a single endocrinological
Anna Kasperlik-Zaluska1, Elzbieta Roslonowska1, Jadwiga SlowinskaSrzednicka1, Wojciech Zgliczynski1, Wojciech Jeske1, Lucyna Papierska1,
Maciej Otto2, Rafal Slapa2, Andrzej Cichocki3 & Jaroslaw Cwikla4
Centre for Postgraduate Medical Education, Warsaw, Poland; 2Warsaw
University of Medicine, Warsaw, Poland; 3Centre and Institute of Oncology,
Warsaw, Poland; 4Hospital of MSWiA, Warsaw, Poland.
Incidentally found adrenal tumour (adrenal incidentaloma Z AI) is the most
frequent adrenal disorder. Every patient with AI has to be evaluated carefully to
choose the best method of management. We present our experience with a group
of 1300 patients with AI, registered at our department.
Material and methods
Material consisted of 1300 patients (female/male ratio 2.6, age 10–87 years) with
AI ranging in size from 0.8 to 23.0 cm. Methods: clinical examination, biochemical
assays, hormonal determinations (cortisol, androgens, ACTH, aldosterone,
metanephrines), imaging studies (ultrasound scans, CT, MRI), histological/
immunocytochemical investigations in 420 patients treated by surgery.
Basing on these examinations we diagnosed in our material 116 patients with adrenal
cancer, 14 – with other primary malignant adrenal tumours, 48 – with metastatic
tumours and 1122 with probably benign tumours. The most important criteria for
surgery were imaging phenotype (mainly high density, over 20 HU in the I phase of
CT), size (S5 cm) rapid growth of the tumour and suspicion of a clinically silent
chromaffin tumour (for fear of an unexpected metanephrines crisis). In some cases of
adrenal cancer elevated levels of androgens have been noted. The most frequent form
of subclinical hyperactivity has been pre-Cushing’s syndrome (6.5%).
1/Malignant adrenal tumours were found in 178 patients (14%), in this number
adrenal cancer in 9%. 2/ The oncological criteria for surgery were of primary
importance in our material, with the elevated density in CT (I phase) as the main
single indication.
Results of treatment of patients with pituitary somatotroph adenomas
Andrey Grigoriev, Natalye Molitvoslovova, Galina Kolesnikova &
Anatolij Kuzmin
Endocrinology Scientific Centre, Moscow, Russia.
Endocrine Abstracts (2007) Vol 14
Frequency and type of adrenal tumors in our patients
Milica Medic-Stojanoska1, Branka Kovacev-Zavisic1, Tijana Radovanov1,
Ivana Bajkin1, Jovanka Novakovic1, Milena Mitrovic1, Dusan Z Tomic1,
Nilkola Curic2 & Ljiljana Todorovic-Djilas1
Clinic for Endocrinology, Institute for Internal Medicine, Clinical Center of
Vojvodina, Novi Sad, Vojvodina, Serbia; 2Department for pathological
physiology, Clinical Center of Vojvodina, Novi Sad, Vojvodina, Serbia.
9th European Congress of Endocrinology, Budapest, Hungary, 2007
In recent years, adrenal tumors (AT) are no rare disease. They may arise from all
zones of adrenal cortex and medulla, benign or malignant, sometimes as metastases of
distant malignances. Patient’s present hormone excess or mass effect, but part of them
is clinically silent. The aim of this study was to investigate the frequency, hormonal
secretion and pathohistology of AT in our patients lasting years. All patients with AT
which are hospitalized in the period from January 1st, 2000. to October 15th, 2006. in
our Clinic are included in study. Data of clinical feature, hormonal secretion, imaging
and pathohistology of AT are collected in our hospital register of admitted patients
and medical records. Patients with AT are divided according to hormonal secretion
and pathohistology per years. Linear trend are calculated.
During this 7 years in our Clinic are admitted 102 patients with AT, 65 (63,72%)
females and 35 (36,28%) males. It has been 2,38% of all hospitalized patients.
Hormonally inactive are presented 64,71%. Patients with hormonally active AT be
demonstrated as Cushing’s syndrome (18,63%), Syndrome Conn (8,82%) and
pheochromocytoma (3,92%). According to data of histology and immunohistology
after surgery, 89,22% be presented as benign and 10,78% as malignant. Only 5,88%
of malignant tumors has been metastases of distant tumors. Linear trend is pointed
the increase of incidence patients with AT during period of observation.
The incidence of patients with AT have tendency to increase lasting years in our
region. Benign and non-functionally AT are the most common.
LNCaP: co-incubation of fAd with leptin resulted in decreased cell proliferation;
fAd alone had little effect. gAd alone slightly increased proliferation and had little
effect when co-incubated with leptin. fAd alone increased p53 mRNA expression
and rescued leptin-induced inhibition of p53 expression; both fAd and gAd alone
increased bcl-2 expression, but reduced expression to below basal when
co-incubated with leptin. PC3: fAd decreased proliferation at 100nM, but reduced
proliferation to half of basal when co-incubated with leptin; gAd alone increased
proliferation but reduced proliferation to basal when co-incubated with leptin. Both
fAd and gAd demonstrated significant dose-dependent increases in p53 mRNA
expression when co-incubated with leptin; both fAd and gAd reduced bcl-2
expression to negligible levels despite the addition of leptin.
We show an interaction between adiponectin and leptin in the regulation of prostate
cancer cell proliferation through modulation of p53 and bcl-2 expression; this is most
marked in the advanced PC3 cell line. Concurrent hyperleptinaemia and
hypoadiponectinaemia in obese patients may modulate prostate cancer progression,
and serum leptin:adiponectin ratio could represent a new prognostic marker;
increasing circulating fAd in these patients may be a novel treatment for this disease.
Papillary thyroid cancer – the possible role of death ligands in tumor
Emese Mezosi1, Ferenc Gyory2, Agnes Borbely2, Bernadett Ujhelyi2,
Gyorgyike Soos2, Endre V. Nagy2, Zsuzsa Varga2 & Laszlo Bajnok1
University of Pecs, School of Medicine, Pecs, Hungary; 2University of
Debrecen, Medical and Health Science Center, Debrecen, Hungary.
Papillary thyroid cancer (PTC) cells and immune cells can kill each other by death
ligands. Death ligands induce apoptosis only in sensitive cells. The sensitivity to
apoptosis is regulated in a complex and poorly understood manner. The aim of this
study was to investigate the Fas ligand (FasL) and Tumor Necrosis Factor-Related
Apoptosis Inducing Ligand (TRAIL) expression in PTC cells and tumor infiltrating
immune cells. Twenty-six PTCs without and fifteen PTCs with cervical lymph
node metastasis were examined by immunohistochemistry. Lymphocytic and
macrophage infiltration, HLA-DR, FasL and TRAIL expressions were investigated. The intensity of positive staining was evaluated by a semiquantitative score
system. Macrophages and lymphocytes infiltrated the majority of tumor samples.
FasL expression of cancer cells was universal and did not show any correlation
with the intensity of lymphocytic infiltration and lymph node metastasis. A small
subgroup of lymphocytes in close proximity to tumor cells was strongly positive
for FasL. Lymphocytes did not express TRAIL. TRAIL expression of tumor cells
was increased in PTCs with lymph node metastasis (PZ0.01). Macrophages were
negative for death ligands. In summary, increased TRAIL expression of tumor
cells may inhibit the anti-tumor immunity and promote the formation of lymph
node metastasis. A subgroup of lymphocytes can use FasL for tumor cell killing.
This work was supported by a grant from the Hungarian Medical Research
Council (ETT 186/2003).
Leptin and adiponectin interact in regulating prostate cancer cell
Tina Mistry1, Janet Digby1, Ken Desai2 & Harpal Randeva1
University of Warwick Medical School, Coventry, United Kingdom;
University Hospital Coventry and Warwickshire, Coventry, United
Leptin and adiponectin have opposing properties and are implicated as molecular
mediators between obesity and (aggressive) prostate cancer. Adiponectin, circulates
inversely proportional to visceral fat accumulation, and has demonstrated antiproliferative effects in prostate cancer cells; circulating leptin levels increase with
visceral fat accumulation and has shown mitogenic effects. We propose that
adiponectin and leptin interact in prostate cancer cell growth regulation.
Materials and Methods
We studied the effect of full-length (fAd) and globular (gAd) adiponectin
(0.01 nM–100 nM) G 100 nM leptin on LNCaP and PC3 prostate cancer cell
proliferation. p53 tumour suppressor and bcl-2 oncogene expression was measured
using quantitative RT-PCR.
A novel role for Visfatin/Pre-B cell colony-enhancing factor 1 (PBEF)
/Nicotinamide phosphoribosyltransferase (NMPRTase) in prostate
Tina Mistry1, Janet Digby1, Joe Cross1, Ken Desai2 & Harpal Randeva1
University of Warwick Medical School, Coventry, United Kingdom;
University Hospital Coventry and Warwickshire, Coventry, United
Visfatin/PBEF is a novel adipokine circulating inversely proportional to visceral
fat mass and exerts insulin-mimetic effects; it is expressed in normal, inflamed
and tumour tissues. Visfatin/PBEF has also been identified as NMPRTase, a key
intracellular enzyme involved in NADC metabolism, replenishing NADC during
cellular respiration. Inhibition of NMPRTase by the anti-cancer agent FK866 has
been shown to induce apoptosis in tumours. Prostate cancer progression is
associated with obesity and its metabolic sequelae, and we propose a role for
visfatin/PBEF/NMPRTase in prostate carcinogenesis.
Materials and Methods
Visfatin expression was studied in normal and malignant prostate cancer tissue
and LNCaP and PC3 human prostate cancer cell lines using RT-PCR,
immunocytochemistry and confocal analysis. Regulation of visfatin expression
by testosterone, 5-alpha dihydrotestosterone (DHT) (10K6M) interleukin-6
(30 ng/ml) and insulin-like growth factor-1 (IGF-1) (10 ng/ml) was studied
using quantitative RT-PCR and Western blotting. We also investigated the effect
of visfatin G IGF-1 on LNCaP and PC3 cell proliferation.
Visfatin mRNA and protein were detected in LNCaP and PC3 cells and normal
and malignant prostate cancer tissue; visfatin protein demonstrated cytoplasmic
and nuclear distribution. Testosterone, DHT and IGF-1 increased visfatin mRNA
and/or protein expression in both the androgen-sensitive LNCaP and androgeninsensitive PC3 cell line. Treatment of PC3 cells with visfatin resulted in a dosedependent increase in PC3 cell proliferation which was enhanced in the presence
of IGF-1; co-incubation of visfatin and IGF-1 showed a synergistic dosedependent increase cell proliferation in LNCaP cells.
Our novel findings demonstrate a multifunctional (intra- and extra-cellular) role
for visfatin in prostate carcinogenesis, and provide greater insight into the
molecular association between obesity and prostate cancer. High visfatin
expression in prostate cancer cells may indicate poor prognosis, and inhibition
of visfatin may represent a novel therapeutic target for treatment of this disease.
Initial presentation of patients with acromegaly - analysis of the
German acromegaly register
Stephan Petersenn1, Martin Reincke2, Michael Buchfelder3, Holger Franz4
& Hans-Jürgen Quabbe5
Division of Endocrinology, University of Duisburg-Essen, Essen,
Germany; 2Klinikum Innenstadt, University of Munich, Munich, Germany;
Department of Neurosurgery, University of Erlangen-Nuremberg, Erlangen, Germany; 4Lohmann & Birkner Health Care Consulting GmbH, Berlin,
Germany; 5Prof. emer., Free University Berlin, Berlin, Germany.
Endocrine Abstracts (2007) Vol 14
9th European Congress of Endocrinology, Budapest, Hungary, 2007
Due to its rarity, initial endocrine abnormalities in acromegaly are difficult to
investigate in a large cohort, especially with respect to cofounding variables. We
searched the German Acromegaly Register for data on the first presentation of
patients with acromegaly.
Up to November 2005, 1485 patients with acromegaly had been entered into
the database. Male patients demonstrated significantly higher random GH (21.0
(0.2–620.0) ng/ml, median (range)) and IGF-1 (773.0 (118–2000) ng/ml) levels
than females with 14.0 (0.06–556.0) ng/ml (P!0.005) and 679.0 (136–2103)
ng/ml (P!0.0001). Furthermore, comparison of biochemical parameters for
various age decades demonstrated a significant association between increasing
age and decreasing random GH and IGF-1 levels. Gonadal insufficiency occurred
in 18.8%, secondary adrenal insufficiency in 11.8%, TSH deficiency in 7.5%, and
diabetes insipidus in 1.3% of subjects. Pituitary insufficiencies occurred with
higher frequency in male patients (39.1% vs. 22.0%, P!0.0001), and in a
significantly higher percentage of patients with macro- (31.6%) compared
to microadenomas (18.1%, P!0.005). During initial biochemical analysis, 6.4%,
1.5%, and 3.7% of subjects revealed non-pathological results for random GH
(!2.5 ng/ml), minimal GH during oGTT (!1 ng/ml), and IGF-1, respectively.
None had normal, and 91,4% had pathological results for all three parameters.
Whereas the combination of GH during oGTT and IGF-1 raised suspicion of
acromegaly in all subjects, 0.5% and 1.1% of subjects demonstrated normal
values with combinations of random GH and IGF-1, or random and glucose
suppressed GH, respectively.
In conclusion, biochemical activity of acromegaly may depend on age
and sex. Therefore, therapy may need to consider and being adapted according
to these parameters. Patients with acromegaly may need to be evaluated
for pituitary insufficiencies, even with microadenomas. The combination of
glucose-suppressed GH and IGF-1 may be the best screening parameters
for acromegaly.
Endocrine tumors and neoplasia – presented on Tuesday
Survivin – a promising target for immunotherapy in patients with
adrenocortical carcinoma
Martin Fassnacht1, Sebastian Wortmann1, Silviu Sbiera1,
Dorothee Kuehner1, Marion Wobser2, Patrick Adam3, Juergen C. Becker2 &
Bruno Allolio1
University of Wuerzburg, Dept. of Medicine I, Wuerzburg, Germany;
University of Wuerzburg, Dept. of Dermatology, Wuerzburg, Germany;
University of Wuerzburg, Dept. of Pathology, Wuerzburg, Germany.
Adrenocortical carcinoma (ACC) is a rare tumor with poor prognosis and limited
therapeutic options. Survivin is an anti-apoptotic molecule expressed by
neoplastic and tumor-specific endothelial cells of various carcinomas, but rarely
or only weakly in normal differentiated tissue. In melanoma and pancreatic
cancer, preliminary results of a survivin vaccination trial (www.clinicaltrials.gov)
indicated that an immunological response in patients is often paralleled by tumor
control. Hence, we investigated, whether survivin may also be a reasonable target
for an immunotherapy in ACC.
We performed survivin real-time-PCR in 14 ACCs and 13 normal adrenals. In
addition, survivin protein was analysed by immunohistochemistry in 78 ACC
samples and 5 normal adrenals using a tissue array (scoring of expression: 0–3).
Finally, the presence of spontaneous survivin-recognizing T-cells in the
peripheral blood of 7 ACC patients were investigated by indirect interferongamma-ELISPOT using HLA-A1, -A2 or -B35 restricted survivin peptides.
Survivin RNA was detectable in 11/12 ACCs and 8/13 normal adrenals.
However, the mean expression in ACC was an order of magnitude higher than
in normal adrenals (9071G5561% vs. 100G25%, P!0.001). Immunohistochemistry confirmed survivin protein expression in 89% of ACCs.
Moreover, in 38/78 of the ACCs but in none of the normal adrenals the
expression was judged as moderate-to-high (score 2 or 3). Notably, in 1/7
ACC patients spontaneous HLA-A2-restricted survivin-specific T cells
response was detected suggesting that the used epitope might be of
immunotherapeutic value.
This is the first study addressing survivin expression in a large series of ACC
patients. Since antiapoptotic survivin is overexpressed in many ACCs and
exhibits immunogenic properties, it is an intriguing target for immunotherapy also
in this rare disease. Especially in patients with refractory ACC having progressed
after several cytotoxic therapies an experimental vaccination approach seems to
be justified and promising.
Endocrine Abstracts (2007) Vol 14
Thyroid cancer: with an unexpected location – in the pancreas and in an
unexpected combination with Boeck’s sarcoidosis
Zsuzsanna Valkusz1, Éva Csajbók1, János Gardi1, Lilla Kardos2,
László Tiszlavicz3 & László Pávics4
Endocrin Unit, University of Szeged, Szeged, Hungary; 2International
Medical Center, Szeged, Hungary; 3Dept. of Pathology, University of
Szeged, Szeged, Hungary; 4Dept. of Nuclear Medicine, University of
Szeged, Szeged, Hungary.
The incidence of differentiated thyroid cancer gradually increased in the last few
decades. Primery thyroid cancer is usually located in the thyroid gland and can be
classified into well differentiated and poorly differentiated forms. Sooner or later,
these cancers metastatize into local lymphnodes or distant organs.
We present the histories of two patients with anusual forms of thyroid cancer.
A woman of 64 was admitted in our department in 2004, due to an
inoperable tumor in the pancreas. Histological sampling revealed a well
differentiated ectopic follicular thyroid cancer. After total thyroidectomy (no
malignancy in the thyroid), 131-I scintigraphy showed isotope accumulation
int he pancreas.
Repeated high-dose 131-I therapy shrank the size of the pancreatic tumor
and markedly decreased the thyroglobulin level in the serum. One year after
these interventions, the patient feels well, has no further distant metastases
and is treated for insulin-dependent diabetes mellitus; TSH is sctrictly
suppressed by thyroxine medication.
A man 28 was admitted in our department for severe dyspnea in 2004.
The computed tomography of the chest detected disseminated patches in the
lung with enlarged lymphnodes both int he mediastinum and ont he neck.
Total thyroid surgery plus modified cervical and mediastinal lymphnode
dissection showed a papillary type thyroid cancer metastatizing into the lung
and combined with Boeck’s sarcoidosis. Postoperative thyroglobulin level
was foud extremely high and 131-I scintigraphy showed pulmonary
accumulation. Repeated radioiodine treatment resulted in decreasing
thyreogobulin level and strongly improved picture of the chest by computed
tomography. The patient is under TSH suppressing therapy.
Thyroglobulin-antibodies in the “normal” range may decrease the
diagnostic accuracy of thyroglobulin in the care of patients with
differentiated thyroid cancer
Locsei Zoltán1, Toldy Erzsébet1, Szabolcs István2 & Kovács L. Gábor3
Markusovszky Hospital, szombathely, Hungary; 2National Medical Centre,
Budapest, Hungary; 3University of Pécs, Pécs, Hungary.
The use of thyroglobulin (Tg) as tumor marker in differentiated thyroid cancer
(DTC) is limited in the presence of thyroglobulin-antibodies (TgAb) but it is
generally believed that this is true only for TgAb concentrations over the normal
‘cut off’ point.
The aim
Of this study was to investigate if TgAb-s in the normal range, considered to be
physiological, may also influence the accuracy and clinical relevance of Tg
Recombinant human TgAb (Roche) was added stepwise to serum-samples
(nZ45) with TgAb concentrations near to the analytical sensitivity of the method
(10 IU/ml), aiming to have TgAb concentrations of 50–100–150 and 200 IU/ml
(ECLIA Elecsys 2010 Roche, normal ‘cut off’ !115 IU/ml). After this, Tg levels
were measured at all TgAb concentrations by electrochemiluminescence
immunoassay (ECLMA, Elecsys 2010, Roche). Additionally, 134 samples from
27 patients with DTC were measured for Tg, Tg-recovery (Tg%) and TgAb.
In the in vitro experiment, TgAb and Tg concentrations showed strong correlation
(rZ0.93, P!0.01) both at normal and elevated TgAb levels, which could be
described mathematically as: Loss of TgZK0.43 Ln(TgAb IU/ml)C1,06.
Patients with non-detectable Tg had higher antibody levels than those with
detectable Tg. There was a rather weak negative correlation (rZK0,32
P!0.001) of Tg% to TgAb and in 19% of the samples the results were clinically
discordant. In 2/27 patients, on-T4 Tg levels of !2.0 ng/ml were corrected to be
O2,0 ng/ml by using the above function. Subsequent off-T4 Tg levels appeared to
be significantly elevated in both.
Physiological (normal) TgAb concentrations may also decrease serum Tg but
their effect can be calculated from the actual Tg and TgAb concentrations by the
9th European Congress of Endocrinology, Budapest, Hungary, 2007
mathematical model described. The findings stress the importance of parallel
Tg and TgAb measurements in patients with DTC expected to have undetectable
or low Tg.
Dopamine receptor expression and dopamine agonist effectiveness in
post-surgical persistent medullary thyroid cancer
Rosario Pivonello1, Piero Ferolla2, Antongiulio Faggiano1, Diego Ferone3,
Enrica Cerasola3, Gabriella Angeletti2, Fausto Santeusanio2,
Francesco Minuto3, Gaetano Lombardi1, Steven WJ Lamberts4, Leo
J Hofland4 & Annamaria Colao1
Department of Molecular and Clinical Endocrinology and Oncology,
“Federico II” University, Naples, Italy; 2Department of Internal Medicine
and Endocrinological Sciences, University of Perugia, Perugia, Italy;
Department of Endocrinological and Metabolic Sciences, University of
Genova, Genova, Italy; 4Department of Internal Medicine, Erasmus Medical
Center, Rotterdam, Netherlands.
Dopamine receptors was suggested to be expressed in medullary thyroid cancer
(MTC). The aim of the current study was to evaluate the expression of D2
dopamine receptor in MTC and the effectiveness of the dopamine agonist
cabergoline in patients with MTC. Five paraffin-embedded cases of MTC
obtained after thyroidectomy were used to evaluate D2 receptor expression by
immunohistochemistry. Fifteen patients (7 males, 8 females, 36–78 years) with
post-surgical persistent and not operable MTC were treated with cabergoline for 4
months, in order to evaluate its effect on clinical syndrome, serum calcitonin (CT)
and CEA levels, and metastasis number and size. Cabergoline was administered at
the dose of 1 mg/week for the first month and 3.5 mg/week for the following 3
months. D2 receptor was variably expressed in all 5 cases of MTC. Before
treatment, all patients had progressively increasing serum CT and/or CEA levels.
Lymph node metastasis were visible in 4, whereas liver and lung metastasis were
identified in 1 and 2 patients, respectively. At the 4-month follow-up, a significant
decrease of serum CT (PZ0.027) but not CEA (PZ0.244) levels was found.
A O50% decrease in serum CT levels was found in 3 (20%), a 25–50% decrease
was found in 10 (66.7%) and an increase in serum CT levels was found in 2
(13.3%) patients. A significant improvement in flushing (PZ0.039) and fatigue
(PZ0.023) and a slight improvement in diarrhoea (PZ0.066) score was also
found. No significant change was found in body weight. No significant change
was observed in metastasis number and size, although one patient experienced a
disease progression. In conclusion, the results of this study demonstrated that D2
receptor is expressed in MTC and that cabergoline treatment improve clinical
syndrome and decrease serum CT levels in patients with post-surgical persistent
MTC. Further studies on a larger number of patients and longer period of
treatment are mandatory to draw definitive conclusions on the usefulness of
cabergoline treatment in patients with MTC.
Somatostatin analogues and the PI3K-AKT-MTOR-P70S6K pathway:
how do they control the proliferation of neuroendocrine tumours?
Giulia Franchi, Simona Grozinsky-Glasberg, Antonio Ribeiro de Oliveira,
Nabila Salahuddin, Márta Korbonits & Ashley B. Grossman
Department of Endocrinology, William Harvey Research Institute, Barts
and the London, Queen Mary School of Medicine, University of London,
EC1M 6BQ, UK, London, United Kingdom.
Somatostatin analogues are very useful in the treatment of symptomatic
neuroendocrine tumours, but effects on proliferation remain unclear. Overexpression of the proto-oncogene protein kinase Akt has been demonstrated in
certain endocrine tumours, and activates downstream proteins including mTOR
and p70S6K, which play a significant role in cell growth and proliferation. We
have therefore explored the site of action of somatostatin in causing inhibition of
proliferation in a neuroendocrine cell line.
To confirm the anti-proliferative effects of SS analogue treatment in a rat
insulinoma cell line (INS-1), and to investigate whether the SS analogues act on
the PI3K-Akt-p70S6K pathway.
RT-PCR was used to demonstrate SS receptors (SSTR) in the INS-1 cell lines.
MTS and thymidine incorporation were used to determine the effects of the
SS analogues octreotide (SSTR2 agonist) and pasireotide (SOM230, Novartis;
activation of SSTR-1, 2, 3 and 5) on cell proliferation. Western blotting was
used to characterise phosphorylated-Akt and p70S6K expression in the
SS-treated cells.
The INS-1 cells expressed SSTR 1, 2, 3 and 5. Treatment with octreotide and
pasireotide caused significant dose-responsive inhibition of proliferation. No
difference in phospho-Akt (either Ser473 or Ser308) expression was detected in
the octreotide-treated INS-1 cell lysates. However, phospho-p70S6K (Thr389)
expression was significantly reduced at 10 minutes-6 hours treatment with
octreotide 10K9M (PZ0.01), while no effect on phospho-p70S6K (Thr229)
expression was observed at 30 and 60 minutes. It is known that Thr229 site of
phosphorylation is affected by PDK1 upstream of Akt. Treatment with IGF-1
(10nM) increased both phospho-p70S6K (Thr389) and phospho-Akt
Octreotide and pasireotide treatment inhibited proliferation of INS-1 cells and, at
a concentration achieved in clinical human use, octreotide attenuated p70S6K
(Thr389) phosphorylation, but not Akt phosphorylation. We conclude that SS
analogues acts downstream of Akt to inhibit the mTOR-p70S6K pathway.
Angiotensin 4–8 and angiotensin 5–8 inhibit cell proliferation in GH3
rat pituitary lactosomatotroph tumor cell culture
Dorota Ptasinska-Wnuk, Jolanta Kunert-Radek, Hanna Lawnicka &
Marek Pawlikowski
Medical University of Lodz, Lodz, Poland.
In many tissues angiotensin peptides acts as the auto/paracrine growth factors.
Their effects are dependent on activation of various intracellular signaling
pathways, including mitogen-activated protein kinases (MAPK).
Angiotensin II (ang II) is the best known angiotensin peptide. The ang II
derivatives, angiotensin III (ang III) and angiotensin IV (ang IV) posses
biological activity as well. Both ang II and ang IV are known to promote the
proliferation of rat prolactinoma cells in vitro and rat anterior pituitary cells
in vivo. The role of ang IV degradation products, angiotensin 4–8 (ang 4–8) and
angiotensin 5–8 (ang 5–8) in the regulation of cellular growth has not already
been investigated.
In our study we examined the influence of ang 4–8 and ang 5–8 on the GH3 cells
(rat pituitary lactosomatotroph tumor cells line) proliferation and the possible role
of two MAPK pathways (p44/42 and p38) in ang 5–8 regulatory action.
Material and Methods
GH3 cells were cultured in F-10 medium and then plated at 96-multiwell plates
(10!103 cells/well). After 12 hours of preincubation cells underwent to 72-hours
treatment either with ang 4–8 or ang 5–8 alone or with the combination of ang 5–8
and p44/42 MAPK-kinase or p38 MAPK inhibitor (PD98059 or SB203580
respectively). Cell proliferation was evaluated using two colorimetric assays:
based on the measurement of cell activation and on the BrdU incorporation during
DNA synthesis.
Ang 4–8 and ang 5–8 decreased both the cell activation and BrdU incorporation in
GH3 cells culture. SB203580 prevented only the ang 5–8-induced inhibition of
cells activation. Non of ang 5–8 effects was abolished by PD98059.
Ang 4–8 and ang 5–8 inhibit GH3 cell proliferation. This mechanism is
independent of both MAPK p44/42 and MAPK p38. They probably exert
additional proapoptotic effect, mediated by MAPK p38.
Epidermal growth factor receptor (EGFR) as a potential new target in
the treatment of patients with adrenocortical carcinoma – results of preclinical studies
Martin Fassnacht1, Stefanie Hahner1, Barbara Heinrich1, Patrick Adam2,
Sarah Johanssen1, Marcus Quinkler3, Ann-Cathrin Koschker1,
Philipp Stroebel4, Alexander Marx4 & Bruno Allolio1
University of Wuerzburg, Dept. of Internal Medicine I, Wuerzburg,
Germany; 2University of Wuerzburg, Dept. of Pathology, Wuerzburg,
Germany; 3Charite University, Dept. of Medicine, Campus Mitte, Berlin,
Germany; 4University of Heidelberg, University Hospital Mannheim, Dept.
of Pathology, Mannheim, Germany.
Endocrine Abstracts (2007) Vol 14
9th European Congress of Endocrinology, Budapest, Hungary, 2007
Adrenocortical carcinoma (ACC) is a rare malignancy with incompletely
understood pathogenesis and poor prognosis. Overexpression of epidermal
growth factor receptor (EGFR) has been demonstrated in several tumors and
is partly associated with a more aggressive phenotype and a worse
prognosis. In addition, targeting the EGFR tyrosine kinase represents a
successful new therapeutic strategy, e.g. in non-small cell lung cancer.
Therefore, we investigated the role of EGFR in ACC as a potential
therapeutic target.
EGFR expression was analyzed by immunohistochemistry in 95 ACCs and 5
normal adrenals using paraffin sections and tissue arrays (scoring of
expression: 0–3). Utilizing the clinical data from the German ACC registry,
Kaplan Meier survival analyses were performed. In 30 patients the tumor
DNA was sequenced for mutations of the ‘hot spot’ exons 19–21 of the
EGFR gene. In addition, cells of the ACC cell line NCI-h295 were
incubated with the EGFR antibody cetuximab (1–100 mg/ml) and cell
proliferation was measured by MTT tests.
Immunohistochemistry revealed EGFR expression in 78% of ACCs.
In 55/95 (58%) of the ACCs and 0/5 of the normal adrenals the expression
level was judged as moderate-to-high (score 2 or 3). However, the
expression level did not correlate with the clinical outcome in these
patients. In addition, none of the sequenced tumor DNA samples showed
a mutation in exon 19–21. Cetuximab exhibited a dose dependent
antiproliferative effect in NCI-H295 cells (cell viability: 1 mg/ml: 95G2%;
10 mg/ml 90G3%*; 100 mg/ml 85G4%* vs untreated control cells:
100G3%; *ZP!0.01).
EGFR is overexpressed in the majority of ACC. Moreover, in vitro experiments
demonstrated that inhibition of EGFR signalling lead to moderate growth
inhibition in ACC cells. Therefore, in patients with ACC refractory to
established cytotoxic therapies the experimental use of EGFR inhibitors
(combined with cytotoxic therapy) seems to be justified.
Acromegaly due to a lung carcinoid: a case report
Rezzoug malika & Chentli Farida
Bab El Oued Hospital, Algiers, Algeria.
Acromegaly secondary to a lung carcinoı̈d is a very rare entity. Secretion of
GHRH (Growth hormone releasing hormone) or GHRH like by neuroendocrine tumor induces pituitary hyperplasia and a production of Growth
hormone (GH) with or without others anterior pituitary hormones. Total
resection of lung tumor induces normalisation of pituitary function as in our
AD, 37 years, male, came to our unit for diabetes mellitus and
acromegaly. His chest X ray showed a 7 cm right lung tumor. On hormonal
exploration there was a very high GH Z92 to 132 ng/ml (N!5), high
prolactine (PRL)Z120 ng/ml (N!20), elevated ACTHZ70 pg/ml
(NZ0–46)) and cortisol Z262 ng/ml (NZ50–210) without clinical signs
of Cushing’s syndrome. Thyreotrop function was preserved but there was
a gonadotrop deficit: testosterone Z0,91 ng/ml (NZ3–5). On MRI there
was a huge pituitary process impading the third ventricle and a destroyed
sella turcica.
GHRH and 5 HIA (5 hydroxyindolacetic acid) were not evaluated.
Surgical exploration and pathology study showed typical picture of carcinoı̈d
in the right lung. On post operative period there was a dramatic fall of GH
(Z1,2 ng/ml). PRL, ACTH and cortisol normalized and diabetes mellitus
disappeared. Three month after surgery MRI showed a significant reduction
of pituitary process with partial empty sella.
In this observation even if evaluation GHRH assay and immunohistochimy of
the tumor was not available, clinical, biological and radiological evaluation
confirmed that all endocrine abnormalities observed in our patient were due to
lung carcinoı̈d.
Time necessary to achieve the maximum effect of goserelin, LH-RH
agonist, in therapy of hormone dependent breast cancer
Jure Murgic, Martina Matovinovic, Lucija Fabijanic, Darko Katalinic &
Milan Vrkljan
University hospital Sestre milosrdnice, Zagreb, Croatia.
Nearly one third of women diagnosed with invasive breast cancer are younger
than 50 years with regular menstrual cycles. 60% of these tumors express
estrogene and progesterone receptors. Common treatment procedure is surgery
followed by chemotherapy, radiotherapy and hormone therapy. Often in younger
patients chemotherapy causes permanent amenorrhoea. In case that menses
afterwards occurs ovarial suppression is needed, mostly by goserelin, LH-RH
agonist. The principle of therapy is to cause inhibition of LH and FSH pituitary
secretion (medicamental ovariectomy). Sometimes in premenopausal women
ovarian suppression is added to standard chemohormonal therapy. In this review
two high-risk node positive premenopause breast cancer patients are presented,
diagnosed at the age of 38 and 28. Both had hormone receptors positive tumor and
underwent breast surgery followed by FEC regimen chemotherapy and
radiotherapy. Chemotherapy caused them temporary amenorrhoea, but soon
after radiotherapy and tamoxifen introduction regular menstrual cycle began. Due
to high-risk node positive cancer combined therapy with tamoxifen 20 mg daily
and goserelin 3,6 mg S.C. monthly was introduced. The first patient needed a three
months goserelin application to obtain amenorrhoea but the other patient needed
only one. After six months of goserelin plus tamoxifen therapy gynaecological
and endocrinological evaluation was preformed. In both patients LH value was
lower than 1.0 IJ/L but in the first one FSH, estradiole and progesterone values
were within menopausal ranges with ultrasound proof of ovarial and endometrial
inactivity. In the other patient FSH, estradiole and progesterone values were
within fertile range, with present ovary follicles, although ammenorrhoic. This
review refered that numerous individual factors influence the effect of adiuvant
LH-RH agonist therapy in high-risk breast cancer patient and that different time
period is needed to obtain its maximum effect.
Endocrine Abstracts (2007) Vol 14
Intra- and supra-sellar immature teratoma mimicking pediatric
Chentli Farida
Bab El Oued Hospital, Algiers, Algeria.
Immature teratoma arising from the brain is very rare. The intra and supra sellar
localization is very exceptional. Its clinical symptoms and radiological aspects on
TDM are similar to those of craniopharyngiomas but on MRI the fat signal
characterize teratomas, but only the histological exam gives the confirmation of
this last lesion and makes differential diagnosis with mature tumor whose
prognosis is better than the immature one. Our observation illustrates all these
LM, 6 years, female, is referred to our unit for craniopharyngioma. She
complaints of headaches, vomiting and a decrease in visual acuity. On
clinical exam we noted a blindness, diabetes insipidus and a statural deficit
with hypothyroidism wich are confirmed by hormonal results. On TDM
there is huge (60!32 mm) solid intra and supra sellar tumor with cysts and
calcifications wich arrives to the third ventricule but on MRI there is a fat
signal evocating a teratoma. histological exam of this very hemorrhage
tumor argue for an immature teratoma.
This observation prouves that clinical and TDM aspects of craniopharyngiomas are similar with those of teratomas. Only the fat signal on
the MRI argue for the teratoma. Histological exam is the only one
wich makes the proof and the differential diagnosis between craniopharyngioma and mature or immature teratoma. The last one has the worst
9th European Congress of Endocrinology, Budapest, Hungary, 2007
Pituitary microprocess
Chentli Farida
–Bab El Oued Hospital, Algiers, Algeria.
Nowadays neuro-radiological explorations are so frequent that radiologists
discover more and more pituitary lesions. In this work we would like to study
pituitary microlesions (PML: inferior or equal to 10 mm) in order to analyze age
and sex repartition, clinical symptoms leading to the diagnosis, position in the
pituitary area and the apparent etiologies.
All our patients are examined and hormonal exploration is as complete as
Among 85 subjects with PML proved by TDM and or MRI, there are 79 women
and 6 men (sex ratioZ13/1). Age at diagnosis Z30.8 years (14–73), most of them
are between 21 and 30 years old. The complaints are: Gonadal dysfunction Z
72%, galactorrhea Z10.5%, headaches Z5.8%, metabolic abnormalities Z6.7%
and visual troubles Z4.3%. The diagnosis is really fortuitous in 2 subjects Z
2.3%. For the apparent etiology there are 58 prolactinomas, 12 ACTH (19.2%), 10
non functioning (11.8%) and 5 somatotrop adenomas Z5.7%. The average size
Z6.45 mm (3–10). 58% are in right pituitary area, 23%, in the left and 13% in the
In our population the diagnosis of pituitary microlesions is rarely fortuitous.
Gonadal abnormalities are the most complaints. This may be explained by the
high frequency of female cases and secreting tumors. The diagnosis is relatively
late (mean size Z6.5 mm). PML are frequently located in the right area. ACTH
PML are the smallest and the GH one are the biggest
Adrenal incidentalomas and insulin sensitivity – are there any
differences between adenomas and hyperplasia?
Daniela Dudasova, Ivica Lazurova, Hedviga Wagnerova & Ingrid Dravecka
–Faculty of Medicine, P. J. Safarik University, Kosice, Slovakia.
It is well known that adrenal masses, particularly adenomas are frequently related
to metabolic syndrome and insulin resistance. However, there are no reported data
about the differences between adenomas and hyperplasia.
Authors examined the prevalence of symptoms of the metabolic syndrome and
insulin resistance in 25 patients with adrenal incidentalomas (10 men, 15 women)
of the mean age 57.9C15 years. 15 patients had adrenal adenoma determined by
CT or MR scan and 10 had unilateral or bilateral hyperplasia. The prevalence of
obesity was 72%, arterial hypertension 60%, diabetes mellitus or impaired
glucose tolerance 28%, hyperlipidemia 56% and hyperuricemia 20%, respectively, which is more frequent occurrence than that in normal human population.
Patients with adrenal adenomas had mildly but significantly higher body mass
index (BMI, P!0.05) and insulin resistance calculated as HOMA IR (P!0.05)
and FIRI (P!0.05) and significantly higher values of serum ferritin (P!0.01).
Plasma cortisol values were slightly but not significantly higher in the group with
adrenal adenomas.
Authors conclude that adrenal adenomas are probably more related to the
metabolic syndrome than adrenal hyperplasia.
Frequency of occurence of MEN1 syndrome in patients admitted with
primary hyperthyroidism
Agata Baldys-Waligorska, Grzegorz Sokolowski, Malgorzata Trofimiuk,
Filip Golkowski & Bohdan Huszno
Department of Endocrinology, Collegium Medicum of the Jagiellonian
University, Krakow, Poland.
Primary hyperparathyroidism (HPT) is the most common endocrinopathy in
MEN1 and usually its first clinical manifestation. Yet MEN1 is a rare disease,
representing only 2–4% of all cases of HTP. We studied the frequency of MEN1
syndrome in HPT patients admitted to our Department.
In a retrospective analysis of 84 suspected HPT patients hospitalized in 1999–
2006, case reports of 11 patients with suspected MEN1 were analysed. MEN1 was
stated if two of the three main MEN1-related endocrine tumours occurred.
HPT diagnosis was confirmed in 69 patients: of mean age 55.4G14.1 yrs. Median
values of PTH and total calcium concentration were 57.4 pg/ml (min – 60.6, max
– 1580) and 2.95 mmol/l (min – 2,2, max – 4,0), respectively. In parathyroid
scintigraphy equivocal tracer accumulation was found in 72% of cases. MEN1
was diagnosed in 9 patients of mean age 51.3G12,0 yrs, in 8 of whom (89.0%)
HPT was confirmed. Pituitary adenoma was found in 7 patients: 3 prolactinomas,
1 acromegaly, 1 Cushing disease and 2 non-functioning tumours. In 2 patients
pancreatic tumours were diagnosed: somatostatinoma and gastrinoma were
confirmed by laboratory tests and immunohistochemistry. Four carcinoids: 3
gastric and one bronchial were found. Mean 5-HIAA (5-hydroxyindoloacetic
acid) urine excretion in the carcinoid patients was 144.0 mmol/24hrs (norm: up to
40), mean serum concentration of CgA (chromogranin-A) 728.7 U/L (norm: up to
18.0). Moreover, in the patient with HPT and somatostatinoma concurrent von
Recklinghausen’s disease was diagnosed and in the HPT and prolactinoma
patient, meningioma was found. Adrenal tumours were observed in two cases:
one pheochromocytoma and one non-functioning tumour.
The frequency of MEN1 occurrence in our patients (13%) is much higher than
that quoted in the literature (2–4%), clearly, due to referral of complicated cases
to our Department. Patients with symptoms atypical for HPT should be screened
towards MEN1.
Evaluation of the efficacy of sandostatin LAR in the treatment of
Agata Baldys-Waligorska, Anna Krzentowska, Filip Golkowski &
Bohdan Huszno
Department of Endocrinology, Collegium Medicum of the Jagiellonian
University, Krakow, Poland.
Somatostatin analogues are used to treat acromegaly patients who, following
surgery, have not fulfilled cure criteria (hGH!2,5 ng/ml, IGF-1 below normal
range for age and post-OGTT hGH !1,0 ng/ml). We evaluated the efficacy of
Sandostatin LAR in managing such patients.
Material and method
In our Clinic, 81 acromegaly patients (mean age 51.6G14.4 yrs) were registered
over the years 1983-2005. Based on CT i MRI, macroadenoma and
microadenoma were stated in 63% and 37% of these patients, respectively. 70
patients (86.5%) underwent surgery, 6 (7.4%) refused surgery and 5 (6.1%)
underwent radiotherapy., Independently of time after surgery, 60 patients
underwent diagnostic tests to qualify them for Sandostatin LAR treatment.
Treatment efficacy was based on measuring concentration of hGH i IGF-1 3, 6, 9
and 12 months, and performing control MRI 6 and 12 months after the beginning
of Sandostatin LAR treatment (20 mg/month, increased to 30 mg/month if
Criteria of post-surgery cure were not fulfilled by 40 patients (66.6% of the 60
evaluated). Due to poor tolerance, one patient was treated with Pegvisomant. 19
patients (31.6%) required no further treatment. After 6 months of treatment,
hGH!2.5 ng/ml was stated in 63%, and IGF-1 below normal ranges for age in
58.8% of patients, and after 12 months – in 68.4% and 36.8% of patients,
respectively. In control MRI, recurrence, correlated with enhanced concentration
of IGF-1, was stated in 7 patients (17,5%).
In terms of hGH and IGF-1 levels, satisfactory acromegaly control was obtained
in about 40% of patients treated with Sandostatin LAR. This result may be biased
by the high number of macroadenoma, and possible non-radical surgery in our
patients. Due to evident disparity between 12-month normalization of hGH and of
IGF-1 levels, measurements of IGF-1 concentration are of considerable
diagnostic value in assessing the activity of acromegaly.
The beta-HLH transcription factor neurogenin-2 is preferentially
expressed by secreting pituitary adenomas
Amato Fratticci1, Fabio Grieco1, Cristina Spilioti1, Felice Giangaspero2,
Vincenzo Esposito2, Antonio Santoro3, Luca Ventura4, Edoardo Alesse1 &
Marie-Lise Jaffrain-Rea1
Experimental Medicine, University of L’Aquila, L’Aquila, Italy; 2Neuromed, IRCCS, Pozzili, Italy; 3Neurosurgery, University “La Sapienza”,
Rome, Italy; 4Pathology, S. Salvatore Hospital, L’Aquila, Italy.
Endocrine Abstracts (2007) Vol 14
9th European Congress of Endocrinology, Budapest, Hungary, 2007
Beta-HLH transcription factors are involved in the ontogenesis of neural/neuroendocrine cells, and may play a role in the pathogenesis of neuroendocrine
tumours. Neurogenin 2 (Ngn2) is expressed by the developing mouse pituitary.
After preliminary data indicating its expression in the normal human pituitary, we
have studied its phenotypic expression in normal and adenomatous pituitary
Fifty-two pituitary adenomas (PA) – 23 clinically non-secreting (CNS) and 29
clinically secreting (CS) (13 GH-, 8 PRL-, 6 ACTH- and 2 TSH-secreting PA,
respectively) - and 4 normal pituitaries (NP) were studied. Ngn2 transcripts were
determined by realtime qRT-PCR and compared to beta-actin transcripts, using
Taqman on-demand assays (Applied Biosystems). Immunohistochemistry was
performed on 21 PA and 2 NP, using a rabbit polyclonal antibody (Chemicon).
Mouse monoclonal antibodies for pituitary hormones (Dako) were used for
co-localization experiments.
Ngn2 transcripts were observed in all NP and 39/52 (75%) of PA, with a higher
frequency in CS versus CNS PA (89.6% vs 56.5%, c2Z7.51, PZ0.006).
Accordingly, Ngn2 levels were higher in CS than in CNS PA (PZ0.006, MannWhitney). Only a subset of PA (11/52Z21.1%) were found to moderately
overexpress Ngn2 as compared to NP: 8 were CS and 3 were CNS, including 2
silent-secreting PA. Nuclear immunopositivity for Ngn2 was detected in scattered
cells of the NP, co-localizing with most pituitary hormones, and in 17/21 PA
(14/15 CNS and 3/6 CNS, respectively). No significant correlation was found
between Ngn2 expression and tumour volume, invasiveness or Ki-67 labelling
Ngn2 is expressed by the NP and a significant subset of PA. Its preferential
expression by CS PA, the lack of significant overexpression or correlation with
tumour aggressiveness, suggest that Ngn2 may contribute to maintain a
differentiated secreting phenotype in PA but plays no role in pituitary
tumorigenesis itself.
The effect of SOM230 on cell proliferation and cortisol secretion in the
human adrenal carcinoma cell line H295R
Barbara Mariniello, Sara Cervato, Giuseppe Opocher, Nora Albiger,
Gianluca Occhi, Carla Scaroni & Franco Mantero
Division of Endocrinology, Department of Medical and Surgical Sciences,
University of Padova, Padova, Italy.
Adrenocortical carcinoma (AC) is a rare neoplasm with poor prognosis. Medical
treatment of AC is actually based on the use of op’DDD (mitotane) with or
without traditional chemotherapeutic agents. Only very few information are
available about the effectiveness of somatostatin analogs in AC. In human adrenal
gland the expression of all five somatostatin receptor (SSTR) subtypes was
previously demonstrated. A differential expression was shown in adrenal
adenomas and carcinomas.
SOM230 is a new somatostatin analog able to interact with SSTR type 5. The
effect of SOM230 on cell proliferation and hormone secretion was demonstrated
in corticotroph pituitary adenomas primary cultures, but no data are available on
adrenal gland.
The aim of the present study was to evaluate the effect of SOM230 on
H295R, a human cell line derived from adrenal carcinoma. Cell proliferation
was assessed by MTT-assay, whereas cortisol secretion was determined,
with and without forskolin stimulation, using a competitive chemiluminescence immunoassay. Moreover, SSTR expression profile study was
performed by RT-PCR.
SSTR 3, 4 and 5 were expressed in H295R cells, whereas no expression
of SSTR1 and 2 was shown instead. The effect of SOM230 on H295R was
determined in a 5 days treatment. A slight decrease of cell proliferation
(11.4%) was observed after 72 h of treatment with a high dose of SOM230
(10K5M). At the same high dose (10K5M) SOM230 significantly (P!0.05)
inhibits cortisol secretion already after 24 h. A lower concentration of the
drug (10K8M) is effective only after 72 h of treatment.
These preliminary data show that SOM230 seems to have an effect on
adrenal cell proliferation only at high dose, while a significant dose
dependent effect on suppression on cortisol release was observed at 72 h
also at low doses. Further studies are required to determine if SOM230
might be used for treatment of patients with AC.
TGFß1 signalling in human insulinomas compared with human islets.
Anastasiya Nabokikh1, Martin Bilban2, Wolfgang Gartner1, Greisa Vila1,
Bruno Niederle3, Jens Nielsen4, Christoph Zielinski5, Anton Luger1 &
Ludwig Wagner1
Medical University of Vienna, Department of Medicine III, Vienna,
Austria; 2Medical University of Vienna, Department of Medical and
Chemical Laboratory diagnostics, Vienna, Austria; 3Medical University of
Vienna, Department of Endocrine Surgery, Vienna, Austria; 4University of
Copenhagen, Department of Medical Biochemistry and Genetics, Copenhagen, Denmark; 5Medical University of Vienna, Department of Medicine I,
Vienna, Austria.
Insulinomas are thought to be the result of reduced ß-cell death and
hyperproliferation of this specific and highly differentiated cell type. Specific
growth- factors are responsible for inducing ß- cell replication and might
therefore be involved in insulinoma formation. Pluripotent islet progenitor
cells are thought to be located at pancreatic ducts, which can give rise to
novel islets as well as exocrine pancreas formation. TGFß1 signalling
disruption has been shown to result in premalignant ductal lesions in mouse
models as well as in humans.
The specific objective of this study was to evaluate the gene expression
profile of human insulinoma tumors compared with human islets. The gene
expression profile of three human insulinomas originating from different
individuals was compared to one islet donor. The comparative Affimetrix
gene chip analysis of 8000 spotted genes revealed 1102 upregulated (O
1.5x) and 210 downregulated (O1.5x) genes. The results revealed significant
differences in the expression of members of the TGFß signalling pathway.
Insulinomas contained reduced TGFß1 and TGFß-induced proteins, but
overexpressed TGFß receptors. These data were confirmed by quantitative
real-time PCR expanding the numbers of insulinomas to 7 and islets-donors
to 3. Our results suggest a novel important function of TGFß in
development of human insulinomas and cell growth regulation at the islet
of Langerhans. Furthermore they are in accordance with earlier data on the
exocrine counterpart, where impairment of TGFß signalling is documented
in ductal progenitor cells and premalignant ductal lesions leading to
pancreatic adenocarcinomas. Apparently, in the presence of aberrant TGFß
signalling, these unique pluripotent progenitor cells might be able to give
rise to both endocrine and exocrine neoplasias.
Endocrine Abstracts (2007) Vol 14
MEN2B – Two simultaneous cases of a rare syndrome
Ágnes Sallai, Éva Hosszú1, Péter Gergics2, Zsolt Tulassay2, Károly Rácz2 &
György Fekete1
Semmelweis University 2nd Dep. of Paediatrics, Budapest, Hungary;
Semmelweis University 2nd Dep. of Medicine, Budapest, Hungary.
A 17-year-old boy was referred to our Department. In his medical history Crohn’s
disease had been supposed because of abdominal pain and distention. He had
previously undergone minor surgery as having large tongue with neuromas and
hypertrophic gums. Due to his marfanoid appearance, arachnodactyly, massive
eyebrows and lips together with his medical history, multiple endocrine neoplasia
type 2B (MEN2B) was suspected, which is a very uncommon hereditary disease.
It consists of typical dysmorphia, mucosal neuromas, ganglioneuromatosis,
medullary thyroid carcinoma (MTC) and phaeocromocytoma, and the prognosis
depends on the presence of MTC.
Two weeks later a 10-year-old girl presented with a hard mass at her neck. She
had massive lips, neuromas on the tongue and solitary thyroid nodule. Thyroid
scan showed a cold nodule in the right lobe, and fine needle aspiration cytology
suggested MTC.
Genetic analysis was carried out in both patients and revealed a point
mutation at codon 918 (M918T) of the proto-oncogene RET. Adrenomedullary function tests showed normal levels of serum and urinary
fractionated catecholamines, however, high levels of plasma calcitonin
related to MTC. Imaging studies did not identify metastases. Both patients
underwent total thyroidectomy and lymph node dissection. Histological
examination verified MTC in the thyroids and in the lymph nodes, too.
After the operation the plasma calcitonin level of the girl decreased, but it
remained high in the boy, so PET-CT was performed to look for metastases.
These were found at his cervical region, therefore a reoperation was made
with a more extensive node dissection. Since the operations (2006) both
patients have been doing well.
Our conclusion is that whenever the M918T mutation of proto-oncogene
RET is found total thyroidectomy should be done right after the diagnosis,
or if possible within the first 6 months of life.
9th European Congress of Endocrinology, Budapest, Hungary, 2007
Prevalence of autonomous cortisol and aldosterone secretion in patients
with a single benign cortical adrenal adenoma after modification of the
diagnostic tests
George Piaditis1, Gregory Kaltsas1, Theodora Kounadi1, Athina Markou1,
Nikos Mazarakis1, Aggeliki Gouli1, Polyzois Makras1,
Dimitrios Papadogias1, Kostantina Dimitriou1, Alexandra Stathopoulou1,
Kostantinos Kossyvakis1, Ragkou Despoina1, Vamvakidis Kyriakos2,
George Zografos2, George Kontogiorgos3 & George Chrousos4
Department of Endocrinology & Diabetes Center, General Hospital of
Athens G. Gennimatas, Athens, Greece; 23rd Department of General
Surgery, General Hospital of Athens G. Gennimatas, Athens, Greece;
Department of Pathology, General Hospital of Athens G. Gennimatas,
Athens, Greece; 4First Department of Pediatrics, University of Athens
Medical School, Agia Sophia Children’s Hospital, Athens, Greece.
The normal cut-offs of screening and diagnostic tests for autonomous aldosterone
(AAS) and cortisol (ACS) secretion are poorly defined, mainly due to the
presence of adrenal adenomas among those who have served as controls and the
stimulating effect of ACTH on aldosterone secretion.
We investigated cortisol and aldosterone secretion in 151 patients with benign
cortical adrenal adenomas (BCAA) and in 119 healthy controls with a normal CT of
adrenals. Tests for AAS were performed before and after dexamethasone
suppression to eliminate the ACTH effect on aldosterone secretion. Performed
tests: 1. ACTH-test (250 mg ACTH 1-24, IV) for cortisol, plasma active renin (PRC),
aldosterone (PAC) and PAC/PRC ratios measurements at 0, 30 and 60 min. 2.
Classical saline infusion test (SIT, 2 liters NaCl 0.9%/4 h, IV) for PRC, PAC and
PAC/PRC ratios measurements, 3. LDDST (0.5 mg DEX/6hX24 h) for ACTH and
cortisol measurements. 4. A further saline infusion test (POST-DEX-SIT) 2 h after
the LDDST.
Using ROC analysis the POST-LDDST cortisol levels (26.90 nmol/L), as well as
the POST-DEX-SIT PAC (53.45 pmols/L) and POST-DEX-PAC/PRC
(6.18 pmols/L/mU/L) achieved a 100% sensitivity and specificity. Using these
new cut-offs the estimated prevalence of ACS and AAS among the BCAA-patients
was 61.58% and 33.74% respectively, whereas simultaneous AAS and ACS was
observed in 15.68% of the patients. Both systolic and diastolic blood pressure were
significantly correlated with POST-DEX-SIT PAC/PRC ratio (P!0.003 and P!
0.002 respectively) and PAC/PRC ratio at 60 min of ACTH-test (P!0.0003 and
!0.001 respectively) but not with the basal measurements.
With the newly defined normal cut-offs even mild forms of ACS and AAS
were identified. As a consequence the estimated prevalence of ACS and
AAS in BCAAs was found much higher than the reported previously,
whereas a high prevalence of simultaneous cortisol and aldosterone secretion
was identified for first time.
observed in the walls of intratumoral blood vessels and in the interstitial
tissue. Our data indicates that the expression of AT1 receptors is altered in
adrenal cancer and in pheochromocytomas. The expression of AT2
receptors, in turn, may be connected with the process of tumoral neoangiogenesis.
Bilateral adrenal incidentalomas: exploration of aberrant responses
and comparison with unilateral lesions
Eirini Vicha, Dimitra-Argyro Vassiliadi, Christos Avgoustis,
Theodossia Palouka & Stylianos Tsagarakis
Department of Endocrinology, Athens’ Polyclinic, Athens, Greece.
Aberrant hormone receptors have been demonstrated in macronodular adrenal
hyperplasia or, rarely, unilateral adenomas causing Cushing’s syndrome but their
prevalence in adrenal incidentalomas (AI) remains uncertain. Therefore we
evaluated patients with bilateral AI for evidence of abnormal response to
physiological stimuli. We also compared their biochemical characteristics with
those of patients with unilateral AI.
Assessment of adrenal function was performed in 93 patients (27 men, 66
women, mean age 59.2C/K12 years) with AI; 27 patients (29%) with bilateral
(Group A) and 66 patients with unilateral adenomas (Group B). Non-diabetic
patients (nZ68) underwent a 75g-OGTT. Eighteen patients of Group A were
submitted to a meal test and 15 to a posture test. The posture test was positive in
3/15 (20%) patients and the meal test in 1/18 (5.5%). The size of the largest
adenoma in Group A was significantly greater compared to Group B (3.1C/K1.1
vs. 2.3C/K1.1, PZ0.01). No significant difference regarding the mean levels of
UFC, ACTH, DHEAS and midnight cortisol existed between the groups. A
significantly greater proportion of Group B patients had fully suppressed cortisol
levels (!1mg/dl) post-LDDST (37.9% vs. 14.8% for Group A, PZ0.023). The
prevalence of diabetes and hypertension and mean glucose levels during OGTT
were similar among groups, but in Group B the HOMA-R was significantly higher
(2.74C/K1.3 vs. 1.89C/K0.78 PZ0.037) and the QUICKI and ISI-composite
indices significantly lower (0.33C/K0.03 vs. 0.35C/K0.03, PZ0.046 and
3.3C/K1.5 vs. 4.7C/K2, PZ0.016).
In conclusion, evidence for aberrant responses to physiological stimuli,
particularly to upright posture, is occasionally found in patients with bilateral AI.
Although there are no major biochemical differences between subjects presenting
with bilateral or unilateral lesions, bilateral lesions tend to be larger and are more
often associated with lack of dexamenthasone suppression whereas unilateral
adenomas are more related to increased insulin resistance.
Immunohistochemical detection of angiotensin receptors AT1 and AT2
in adrenal tumors
Marek Pawlikowski, Beata led & Katarzyna Winczyk
Department of Neuroendocrinology, Chair of Endocrinology, Medical
University of Lodz, Lodz, Poland.
Immunohistochemical detection of angiotensin receptors AT1 and AT2 in adrenal
Angiotensin II is well known to affect the adrenal cell growth and function.
Angiotensin receptors AT1 and AT2 were found to be present in the normal
adrenal gland. However, the data on the expression of angiotensin receptors in the
adrenal tumors is very scarce.
To overcome this gap, the paraffin sections of the adrenal cortical tumors
and of pheochromocytomas from the archival material were immunostained
with antibodies raised against AT1 (sc-1173) and AT2 (sc-9040) receptor
proteins. In hyperplasia of the adrenal cortex and in benign adrenocortical
adenomas, both functioning and non-functioning, the AT1 immunostaining
was present mainly in the cell membranes. A positive immunoreaction was
also found in a subpopulation of cell nuclei and within the cytoplasm. In the
adrenal cancer, as well as in pheochromocytomas neither cell membranes
nor cell nuclei were immunostained with anti-AT1 antibody. However, a
weak AT1 immunostaining was present within cytoplasm of the tumoral
cells. With anti-AT2 antibody, in all tumors investigated, the tumoral cells
were immunonegative but moderate to strong AT2 immunostaining was
Inhibitory effect of rosiglitazone – PPARgamma receptor ligand on
growth of human adrenocortical tumor cells in vitro
Katarzyna Winczyk, Hanna Lawnicka, Julita Fuss-Chmielewska,
Krzysztof Kolomecki, Jacek Kuroszczyk & Marek Pawlikowski
Department of Neuroendocrinology, Chair of Endocrinology, Medical
University of Lodz, Lodz, Poland.
The peroxisome proliferator-activated receptors gamma (PPARg) are nuclear
receptors which are detected in normal and pathological tissues. Our earlier study
showed the overexpression of PPARg in human adrenal tumors and pituitary
adenomas in comparison to normal glands. The in vitro experiments indicated that
ligands of PPARg inhibit growth of many tumors including pituitary adenomas,
thyroid cancers and adrenal carcinomas. However, the data concerning the effects
of PPARg ligands on adrenal tumors is very scarce.
In the present study, we investigated the action of PPARg ligands rosiglitazone on
growth of human adrenocortical tumors in vitro.
Materials and methods
Ten surgically removed adenomas (five non-functioning adenomas, four
aldosterone-secreting tumor and one cortisol-secreting adenoma) were examined.
The adrenal tumors cells were exposed in the primary culture to rosiglitazone at
the concentration of 10K3, 10-4 and 10K5 M for 24 hours. To measure cell growth
the modified colorimetric Mossman method detecting the viable cells was
applied. Moreover, the immunohistochemical evaluation of PPARg expression in
paraffin sections of adrenal tumors was performed. The study protocol was
approved by local Ethical Committee of Medical University of Lodz.
Endocrine Abstracts (2007) Vol 14
9th European Congress of Endocrinology, Budapest, Hungary, 2007
We have shown that rosiglitazone significantly inhibited the cell growth in 9 out
10 examined adrenal tumor in a dose-dependent manner. Rosiglitazone was the
most effective at concentration of 10K3 M. PPARg receptors were found in all
tissue, but the number of cells with positive immunoreaction was the lowest in
aldosterone-secreting adenoma, which was insensitive to rosiglitazone.
Our results suggest that rosiglitazone may be useful in the treatment of human
adrenocortical adenoma. However, the efficacy of PPARg ligands requires a
confirmation in study performed on the larger group of adrenal tumors.
The modern pre- and intraoperative diagnostic algorithm of pancreatic
NET with the use of 99mTc-EDDA/HYNIC-octreate scintigraphy – the
impact of SRS on patients’ management
Alicja Hubalewska-Dydejczyk1, Katarzyna Fröss-Baron1,
Renata Mikolajczak2, Bogdan Huszno1, Piotr Szybinski3, Jan Kulig3,
Aleksandra Januszewska1, Anna Sowa-Staszczak1 & Dorota Pach1
Chair and Department of Endocrinology, Medical College, Jagiellonian
University, Cracow, Poland; 2Radioisotope Centre POLATOM, OtwockSwierk, Poland; 3Gastrointestinal and General Surgery Department, Medical
College, Cracow, Poland.
Pancreatic NETs often cause difficulties in imaging diagnostics and optimal
diagnostic algorithm is searched for. According to the latest reports MDCT
sensitivity amounts 60-90%, MR: 80-90%, SRS: 62-100%, EUS: 70-90%.
Assessment of the usefulness of 99 mTc-EDDA/HYNIC-octreotae scintigraphy in
detection of primary and metastatic tumours of pancreatic NET in comparison to
CT, EUS and IOUS and evaluation of the impact of scintigraphic results on
clinical management of these patients.
Materials and methods
27 patients (aged 52.0G17.3 y) with suspected or histopathologically confirmed
pancreatic NET were qualified for the study. Imaging diagnostics was performed
in order to detect the primary lesions, local recurrences an metastases.
99 m
Tc-EDDA/HYNIC-octreotate SRS, CT, EUS and IOUS were performed.
The patients with positive SRS were qualified for RGS.
On the basis of the imaging methods results and histopathologic verification:
insulinoma- 8, glucagonoma-6, gastrinoma-5, somatostatinoma-2, NET with
ACTH ectopy-2, non-functioning NET- in 4 pts were finally diagnosed. Primary
lesions (16) and local recurrences (4) were revealed in 20pts, and metastases in
8pts. Sensitivity of SRS and CT was 85% vs 65% respectively. SRS visualized
metastatic lesion in 100%, while CT in 87.5% of pts. IOUS revealed the primary
tumours in all cases of insulinoma and gastrinoma (9/9). SRS and EUS detected
5/7 insulinoma and 2/2 gastrinoma (CT: 3 insulinomas, 1gastrinoma). SRS
changed the diagnostic approach in 13 pts: 8 were qualified for 90Y-DOTA-TATE
therapy and 2pts with negative SRS were referred for chemiotherapy. 2
insulinomas and glucagonoma liver metastases were visualised only in SRS
and detected with hand-held gamma-probe intra-operatively.
99 m
Tc-EDDA/HYNIC-octreotate SRS is a sensitive method of pancreatic NET
detection. It is particularly useful in visualisation of the small tumours of the
pancreatic tail and small liver metastases. It has essential impact on patients
treatment as it enables tumours’resection with RGS and selects patients for PRRT
with 90Y-DOTA-TATE.
Segregation of P25L and S80I mutations of the vhl gene in an extended
Hungarian family with von Hippel-Lindau syndrome
Attila Patócs1, Katalin Balogh1, Miklós Tóth1, Ferenc Fazakas2,
István Likó3 & Károly Rácz1
2nd Department of Medicine, Semmelweis University, Budapest, Hungary;
Department of Clinical Biochemistry and Molecular Pathology, University
of Debrecen, Debrecen, Hungary; 3Gedeon Richter LTD, Budapest,
von Hippel-Lindau syndrome (VHL) is a rare autosomal dominant disease caused
by alterations of the vhl tumor-suppressor gene. Patients with VHL are at risk for
development of retinal, central nervous system and spine hemangioblastomas,
Endocrine Abstracts (2007) Vol 14
clear-cell renal cell carcinomas, pheochromocytomas, endolymphatic sac tumors
and cysts; and pancreatic islet cell tumors. Based on the presence or absence of
pheochromocytoma as a phenotypic marker, VHL can be divided into different
subtypes. According to Knudson’s two-hit hypothesis, tumor formation in VHL
requires inactivation of both copies of the tumor suppressor vhl gene. Some
specific genotype-phenotype correlations have been recognized, but the majority
of families have their own specific genetic alteration.
To identify the disease-causing vhl gene mutation in a large Hungarian VHL
kindred and to study the genotype-phenotype correlations.
Patients and methods
32 family members spanning 5 generations were evaluated. Initial screening
included medical history, physical examination, abdominal ultrasonography,
abdominal and cranial CT or MRI, as well as ophthalmologic examination and
laboratory tests. Mutation analysis of the vhl gene was performed in DNA
samples obtained from peripheral blood. Written informed consent was obtained
from all family members who participated in the study.
Results and conclusions
Two genetic alterations of the vhl gene (P25L and S80I), both resulting in
an amino acid change were identified. The detailed medical examination
confirmed that VHL-specific tumors were associated with the presence of
S80I mutation. In three family members this mutation was associated with
the presence of pheochromocytoma. To our knowledge, the S80I mutation
has not been previously described in VHL patients who had pheochromocytoma. Therefore, this finding represents a novel genotype-phenotype
association. The P25L variant was identified in clinically healthy family
members, suggesting that this variant represents a sequence polymorphism
rather than a real disease-causing mutation.
High prevalence of novel mutations of the MEN1 gene in Hungarian
patients with multiple endocrine neoplasia type 1
Katalin Balogh1, László Hunyady2, Attila Patócs1, Peter Gergics1,
Zsuzsa Valkusz3, Miklós Tóth1, Ibolya Varga1, Edit Gláz1 & Károly Rácz1
2nd Department of Medicine, Semmelweis University, Budapest, Hungary;
Department of Physiology, Semmelweis University, Budapest, Hungary;
Division of Endocrinology, University of Szeged, Szeged, Hungary.
Multiple endocrine neoplasia type 1 (MEN 1) may present as a familial or a
sporadic disorder with multiple endocrine tumours including parathyroid
adenomas or hyperplasias, tumours of endocrine pancreatic and pituitary gland.
Familial and sporadic MEN 1-related states which do not fulfill current diagnostic
criteria but may be related to MEN 1 syndrome have been also described.
The aim of this study was to examine the prevalence and spectrum of MEN1 gene
mutations in Hungarian patients with familial and sporadic MEN 1 and in those
with an MEN 1-related state.
We performed mutation analysis using temporal temperature gradient gel
electrophoresis (TGGE) and direct sequencing of the entire coding and
exon-intron boundaries of the MEN1 gene. Genomic DNA was obtained
from 32 patients (19 index patients with familial or sporadic MEN 1 and 13
index patients with familial or sporadic MEN 1-related state). Family
screening was performed in families of patients with identified MEN1
Ten different MEN 1 gene mutations were identified in 10 index patients,
including 5 novel mutations (A91V, G28A and E26X in exon 2, L301R in
exon 6, and C354X in exon 8). All but one mutations occurred in index
patients with familial or sporadic MEN 1; the prevalence of mutation was
considerably higher in index patients with familial MEN 1 (6/6 patients,
100%) than in those with sporadic MEN 1 (3/13 patients, 23%). Of the 13
index patients with MEN 1-related state, only one patient with recurrent
isolated primary hyperparathyroidism had MEN1 gene mutation. Family
screening indicated mutations in 6 symptomatic and in one asymptomatic
first-degree relative.
These results confirm previous reports on the high prevalence of novel
MEN1 gene mutations among patient with MEN 1, and support the
questionable efficacy of mutation screening in patients with sporadic MEN
1-related states.
9th European Congress of Endocrinology, Budapest, Hungary, 2007
Analysis of germline mutations in patients with pheochromocytomas
and paragangliomas
Aleksandra Krawczyk1, Kornelia Hasse-Lazar1, Jacek Ziaja2,
Agnieszka Pawlaczek1, Jolanta Krajewska1, Mariola Peczkowska3,
Aleksander Preibisz3, Agata Kubaszek3, Andrzej Januszewicz3 &
Barbara Jarzab1
Department of Nuclear Medicine and Endocrine Oncology, MSC Memorial
Cancer Center and Institute of Oncology, Gliwice, Poland; 2Department of
General, Vascular and Transplant Surgery, Medical Silesian University,
Katowice, Poland; 3Department of Hypertension, National Institute of
Cardiology, Warsaw, Poland.
Cabergoline suppression test in distinguishing the variability of
response to dopamine agonists in prolactinomas
Corin BADIU2, Daniela VOICU4, Andra Caragheorgheopol1,
Dan Hortopan1 & Luigi Silvestro3
Institute of Endocrinology, Bucharest, Romania; 2C. Davila University of
Medicine and Pharmacy, Bucharest, Romania; 3Pharmaserv, Bucharest,
Romania; 4Medicover, Bucharest, Romania.
There are two types of neoplasms derived from chromaffine tissue:
pheochromocytomas (tumors of adrenal core) and paragangliomas (tumors
located extraadrenally). Majority of these tumors are sporadic, although
according to literature, when DNA analysis is carried out, hereditary disease
can be diagnosed in about 25% of patients: Multiple Endocrine Neoplasia
type 2 (MEN2A and MEN2B), von Hippel-Lindau Syndrome (VHL),
Pheochromocytoma/Paraganglioma Syndrome (PPS) and neurofibromatosis
type 1 (NF-1), caused by DNA germline mutations in RET protooncogene
and VHL, SDHB, SDHD, NF-1 genes respectively. The aim of our study is
evaluation of the frequency of hereditary chromaffine tissue neoplasms in
group of apparently sporadic patients, diagnosed and treated by our
cooperation. DNA was isolated from peripheral blood leukocytes. Analysis
of RET, SDHB and SDHD was carried out in order to seek for DNA
changes. DNA fragments were amplified with the use of the polymerase
chain reaction (PCR). Multiplex Single Strand Conformation Polymorphism
(MSSCP) analysis was used as the screening method. When a conformation
change was observed, it was confirmed by sequence analysis. The whole
analysis was completed in 63 patients. Germline mutations were found in 16
patients (25.5%); in the group with pheochromocytomas as the sole
manifestation in 14 patients (26.4%). Most frequent germiline mutations
in pheochromocytoma patients were mutations of RET: codon 634 (9
patients) and codon 791 (5 patients) and in paraganglioma patients –
mutation in SDHD codon 33.
Our analysis confirms the significant contribution of inherited disease to the
occurrence of apparently sporadic pheochromocytomas and paragangliomas.
Primary therapy in prolactinomas, the most frequent pituitary adenomas, consists
in ergot derivatives dopamine agonists (bromocriptine or cabergoline) which
lowers prolactin levels and shrink the tumour. Bromocriptine was the first drug
used, but the therapeutic levels are attained after several days/weeks, therefore an
acute suppression test is not possible. However, the biological response is variable
and 10% of prolactinomas are resistant to medical therapy. In order to evaluate the
degree of response to dopamine agonists, we tempted a short (48 h) cabergoline
(CAB) suppression test. Twenty-nine patients with hyperprolactinemia, 21
prolactinomas (14 women and 7 men), 2 GH-PRL secreting adenomas (2 women)
and 6 idiopathic hyperprolactinemia (5 women, 1 man), received a single
cabergoline dose (0.5 mg) and were sampled for PRL at baseline, 12 h, 24 h and
48 h after CAB administration. Simultaneously, CAB levels were determined by
mass spectrometry. Subsequently, patients were treated with Cab in doses up to
2 mg/twice a week. The final response to treatment was evaluated after
completion of 6 months of therapy. According to this the 21 prolactinomas
were divided into 13 sensitive and 8 resistant to dopamine agonists.
Mean PRL levels decreased from 384.37 ng/mL to 101.9 ng/ml at 12 h,
94.7 ng/mL at 24 h and 73.31 ng/ml at 48 h, in the senstitive group, and from
1508.37 ng/mL to 1060.34 ng/ml at 12 h, 755.33 ng/mL at 24 h and 600.84 ng/ml
at 48 h, in the resistant group. Average cabergoline levels were similar in both
groups. PRL decrease at 48 h as compared to baseline, was at 40% from basal
level in resistant and at 20% in responsive cases, P!0.005. In acromegalic
patients, co-secretion of PRL was suppressed at 65% basal level at 48 h, while in
functional hyperprolactinemia, normal values were attained at 48 h. Suppression
level was not influenced by the tumour size. In conclusion, cabergoline
suppression test could be used as early predictor of PRL suppression and
biological response in prolactinomas.
RET exon 13 germline polymorphism in patients with pheochromocytomas and paragangliomas
Kornelia Hasse-Lazar1, Agnieszka Pawlaczek1, Aleksandra Krawczyk1,
Malgorzata Wiench1, Malgorzata Oczko-Wojciechowska1,
Mariola Peczkowska2, Aleksander Preibisz2, Agata Kubaszek2,
Andrzej Januszewicz2, Jacek Ziaja3 & Barbara Jarzab1
MSC Memorial Cancer Center and Institute of Oncology, Department of
Nuclear Medicine and Endocrine Oncology, Gliwice, Poland;2Department
of Hypertension, National Institute of Cardiology, Warsaw, Poland;
Department of General, Vascular and Transplant Surgery, Medical Silesian
University, Katowice, Poland.
Germinal mutations in protooncogene RET are associated with the inherited
medullary thyroid carcinoma (MTC) which occurs as the sole manifestation of
disease (FMTC) or, more frequently, as the part of multiple endocrine neoplasia
(MEN2). The contribution of RET polymorphism to the occurrence of apparent
sporadic MTCs is controversial. In our previous study we have found out that the
frequency of RET 769 CTTOCTG polymorphism in patients with MTCs is not
significantly higher when compared to control group.
In the present study we analyzed RET 769 polymorphism in 61 patients with
apparent sporadic pheochromocytomas or paragangliomas, in whom known
germline RET mutations and SDHB/D mutations were excluded.
DNA was isolated from peripheral blood leukocytes. Polymorphism 769
CTTOCTG was found in 39 patients (59%). Its frequency was 56% in patients
with pheochromocytoma and 72.7% in the group of non functional paraganglioma. Simultaneously, its frequency was 23% in patients with true sporadic
MTC and 27% in the control group of healthy patients (P!0.05).
The protooncogene RET exon 13 polymorphism is associated with the occurrence
of apparent sporadic pheochromocytomas and paragangliomas
Predictive value of pituitary histology on clinical outcome in
acromegaly: a retrospective cohort study
Birgit Steffin1, Wolfgang Saeger2, Hans-Jürgen Quabbe3,
Stephan Petersenn4, Dieter K Ludecke5, Jürgen Honegger6,
Michael Buchfelder7 & Martin Reincke1
Medizinische Klinik Innenstadt, Klinikum der Universität, München,
Germany; 2Marienkrankenhaus, Hamburg, Germany; 3Deutsches Akromegalie-Register, Berlin, Germany; 4Universitätsklinikum, Essen, Germany;
Universitätsklinikum Eppendorf, Hamburg, Germany; 6Universitätsklinikum, Tübingen, Germany; 7Universität Erlangen-Nürnberg, Erlangen,
Immunohistochemistry is commonly performed on tumour specimen obtained
during transsphenoidal surgery, but its predictive value for clinical outcome is
largely unknown. The aim of this study was to compare clinical and biochemical
outcome characteristics after surgery with histological tumour properties. This was
achieved by matching data from the German Acromegaly Register with those of the
Pituitary Tumour Registry of the German pituitary working group. From 285 out of
1543 acromegalic patients of the German Acromegaly Register (145 f,140 m), data
on morphological properties analyzed by a single pathologist (W.S) in the
department of pathology, Marienkrankenhaus, Hamburg were available. Using
immunohisto-chemistry, the density of cytoplasmatic granules, pattern of hormone
expression and mitotic activity (Ki67) were analyzed. Tumours were stratified
according to growth hormone (GH) and prolactin expression and Ki67 index.
Clinical and biochemical parameters predicting disease outcome such as postsurgical GH and IGF-1 were analyzed. Control of acromegaly was defined as random
GH !2.5 mg/l and normal IGF-1. Results are presented as range, mean and SEM.
Before surgery, GH and IGF-1 concentration did not differ between patients with
sparsely (nZ93) and densely granulated (nZ145) adenomas. However, after
transsphenoidal surgery, patients with densely granulated adenomas had significantly higher GH (0–100, 5.4G1.14 vs 0–57, 2.98G0.917 mg/l, PZ0.03) and IGF1 (94–1963.522G14.81, vs.12–1002.456G36.38 ng/ml, PZ0.006) concentrations
compared to sparsely granulated adenomas. These patients had a lower rate of biochemical control (31% vs 54%, PZ0.01). Co-expression of prolactin was found in
14% of adenomas. This was associated with higher postsurgical GH and IGF-1 (GH
Endocrine Abstracts (2007) Vol 14
9th European Congress of Endocrinology, Budapest, Hungary, 2007
10.5G8.31 vs 3.3G1.23mg/l, IGF-1 437G149.01 vs 348G27.3 ng/ml) compared to
tumours not expressing prolactin. Ki67 staining (Ki67 index !1% vs O1%) did not
have impact on clinical and biochemical variables (PZn.s.). The granulation density
of GH producing adenomas is a useful parameter predicting patient’s biochemical
outcome in acromegaly.
Somatostatin receptor immunohistochemistry in neuroendocrine
tumors: a proposal of scoring system for clinical characterization and
therapy selection
Antongiulio Faggiano2, Marco Volante1, Maria Pia Brizzi1, Stefano La
Rosa3, Ida Rapa1, Anna Ferrero1, Anna De Chiara4, Luisella Righi1,
Carlo Capella3, Gaetano De Rosa4, Luigi Dogliotti1, Annamaria Colao2 &
Mauro Papotti1
Dept. of Clinical and Biological Sciences, San Luigi Hospital, University
of Turin, Orbassano, Turin, Italy; 2Dept. of Molecular and Clinical
Endocrinology and Oncology, “Federico II” University, Naples, Naples,
Italy; 3Section of Anatomic Pathology, Dept. of Human Morphology,
University of Insubria and Ospedale di Circolo, Varese, Varese, Italy; 4Dept.
of General Pathology, Medicine, Human Pathology, and Clinical Pathology,
“Federico II” University of Naples, Naples, Italy.
Typing somatostatin receptor (SSTR) expression in neuroendocrine tumors
(NETs) is of relevance to target an octreotide-based diagnostic approach and
treatment. The expanding use of immunohistochemistry to detect SSTR is to date
not paralleled by an accurate methodological setting and standardized
interpretation of the results.
A multicentric study was designed to compare SSTR immunohistochemical
expression with in vivo scintigraphic data and verify its usefulness in the clinical
management of NETs.
After methodological setting by testing different SSTR antibodies, 107 cases of
NETs with available OctreoScan data and pathological material (both surgical
and preoperative) were retrospectively analyzed for SSTR type 2A immunohistochemical expression, and the results combined in a four grade scoring system
(0 to 3) and compared with scintigraphic images and, whenever available, with
the clinical response to somatostatin analogue treatment.
Restricting “positive cases” to the presence of a membrane pattern of staining
(proposed scores 2 and 3), an overall SSTR type 2A immunohistochemistry/
OctreoScan agreement of 77% (Chi-square test P!0.0001) was reached. Lower
concordance ratios were detected in preoperative and metastatic tumor samples,
possibly as a consequence of SSTR expression heterogeneity. Pure cytoplasmic
staining showed poor correlation with OctreoScan images (54% concordance
rate). In a pilot series, SSTR type 2A immunohistochemistry correlated with
clinical response in 82% of 22 patients undergone to therapy with somatostatin
analogs on the basis of a positive OctreoScan uptake.
A standardized scoring system for SSTR type 2A immunohistochemistry is
proposed as a useful and reliable adjunct to OctreoScan in the clinical
management of NET patients. A membranous SSTR type 2A staining well
predicts clinical response to somatostatin analogue therapy and provides
additional information on receptor distribution into a given tumor tissue and
among primary and metastatic lesions.
Prevalence of primary aldosteronism among hypertensive patients
(preliminary results)
Joanna Matrozova, Sabina Zacharieva, Georgi Kirilov, Mihail Boyanov &
Vladimir Hristov
University Hospital of Endocrinology ‘Akad.Ivan Penchev’, Sofia, Bulgaria.
Until recently primary aldosteronism /PA/ was thought to be rare, accounting for no
more than 0.05–2% of the hypertensive patients. Studies published in the last decade
demonstrate that primary hyperaldosteronism is a much more common cause of
secondary hypertension than was previously thought, accounting for as many as 5%
to 25% of hypertensives in some series. For the present, there are no data concerning
the prevalence of PA in Bulgaria which determined the realization of the present
study. A total of 200 patients/126 females, 74 males/were studied until now,
including 160 patients, referred to the Clinical Center of Endocrinology and
Endocrine Abstracts (2007) Vol 14
Gerontology, 20 patients referred to the Endocrinology Clinic, Internal Medicine
Department, and 20 out-patients. The screening was effectuated using the
aldosterone to renin ratio. Blood samples for aldosterone (pmol/l) and PRA
(ng/ml/h) were taken under standardized sampling conditions and after correction of
antihypertensive medications. We used 750 pmol/l/ng/ml/h as a cut-off for the ratio
aldosterone/renin. The captopril test and the measurement of aldosterone in urine
were used for confirmatory testing. The diagnosis of PA was confirmed in 13 cases,
which suggests a prevalence of 6.5% among hypertensive patients. Adrenal
tomography was performed in all biochemically confirmed cases of PA. The
presence of different types of PA was as follows: 7 cases/54%/ of adrenal adenomas
and 6 cases /46%/ of idiopathic PA. Among the confirmed cases of PA 1
normokalaemic and 12 hypokalaemic patients were found. Our study confirms the
results obtained by other recent investigations for an increased prevalence of PA. In
contrast to other studies in our research work the cases of Conn’s adenoma are
predominant, as well as the hypokalaemic forms of PA.
Leptin modulates the growth of murine Colon 38 cancer and interferes
with the cytotoxic effect of fluorouracil in vitro
Gabriela Melen-Mucha & Hanna Lawnicka
Department of Immunoendocrinology, Chair of Endocrinology, Medical
University of Lodz, Lodz, Poland.
Epidemiological studies underline that obesity represents a significant risk factor for
development of several cancer among them colon cancer. Moreover, multiple recent
data indicate that some of adipose tissue-derived hormones may influence the growth
of malignant cells. Leptin, the product of the ob gene, is one of them. However,
research is still contradictory regarding the role of leptin in colon cancer.
The aim of our study was to examine the direct effect of leptin at various
concentrations (from 10K5 to 10K12 M) applied alone or jointly with fluorouracil
(the classical cytotoxic drug for colon cancer) at two concentrations (0.25 mg/ml and
2.5 mg/ml) on the growth of murine Colon 38 cancer cells in vitro.
Colon 38 cancer cells were preincubated in RPMI 1640 medium supplemented
with fetal calf serum for 24 hours. Then the cells were cultured for 72 hours in the
presence of various concentrations of the examined substances applied either alone
or jointly. The growth of Colon 38 cell line was assessed by the colorimetric
Mosmann method.
We have found that leptin increased the growth of murine Colon 38 cancer at the
concentrations of 10K6, 10K7 M and 10K10, 10K11, 10K12 M. Its stimulatory effect
was rather slight with enhancement of cancer growth by 8% to 15% as compared to
controls. Fluorouracil, at both concentrations (0.25 mg/ml and 2.5 mg/ml) inhibited
the growth of Colon 38 cancer up to 28% and 40% of controls, respectively. Leptin
did not modulate the cytotoxic effect of fluorouracil applied at higher concentration
(2.5 mg/ml) but unexpectedly it enhanced at the concentrations of 10K9 and 10K10 M
the cytotoxic effect of fluorouracil given at lower concentration (0.25 mg/ml).
These data indicate that leptin is involved in the regulation of colon cancer growth
and it may even enhance the cytotoxic effect of fluorouracil.
Grant No. 502-11-295 from the Medical University of Lodz.
Muscle mitochondrial function is impaired in patients with prior
Julia Szendrödi1, Elisabeth Zwettler2, Albrecht Ingo Schmid3,
Marek Chmelik3, Giovanni Pacini4, Gertrud Kacerovsky5,
Christoph Schnack6, Guntram Schernthaner6, Oswald Wagner7,
Klaus Klaushofer2 & Michael Roden5
Karl-Landsteiner Institute for Endocrinology and Metabolism, Vienna,
Austria; 2Dept. Intern. Med. 4 and Ludwig Boltzmann Institute for
Osteology, Hanusch Hospital, Vienna, Austria; 3MR Centre of Excellence,
Med. Univ. Vienna, Vienna, Austria; 4National Research Council, Padova,
Italy; 5Dept. Intern. Med. 1 and Karl-Landsteiner Institute for Endocrinology and Metabolism, Hanusch Hospital, Vienna, Austria; 6Dept.
Intern. Med. I, Rudolfstiftung Hospital, Vienna, Austria; 7Clinical Institute
of Medical and Chemical Laboratory Diagnostics, Medical University
Vienna, Vienna, Austria.
Acromegaly is amongst other symptoms associated with myopathy, alterations of
energy expenditure and insulin action which are mediated by growth hormone
(GH) and insulin-like growth factors (IGFs). It is unclear to which extent these
abnormalities remain after treatment. Thus, we examined glucose metabolism,
intracellular fat deposition and mitochondrial function in patients with prior
acromegaly (AM).
9th European Congress of Endocrinology, Budapest, Hungary, 2007
Six AM (4f/2 m, age: 49G10 years, body mass index, BMI: 27G3 kg/m2) with
an at least 7-years history of successful treatment and age-/BMI-matched healthy
volunteers (CON: 3f/3 m, 43G12 years, 26G4 kg/m2) were studied. Insulin
sensitivity (OGIS) and first-phase insulin secretion were assessed from the
frequently sampled OGTT (insulinogenic index, ISEC). Mitochondrial function
was assessed from ATP synthetic flux (fATP) during fasting using 31P magnetic
resonance spectroscopy (MRS) of calf muscle. Intracellular lipid contents of
tibialis anterior (IMCLt) and soleus muscles (IMCLs) as well as liver (HCL) were
measured with 1H MRS. The protocol was approved by the local institutional
ethics board.
IGF-1 did not differ between groups (AM: 177G88 ng/ml; CON: 145G51 ng/l).
Fasting plasma glucose was w16% higher in AM (99G8, CON: 85G6 mg/dl, P!
0.05), OGIS was comparable (395G74, CON: 415G14), but ISEC was w87% lower
in AM (0.9G0.9, CON: 6.7G4.3, P!0.05). fATP was w22% lower in AM (10.1G
1.5 vs. 12.9G2.4 mmol.lK1.minK1, P!0.05) and related positively to ISEC (rZ
0.687, P!0.01). IMCLt and IMCLs and HCL were not different different between
groups. IMCLs related negatively to insulin sensitivity (rZK0.745, PZ0.005).
Successfully treated acromegaly patients exhibit reduced insulin secretion and
muscle ATP synthesis despite normal insulin sensitivity. The impairment of
mitochondrial function could be explained by previous long-term GH/IGF exposure
and/or chronically increased plasma glucose concentrations resulting from impaired
ß cell function.
Diagnosis and treatment of the ACTH-secreting neuroendocrine
pancreatic tumors
Gilis-Januszewska Aleksandra, Hubalewska-Dydejczyk Alicja,
Trofimiuk Malgorzata, Pach Dorota, Szurkowska Magdalena, BuziakBereza Monika, Mazurek Elwira & Huszno Bohdan
Chair and Department of Endocrinology, Collegium Medicum, Jagiellonian
University, Krakow, Poland.
Neuroendocrine tumors secreting ACTH are a rare cause of Cushing’s syndrome.
Diagnostic and therapeutical difficiulties might be caused due to different clinical
picture of of neuroendocrine tumors.
Patients, diagnostic and therapeutic approach
During 2004–2005 2 female patients 32-years old AL and 67-years old ZS
were hospitalized in Endocrinology Department due to severe hypercorticism signs and symptoms. In both patients biochemical and functional tests
revealed ACTH-dependent Cushing syndrome due to ectopic secretion of
ACTH. In both patients ultrasonography and computed tomography revealed
not well defined pancreas region lesions and multiple hepatic metastases.
Tc-EDTA/HYNIC-Octreotate scinitigraphy showed the uptake of the
tracer in similar locations. Neuroendocrine cells were found in bioptic
examination. Due to the dissemination of the disease process and bad
clinical condition in both patients no surgical treatment could be performed.
Important clinical and biochemical improvement was noted after introduction of aminoglutethymide (AL, ZS) and long acting somatostatin analogue
(Sandostatin LAR) (AL).
The palliative chemotherapy with 5-FU was implemented in AL. Both patients
were approved for therapy with somatostatin analogue labeled with 90Y (90-Y
DOTA-Tate). Patient ZS after three series of 90Y (90-Y DOTA-Tate) was approved to
continous somatostatin analoque treatment; patient in relatively good condition
remains under Endocrinology Outpatient Department control (actually 12 month
after diagnosis). Unfortunately Patient AL before admission to the hospital, suddenly
died for massive pulmonary embolism.
Tc-EDTA/HYNIC-Octreotate scinitigraphy become an important localising
technique in neuroendocrine tumors diagnosis.
Somatostatin analoques and 90Y (90-Y DOTA-Tate) therapy seem to be
promising treatment methods in non-operative neuroendocrine tumor cases.
Novel mutations in genes encoding succinate dehydrogenase complex
subunits B (SDHB) and von Hippel-Lindau protein (VHL) in patients
with nonsyndromic pheochromocytoma
Jovana Vignjevic, Jelena Nikolic, Tatjana Isailovic, Katarina Mirkovic,
Milan Petakov, Jadranka Antic, Djuro Macut, Bojana Beleslin-Cokic,
Bojana Popovic, Ivana Bozic, Sanja Ognjanovic & Svetozar Damjanovic
Institute of Endocrinology, Diabetes&Metabolic Diseases, Clinical Center
of Serbia, Belgrade, Serbia.
Several susceptibility genes have been found to be associated with development
of pheochromocytoma (PHEO): RET, VHL, SDHB and SDHD. We investigate
the frequency of germ-line mutations in SDHB and VHL genes in patients with
apparently sporadic PHEO.
Material and methods
Fifty patients (38 women, mean age 42) with apparently sporadic adrenal and
extra-adrenal PHEO were screened. DNA was extracted from whole blood and
from paraffin embedded tumors using standard phenol-chloroform method. For
detection of SDHB and VHL mutations PCR method followed by direct
sequencing gene was used.
In 5/50 (10%) patients, five novel germ-line variants were identified: four
heterozygous germ-line mutations (nonsense: W218X; frameshift: c.661delG,
p.Asp221ThrfsX27; splicing:c.424-12delTCTT and missense: R116M) of the
SDHB gene and one heterozygous germ-line mutation (V84M) of the VHL gene.
In the patient with adrenal PHEO and heterozygous germ-line W218X mutation,
the same heterozygosity state in the tumor tissue was found. The patient with
c.661delG mutation was found to have extra-adrenal retroperitoneal malignant
PHEO. Family members were also tested and they are negative for the
mutation.The patient with c.424-12delTCTT is 12 years old boy with adrenal
PHEO. He inherited the mutation from his father who is clinically asymptomatic
for PHEO. The patient with V84M mutation was found to have adrenal PHEO.
His family history is negative and he doesn’t have any other tumors associated
with VHL syndrome.
Patients with SDHB mutations are in an increased risk for the development
of extra-adrenal and malignant PHEO. Our patient with extra-adrenal
disease needs careful follow-up, since he is in higher risk for the
development of metastases or novel adrenal/extra-adrenal PHEO. The
patient with VHL mutation (V84M) is apparently classified as 2C. Until
now genotipe/phenotipe correlation is not proven. This patient may develop
some other tumors than PHEO.
Evaluation of plasma and urinary metanephrines as well as serum
chromogranin A for the diagnosis of pheochromocytoma
Nicole Unger1, Christian Pitt2, Martin K Walz2, Klaus Mann1 &
Stephan Petersenn1
Division of Endocrinology, Medical Centre, Essen, Germany; 2Department
of Surgery and Centre of Minimally Invasive Surgery, Kliniken EssenMitte, Essen, Germany.
Adrenal pheochromocytomas are neoplasms characterized by catecholamine
excess. We recently reported on the diagnostic value of plasma metanephrines
measured by RIA for the diagnosis of pheochromocytoma. However, RIA may
not be used in many laboratories.
This study evaluated plasma and urinary metanephrines determined by a newly
available ELISA as well as serum chromogranin A (CgA) for the diagnosis of
pheochromocytoma. Spontaneous blood samples and 24h-urine samples were
collected in 154 subjects, including 24 histologically proven pheochromocytomas, 17 aldosterone-secreting and 21 cortisol-secreting adrenal adenomas, 30
nonfunctioning adrenal masses, 16 patients with essential hypertension and 42
healthy normotensive volunteers. Plasma and urinary metanephrine (MN) and
normetanephrine (NMN) as well as CgA were determined and putative thresholds
calculated by ROC analysis.
Plasma NMN showed highest sensitivity (89.5%) and specificity (98.3%)
using a threshold of 167 pg/ml, with lower sensitivity (85.7%) and
specificity (91.8%) for urinary NMN by a threshold of 318 mg/24 h. Plasma
and urinary MN demonstrated a much lower sensitivity (68.4% resp. 71.4%)
and specificity (90.0% resp. 77.6%) using a threshold of 26 pg/ml and
90 mg/24 h respectively. Analysis of the combination of plasma metanephrines revealed a sensitivity of 89.5% and a specificity of 90.0%.
Considering both urinary parameters demonstrated a slightly higher
sensitivity (92.9%) with lower specificity (77.6%). ROC analysis revealed
a threshold of 215pg/l for CgA with rather low sensitivity (73.9%) and
specificity (74.2%). A weak positive correlation was found between the
tumor size of pheochromocytomas and plasma MN (rZ0.53, P!Z0.05) as
well as CgA (rZ0.60, P!Z0.01).
In conclusion, plasma metanephrines measured by ELISA are convenient
and reliable parameters for the diagnosis of pheochromocytoma. In contrast,
CgA demonstrated poor sensitivity and specificity.
Endocrine Abstracts (2007) Vol 14
9th European Congress of Endocrinology, Budapest, Hungary, 2007
C-5-hydroxytryptophan PET scan in diagnosis of ectopic Cushing’s
syndrome from typical lung carcinoid: a case report
Djuro Macut1, Svetozar Damjanovic1, Jelica Bjekic2, Bojana Popovic1,
Ivana Bozic1, Milan Petakov1, Sanja Ognjanovic1, Tanja Isailovic1,
Miloje Joksomovic3, Radoslav Jakovic4, Jelena Mirkovic1 & Jelena Stojsic4
Institute of Endocrinology, Clinical Center of Serbia, Belgrade, Serbia;
Department of Endocrinology, CHC B. Kosa, Belgrade, Serbia; 3Institute
of Neurosurgery, Clinical Center of Serbia, Belgrade, Serbia; 4Department
of Thoracic Surgery, Clinical Center of Serbia, Belgrade, Serbia.
A 34-year-old woman was initially presented with clinical signs of Cushing’s
syndrome (CS). On endocrinological examination, a diagnosis of ACTH
dependent CS was established (serum cortisol: 08.00 h: 1245 nmol/l; 24.00 h:
275; plasma ACTH concentration 104 ng/l; inadequate cortisol suppresion on
LDDST (787) and suppresion to 318 following HDDST). A magnetic resonance
imaging (MRI) confirmed a microadenoma in the left part of the pituitary.
Ultrasound examination confirmed hyperplastic adrenals. Hypercortisolism
persisted after the transsphenoidal operation of the pituitary adenoma;
immunohistochemical staining was positive only on FSH and LH. Subsequently,
she developed ankle edema, hypokalemia and hormonal profile suggestive on
ectopic CS (plasma ACTH 171.9 and failure to suppress serum cortisol following
HDDST) confirmed by CRF and DDAVP test. Neuroendocrine origin of the
ectopic ACTH production was further suspected with elevated chromogranin A
(489.2 ng/ml). Normal levels of 5-HIAA and PTH were obtained. A genetical
analyses excluded mutation in menin. A subsequently repeated CT/MRI scans of
neck, thorax, abdomen and pelvis were negative. Scintigraphy with 111In-pentreotide did not show any accumulation of the tracer in the body. Whole-body
chateterization and sampling did not reveal an ectopic ACTH source. Positron
emission tomography (PET) using 11C-5-hydroxytryptophan (5-HTP) (Uppsala,
Sweden) showed increased tracer uptake in the retrocardial region of the left lung.
In meantime, octreotide in a dose of 900 mg/day s.c. was applied producing
complete normalizatioon of arterial blood pressure, restoration of menstrual
cyclicity, and complete normalization of cortisol and ACTH. She was
successfully operated 14 months after the onset of first signs of CS with
pathological confirmation of 11 mm typical lung carcinoid. We presented an
unusual case of ectopic CS produced from the typical lung carcinoid that was
detected only by means of 5-HTP PET, and associated with coincidentally
diagnosed gonadotroph pituitary adenoma.
pituitary tumor and he is at high risk for developing other MEN1 manifestations.
Identification of an MEN1 mutation allows genetic testing for family members
who are at risk for developing disease. Only mutation-carriers among family
members need careful follow-up for the clinical manifestations of MEN1
Screening for mutations in exon 10, 11, 13 and 14 of the RET
protooncogene associated with inherited medullary thiroid carcinoma
(MTC) in Serbian population
Jelena Nikolic, Jovana Vignjevic, Katarina Mirkovic, Bojana BeleslinCokic, Jadranka Antic, Tatjana Isailovic, Milan Petakov &
Svetozar Damjanovic
Institute of endocrinology, Clinical Center of Serbia, Belgrade, Serbia.
Ret protooncogene germ-line mutations are associated with the inherited multiple
endocrine neoplasia type 2 syndromes (MEN2a and MEN2b) and also with
familial medullary thyroid carcinoma (FMTC). In this study, we report a large
scale of mutations in exon 10, 11, 13 and 14 RET protoocogene in patients from
Serbia. Our study included patients with MTC.
Our study included 180 patients. Patients were tested for RET protooncogene
mutations in exons 10, 11, 13 and 14 by polymerase chain reaction (PCR)
followed by restriction fragment length polymorphism (RFLP) and sequencing
analyses. Sequencing analysis was performed on ALFexpress II using Thermo
Sequence CY5 Terminator Cycle Sequencing Kit and Applied Biosystem Genetic
Analyzer 3130 using Big Dye Sequencing Kit.
In 41/180 (23%) patients 7 different heterozygous germ-line mutations were
identified: (C634Y, C634R, C634F, C634W in exon 11; C618Y in exon 10;
Y791F in exon 13; and V804M in exon 14). Prophylactic thyroidectomy was
performed in 6 C634R germline mutation carriers. Interestingly in one family
with Y791F mutation MEN 2a was found while in other three components of
brachi-oto-remal syndrome were found without MTC. Two patients with V804M
had MTC.
Base on these data in Serbian population we found similar frequencies of
inherited medullary thyroid carcinoma as in other European countries.
Mutational analysis in patients with nonsyndromic MEN1
Katarina Mirkovic, Bojana Beleslin-Cokic, Jovana Vignjevic,
Jelena Nikolic, Jadranka Antic, Bojana Popovic, Tatjana Isailovic,
Ivana Bozic, Milan Petakov, Djuro Macut, Sanja Ognjanovic &
Svetozar Damjanovic
Institute of endocrinology, Clinical Center of Serbia, Belgrade, Serbia.
Mutational screening of the MEN1 gene has been recommended for patients who
fulfill clinical criteria for familial or sporadic MEN1 and those suspicious or
atypical of MEN1.
Patients and methods
Eighteen apparently unrelated individuals (6 males; 12 females, age range 16–71)
with clinical manifestations of MEN1 were analised. In addition, we evaluated 7
relatives. Genomic DNA from peripheral blood leucocytes was extracted using
standard procedures. PCR amplification followed by bidirectional sequencing of
the entire coding region and exon-intron boundaries of the MEN1 gene was used
to detect mutations.
In 9/18 (50%) of the index cases we identified 9 independent germline MEN1
mutations: 3 nonsense (R527X, Y77X, Y341X), 3 frameshift (c.1089delT,
c.865del4, c.960delG), 2 missense (H317Y, G225V) and one splice-site mutation
(IVS4-1GOA). Three mutations were not previously reported. In addition, we
detected 3 benign polymorphisms: S145S, R171Q and D418D. The patient with
c.865del4 mutation was presented with insulinoma and primary hyperparathyroidism. This mutation is in exon 4 of the MEN1 gene and is predicted to cause
truncation of the protein after 28 amino-acids (p.Asp252AspfsX28). Frameshift deletion c.960delG is located in exon 6 and creates stop codon after three aminoacids (p. A263GfsX3). Patient in whom we detected this mutation had pituitary
tumor and primary hyperparathyroidism. Third novel mutation, G225V, is located
in exon 4 of the MEN1 gene. This patient had hyperparathyroidism, carcinoid and
adrenal gland tumor. Four out of seven relatives were found to be a mutation
carriers. Patient with Y341X mutation is sixteen years old boy with mixed
Endocrine Abstracts (2007) Vol 14
The use of 18F-FDG PET/CT with or without rhTSH stimulation during
follow-up of patients with differentiated thyroid carcinoma
Gelsy Arianna Lupoli1, Annalisa Panico1, Sara Colarusso1,
Francesco Fonderico1, Antonio Gonnella1, Maria Rita Poggiano1,
Luigi Pucci1, Addolorata Martinelli1, Emanuele Nicolai2, Marco Salvatore2
& Giovanni Lupoli1
Department of Molecular and Clinical Endocrinology and Oncology –
University ‘Federico’, Naples, Italy; 2Department of Functional and
Biomorphological Sciences – University ‘Federico II’, Naples, Italy.
Fluorine-18 fluorodeoxyglucose positron emission tomography (FDG-PET) is a
new method employed in the management of differentiated thyroid cancer (DTC).
The integrated FDG-PET plus computed tomography (PET/CT) fusion imaging
system seems able to provide some additional advantages over PET alone, mainly
related to a better anatomical localisation of the hypermetabolic metastatic
lesions. The influence of serum TSH levels on 18F-FDG uptake by recurrences or
metastases of DTC has not been clarified yet.
To evaluate the clinical use of PET/CT during the follow-up of patients with
DTC; moreover, to ascertain whether the administration of recombinant human
thyrotropin (rhTSH) can increase the sensibility and specificity of PET/CT.
Patients and methods
We selected 12 pts with positive or equivocal thyroglobulin (Tg) levels and
negative or equivocal 131I scintigraphy and/or conventional morphological
imaging techniques (ultrasound, MRI, etc); they underwent 18F-FDG PET/CT
during TSH suppression (!0.05 IU/L) and after rhTSH administration (O
30 IU/L).
9th European Congress of Endocrinology, Budapest, Hungary, 2007
For 4 pts both basal and rhTSH-stimulated PET/CT scans were positive: in 3 cases
tumour foci were detected (confirmed also by histology in 2 cases) whereas 1 of
them was false positive results (due to lymph nodes inflammation). PET/CT was
completely negative in 8 pts: 6 results were true negative while 2 were false
negative, since scanning following rhTSH identified metastatic lesions.
Therefore, PET/CT was able to identify the metastatic foci very efficiently and to
localise previously unknown tumour relapse; moreover, in 2 out of 12 patients,
rhTSH administration resulted in detection of new lesions.
Our data confirm that PET/CT is a valuable tool in detecting residual disease in
DTC patients and suggest a potential role for rhTSH in enhancing the diagnostic
accuracy of this method
Abstract unavailable
Growth and development – presented on Sunday
Lower catch-up growth under rGH therapy at pre-pubertal pituitary
dwarves diagnosed at an older age
Dumitru Branisteanu, Corina Galesanu, Cristina Cristea, Eusebie Zbranca,
Carmen Vulpoi, Cristina Preda & Voichita Mogos
University of Medicine and Pharmacy ‘Gr.T.Popa’, Iasi, Romania.
Growth hormone deficiency leads to profoundly decreased growth velocity and,
when untreated, to pituitary dwarfism. We evaluated growth evolution for one to
four years under rGH therapy (0.07 IU/kg/day, subcutaneously) at seventeen
idiopathic pituitary dwarves with isolated GH deficiency, 13 boys and 4 girls, with
a wide span of age at therapy onset (between 4 and 24 years old). Diagnosis was
set subsequent to at least two negative GH stimulation tests. All patients were prepubertal, with a bone age below 13 years (Grunlich and Pyle Atlas) but had
normal thyroid and adrenal function. Patients were divided into two subgroups:
early-diagnosed patients (12 patients younger than 14 at therapy onset) and latediagnosed patients (5 patients, diagnosed at a chronological age of over 16 years).
Growth velocity was significantly increased in the entire group, from 0.33C/K
0.07 cm/month before therapy onset to 0.8C/K0.05 cm/month for the whole
follow-up period (P!0.0005). Catch-up growth was maximal during the first year
of therapy, with a velocity of 1.04C/K0.16 cm/month, which decreased
subsequently. Both mean growth velocities for the whole follow-up period
(0.99C/K0.08 vs 0.5C/K0.06 cm/month) and for the first year of therapy
(1.33C/K0.13 vs 0.61C/K0.09 cm/month) were significantly higher at the
early-diagnosed patients (P!0.01), despite present radiographic growth
potential. Early therapy onset in isolated GH deficiency is therefore important
not only because patients have a smaller height handicap to recuperate in order to
enter the normal growth channel, but also – as our data suggest - because growth
cartilage seems to loose with age its reaction potential to GH administration in
pre-pubertal patients. Our data show, nevertheless, that high-dose rGH therapy is
still beneficial in older pre-pubertal GH deficient patients by significantly
accelerating growth speed. GH dosage should be diminished to adult substitutive
levels and puberty should be triggered therapeutically once growth ceases.
The growth hormone – insulin-like growth factor-I axis in adult
thalassemic patients
Leila Danesi1, Agnese Cattaneo1, Elena Valassi1, Massimo Scacchi1,
Emanuela D’Angelo2, Nadia Mirra2, Laura Zanaboni3, Maria
Domenica Cappellini3 & Francesco Cavagnini3
Chair of Endocrinology, University of Milan, Ospedale San Luca IRCCS,
Istituto Auxologico Italiano, Milan, Italy; 22nd Pediatric Clinic, University
of Milan, Fondazione Policlinico Mangiagalli Regina Elena, Milan, Italy;
Department of Internal Medicine, University of Milan, Milan, Italy.
GH deficiency (GHD) can be recognized in a not negligible proportion of
thalassemic children, while data on the prevalence of this disorder in adult
patients are lacking. Therefore, we elected to study the GH – IGF-I axis in a large
group of adult thalassemic subjects.
Study design
Ninety-four patients (69 with thalassemia major and 25 with thalassemia
intermedia on stable transfusional regimen, 39 men and 55 women, aged 31.5G
6.8 years, receiving sex steroid replacement when necessary) underwent a GHRH
(1 mg/kg as an i.v. bolus)Carginine (0.5 g/kg as a 30 min i.v. infusion) test.
Severe GHD was defined by GH peaks lower than 9 mg/l, whereas partial GHD
was defined by GH peaks ranging from 9 to 16.5 mg/l. Blood samples for IGF-I,
ferritin and pseudocholinesterase measurement were also performed.
Severe GHD was demonstrated in 21/94 patients (22.3%), while 18 additional
patients (19.1%) displayed partial GHD. No correlations were found between
ferritin levels on one side and GH peaks and IGF-I SDS on the other side. GH
peaks were positively correlated with IGF-I SDS (P!0.05), although 1 of the 21
patients with severe GHD showed normal IGF-I SDS values, and 45 of the 55
patients with normal GH reserve displayed low IGF-I SDS. A strong positive
correlation (P!0.0001) between IGF-I SDS and pseudocholinesterase was
a) This study has demonstrated a high prevalence of GHD, either partial or severe,
in adult thalassemic patients. b) The lack of correlation between ferritin and both
GH peaks and IGF-I SDS suggests that mechanisms other than iron overload play
a major role in the pathophysiology of somatotropin-somatomedin deficiency in
this clinical condition. c) The finding of a positive correlation between IGF-I SDS
on one side and GH peaks and pseudocholinesterase values on the other side
indicates that liver protidosynthetic activity, in addition to somatotropin secretory
status, is a major determinant of IGF-I production in thalassemia.
The role of BMP-3B in the establishment of zona glomerulosa in the
adrenal gland
Artem Bakmanidis & Peter King
William Harvey Research Institute, London, United Kingdom.
The adrenal gland is composed of the medulla and the cortex, which is further
subdivided into three zones: zona glomerulosa (zG), zona fasciculata (zF) and
zona reticularis (zR). The zones of the cortex are functionally characterised by
their ability to synthesise different steroids and consequently they express
different steroidogenic enzymes. These and other markers of the zones have been
described but so far no good candidate for a determining factor of zonal
establishment has been discovered. Bone morphogenetic proteins (BMPs) are
multifunctional cytokines belonging to the transforming growth factor-b (TGF-b)
superfamily. In a microarray analysis of transcripts from the rat adrenal zG and
zF, we have discovered that some BMPs are potentially ZG specific and BMP-3B
showed exclusive expression in zG by Real-Time PCR and immunohistochemistry. Adrenal H295R cells (human adrenocorticocarcinoma cell line) were used
as an in-vitro model to examine the role of BMP-3B further. The cells were
differentiated into a zG (by Angiotensin II) and zF (by Forskolin) phenotype in the
presence and absence of exogenous BMP-3B protein. BMP-3B was able to drive
the differentiation of H295R cells into a more zG phenotype while inhibiting the
differentiation into a zF phenotype as judged by the inhibition of CYP11B1
expression and the promotion of CYP1B2 expression respectively. The effect of
BMP-3B on differentiation was confirmed by over-expressing BMP-3B in stable
cell lines and blocking endogenous BMP-3B by siRNA. These experiments imply
a role for BMP-3B in steroidogenesis and by implication in adrenal zonation.
Selenium supply modulates growth spurt of selenoprotein P knockout
Kostja Renko, Marten Michaelis, Ulrich Schweizer, Josef Köhrle &
Lutz Schomburg
Institut für Experimentelle Endokrinologie, Charité Universitätsmedizin
Berlin, Berlin, Germany.
Selenoproteins are playing an important role in body homeostasis and
development. They control thyroid hormone metabolism and are of prime
importance for intracellular redox regulation and cellular defence. The SePP
knockout mouse (SePP-KO) is a model of impaired Se metabolism characterized
by a disrupted distribution system for organified Se. One of the major phenotypes
of the homozygote SePP-KO mice is a reduced increase in size and weight during
the growth spurt that can dose-dependently be rescued by Se supplementation.
Endocrine Abstracts (2007) Vol 14
9th European Congress of Endocrinology, Budapest, Hungary, 2007
Se has an effect on the growth hormone axis and affects bone metabolism by
modifying either growth signal synthesis or the response of target tissues.
Materials and methods
Male and female wild-type, heterozygous and homozygous SePP-KO mice were
raised on regular rodent chow. At the age of 35 days, we studied the expression of
growth-relevant genes in target tissues by realtime-PCR and Nothern blot analysis.
Serum markers like IGF-1 and Leptin were determined by multiplex ELISA technique.
On commercial diets with Se-contents not specified, we identified disarrangements in
the IGF- and IGFBP-mRNA expression levels, which appeared inconclusive. On
diets with defined Se content, male SePP-KO mice had a body weight of 11.3 g (G
0.4 g) at P35 compared to 14.8 g (G0.6 g) in heterozygous or wild-type mice (P!
0.001). The diets revealed a narrow window between rescue (above 0.24 ppm Se) and
lethal progression of the phenotype (below 0.15 ppm). These findings now result in a
well-defined model to study the impact of Se on growth and body mass.
Se metabolism, Se status and Se transport have an important impact on growth and
body mass. Different SePP expression levels modify growth and development in
transgenic SePP-KO mice. Together with specific diets this mouse model offers an
ideal way to study the interaction of Se supply and growth hormone axis.
Factors affecting height velocity (HV) during GnRH analog therapy in
girls with central precocious puberty (CPP)
Dimitrios Thomas1, Elpis Vlachopapadopoulou1, Feneli Karachaliou1,
Eirini Vourliotaki1, Philippos Kaldrimides2 & Stefanos Michalakos1
Dept. of Growth and Development, Children’s Hosp. “P. & A. Kyriakou”,
Athens, Greece; 2Dept. of Endocrinology and Metabolism, “Metaxa”
Memorial Anticancer Research Hospital, Piraeus, Greece.
To assess factors affecting HV during triptorelin suppression treatment for CPP.
Materials and methods
Forty-six girls with CPP, with mean age at diagnosis 8.4 yrs who presented with
signs and symptoms of puberty before the age of 8 years and were treated with
triptorelin for at least 2 years, were studied. All girls were categorized into three
groups according to the difference between bone age (BA) and chronological age
(DBA-CA): group I with DBA-CA!11.99 months, group II with DBA-CA
between 12 and 23.99 months and group III with DBA-CAO24 months.
Furthermore, girls were categorized in two groups: girls with BA before treatment
initiation %10 years and girls with BA O10 years. Four groups were formed
according to Tanner breast staging: group A,B,C,D with breasts TII, TII-III, TIII
and TIII-IV respectively.
A statistically significant difference in mean HV during the 2nd year of treatment was
observed between group I (5.99G2.21), group II (3.87G1.46) and group III (3.09G
1.47) (PZ0.012, AN.O.VA). Mean HV during the 2nd year of treatment was
statistically higher in girls with BA before treatment %10 years (5.78G1.75)
compared to girls with BA before treatment O10 years (3.17G1.27) (PZ0.0001,
t-test). A statistically significant difference in mean HV during the 1st year of
treatment was observed between group A (6.32G0.96), group B (5.56G0.97), group
C (4.96G1.07), and group D (4.26G1.66) (PZ0.05, Kruskal-Wallis AN.O.VA).
HV during the second year of treatment could be statistically predicted using bone
age (PZ0.002) and weight (PZ0.036) before treatment initiation as independent
factors in multivariate linear regression model, according to the following equation:
HV2nd yearZ15,026K0,702X(BA)-0,0892X(W).
Bone age, Tanner breast stage and weight seem to be important factors affecting
HV during triptorelin therapy for CPP.
Auxological and IGF system parameters in African in comparison with
western countries normal children
Mara Boschetti1, Sabrina Piredda1, Marilena Sidoti1, Eliana Di Battista2,
Daniela Larizza3, Diego Ferone1, Antonina Barreca1 & Francesco Minuto1
Department of Endocrinology and Metabolism and Center of Excellence
for Biomedical Research, University of Genova, Italy; 2Department of
Pediatrics, Ospedale Gaslini, University of Genova, Italy; 3Department of
Pediatric Sciences and IRCCS Policlinico San Matteo, University of Pavia,
Endocrine Abstracts (2007) Vol 14
Growth is an integrated process, resulting from the response of cells to nutrient
availability and to hormonal status. Nutrients, in turn, are important regulators of
IGF-IGFBP system which are critical regulators of growth. Genetic factors seem
to be very important determinant of final stature in countries with high quality of
life at variance with underprivileged countries where food intake deficiency is
critical. The aim of our study was to evaluate the influence of environmental
conditions on IGF-I secretion and the role of GH-IGF-I system on the
generational trend of stature in a selected population of children living in
conditions of low dietary intake. We analyzed the auxological parameters and the
circulating levels of the different components of the GH-IGF system in 38 normal
African children from Ivorian Coast (NA) and 50 normal age and sex-matched
Italian children (NE). The results of this study showed that in Africans the levels
of all components of the circulating 150 kDa ternary complex (IGF-I, IGFBP-3,
ALS) were significantly lower as compared with Italians (P!0.001). However,
molar ALS/IGF-I, ALS/IGFBP-3, and IGF-I/IGFBP-3 ratios in African children
were comparable with those found in Italians.
Clinical and auxological data of children (MeanGStandard error)
BMI sds
In conclusion the levels of IGF ternary complex parameters are maintained
higher in Italian than in African children by the higher dietary intake but the molar
ratios and the stature were similar in both groups. It seems therefore that an
optimal concentration of total IGF-I contributes to the improvement of final
stature in generational trend.
X-linked neuronal T3 transport defect: Allan Herndon Dudley
Tabinda Dugal1, Assunta Albanese2 & Muriel Mc Entagart3
St Georges Hospital, London, United Kingdom; 2St Georges Hospital,
London, United Kingdom; 3St Georges Hospital, London, United Kingdom.
Thyroid hormone is absolutely necessary for early brain development.Incidence
of thyroid disorders in infancy is 1:4,000.Thyroid hormones can be deficient
through hormone synthesis and action or very rarely through defective transport.
Some new and exciting transporters for tri-iodothyronine (T3) have recently come
to light.MCT 8 gene encodes the protein that transports T3 into neurons. Its
mutation result in inability of T3 to enter a developing brain neuron. This leads to
peripheral elevation of T3 and TSH and low levels of T4. Clinically this causes a
spectrum of neurological features known as Allan-Herndon-Dudley syndrome
(AHDS).This X-linked mental retardation syndrome was described first in 1944.
We report a case of a male child born in 2002 with intrauterine growth
retardation (IUGR).He was diagnosed with cerebral palsy with supportive MRI
scan. His hypotonia, poor feeding and delayed milestones were attributed to
this,although the phenotypic features of AHDS ie elongated facies, bifrontal
narrowing,flat ears were also present.He had severe cognitive impairment and was
not walking at 42 months. He continued to be hypotonic with athetoid
movements. He was under a paediatric neurologist till his raised T3 and TSH
levels were noted.He was then transferred to endocrinologist. The diagnosis of
AHDS was on genetic studies.Thyroxin treatment has normalised his T4 and
TSH.T3 remains elevated.
Thyroid hormone replacement does not correct any neurological deficits.Therefore ante-natal diagnosis is important.This case is unique as the mother
was a mosaic carrier with no family history.Several families have been
described in literature with affected male relatives. Largest series of 6
(Schwartz et al. 2005).It is important to recognise the defect early to plan
counselling.Sex selection can also be offered for next pregnancy. Females
have 1:2 chance of being a carrier while males have a 1:2 chance of
inheriting the defective gene.
9th European Congress of Endocrinology, Budapest, Hungary, 2007
Cephalometric analysis and dental maturation in patients with Turner’s
syndrome (TS)
Rafaella Shimada Gomes, Darwin Luiz Martins Oliveira, João
Carlos Ramos-Dias, Alcinda Aranha Nigri, Reinaldo José Gianini, Sérgio
Yassuo Nonoyama & Maria Helena Senger
Faculdade de Medicina de Sorocaba - PUC/SP, Sorocaba, São Paulo, Brazil.
Craniofacial proportions of girls with TS, compared to normal children, show
reduced size of the craniofacial complex, retrognathic profile and tendency towards
advanced dental age. Growth hormone (GH) treatment in TS positively affects
stature, but its effects on craniofacial growth and dental development are largely
unknown. The aim of this study was to analyze and to correlate the craniofacial
morphology, chronological, dental and bone ages of TS patients receiving GH or not.
After the study was approved by the local Ethics Committee, we evaluated 21
cephalometric measurements (lateral cephalograms), dental age (DA) (panoramic
radiograph), bone age (BA) (left hand-wrist radiograph) and stature Z-escore in 22
TS patients (9 monosomy X; 10 mosaicism; 3 structural abnormalities of the X
chromosome). The GH treatment lasted from 0 to 6.8 yr. The median chronological
age (CA) was 16G3.4 yr (GS.D.). The variations for BA and DA were 6.8 yr to 17 yr
and 6 yr to 17 yr, respectively. Stature Z-escore was K2.33G1.8 (meanGS.D.).
Statistics were performed using the principal component analysis, simple linear
regression and Pearson correlation coefficient. P values !0.05 were considered
significant. Face height and mandibular length were the most affected measures and
showed correlations with BA, CA and GH treatment duration (P!0.05).
Cytogenetic status did not influence face alterations. CA was greater than BA
(P!0.05) and did not differ from DA, while BA was lower than DA (P!0.05). We
observed a positive correlation between CA and BA (rZ0.7), CA and DA (rZ0.8)
and BA and DA (rZ0.7). In conclusion, we showed that our TS patients present a
short and retropositioned face, mainly in the lower third part, conferring them a
convex profile. A prospective study will provide greater knowledge of GH effects on
craniofacial structures, looking for better orthodontic treatment for these patients.
This study was aimed to test our hypothesis that the brain-derived gonadotropinreleasing hormone (GnRH) and dopamine (DA) are delivered to the general
circulation in fetal and neonatal rats, i.e. before the establishment of the blood-brain
barrier, that is in contrast to adult rats. The GnRH and DA concentrations were
measured in plasma and in the brain on the 18th embryonic day (E18), E21, 3rd
postnatal day (P3), i.e. before the establishment of the blood-brain barrier, and on
P30–36 after the establishment of the barrier. Moreover, the concentrations of GnRH
and DA were measured in fetal plasma after microsurgical lesion of the brain regions
containing most GnRH or DA neurons or after the inhibition of DA synthesis in the
brain with sterotaxically injected a-methyl-p-tyrosine. According to our data, the
concentrations of GnRH and DA in plasma on E18, E21 and P3 enormously
exceeded those on P30–36 being as great as those in the hypophysial portal
circulation in adult rats. Reverse was true for the ontogenetic dynamics of the GnRH
and DA concentrations in the brain. The lesion of the local brain regions resulted in a
drop of the GnRH and DA concentrations in fetal plasma. The DA concentration in
plasma also decreased significantly after the inhibition of DA synthesis in the brain.
The rest of circulating GnRH and DA was shown to be insufficient to provide the
regulation of the respective adenohypophysial functions.
Thus, brain-derived GnRH and DA are delivered to the general circulation in fetal
and neonatal rats in amounts sufficient to influence peripheral targets and the brain
Obesity and metabolism – presented on Sunday
Closure by iptakalim, a cardiovascular K(ATP) channel opener, of rat
islet beta-cell K(ATP) channels and its molecular basis
Sechiko Suga1, Makoto Wakui2, Takanori Kudo3 & Yoshiji Ogawa3
Center for Education and Research of Lifelong Learning, Hirosaki
University, Hirosaki, Aomori, Japan; 2Division of Clinical Research,
Hirosaki National Hospital, Hirosaki, Aomori, Japan; 3Department of
Internal Medicine, Hirosaki University School of Medicine, Hirosaki,
Aomori, Japan.
Craniofacial development and dental maturation in growth hormone(GH)-deficient patients
Darwin Luiz Martins Oliveira, Rafaella Shimada Gomes, Maria
Helena Senger, Alcinda Aranha Nigri, Reinaldo José Gianini, Sérgio
Yassuo Nonoyama & João Carlos Ramos-Dias
Faculdade de Medicina de Sorocaba - PUC/SP, Sorocaba, São Paulo, Brazil.
Growth is a complex process, influenced to a large extent by GH. Children with GH
deficiency (GHD) have typical somatic features, including short stature and a reduction
of the craniofacial structures. Dental age (DA) is normally delayed in relation to
chronological age (CA). The effect of GH replacement on craniofacial growth is still
poorly understood. We studied the craniofacial development and dental maturation in
17 patients (4F, 13M) with GHD of different etiologies. The length of rhGH treatment
lasted from 0–15.2 yr. The median CA was 16.2G3.9 yr (GS.D.). BA varied from
5–18 yr and DA, from 7.7–17 yr. Mean stature Z-escore was K1.8G1.8 (meanGS.D.).
Craniofacial morphology was analysed by standardized lateral cephalometric
radiographs with 21 measurements. DA was calculated by panoramic radiographs
and BA was estimated by left hand-wrist radiographs. This study was approved by the
local Ethics Committee. Statistics were performed using the principal component
analysis, simple linear regression and Pearson correlation coefficient. P values !0.05
were considered significant. The most affected measures were the posterior cranial
base, position of the temporomandibular articulation, facial height and mandibular
length, that had correlation with BA and lenght of GH treatment (P!0.05). BA was
delayed in comparison with CA and DA. There were no significant differences
between CA and DA. We observed a positive correlation between BA and DA
(rZ0.8), CA and BA (rZ0.8), and CA and DA (rZ0.7). In conclusion, we showed
that our group of GHD patients presents with a short face (mainly in the lower third)
and a retropositioned mandible, conferring a more convex face profile to them.
A longitudinal study will provide a greater knowledge of the effect of rhGH treatment
on the craniofacial structures, looking for earlier orthodontic follow-up and better
results in these children.
Developing brain as an endocrine gland secreting GnRH and dopamine
to general circulation
Michael Ugrumov
Institute of Developmental Biology RAS, Moscow, Russia.
Diabetes mellitus is a group of diseases characterized by high levels of blood
glucose resulting from defects in insulin production, insulin action, or both.
Diabetes patients usually have accompanying cardiovascular disorders. Sulfonylureas have been the leading oral antihyperglycemic agents for type 2 diabetes
treatment, which currently still constitute the most popular anti-diabetic drugs.
Nevertheless, concern has arisen over the side effects of sulfonylureas on the
cardiovascular system. Here we report that iptakalim, a novel cardiovascular
ATP-sensitive potassium (K(ATP)) channel opener, closed rat islet beta-cell
K(ATP) channels and increased insulin release. Using whole-cell patch-clamp
recordings, iptakalim depolarized beta-cells, induced action potential firing and
reduced pancreatic KATP channel currents. Using single-channel recordings,
iptakalim reduced K(ATP) channel open-probability independently of intracellular ATP concentrations. We demonstrated that iptakalim elevated
intracellular calcium concentrations and increased insulin release as revealed
by fluorescence imaging (fura-2) and biochemical measurements, respectively. In
addition, iptakalim significantly inhibited the open-probability of recombinant
Kir6.2/SUR1 and Kir6.2FL4A (a trafficking mutant of the Kir6.2) channels
expressed in transfected human embryonic kidney (HEK) 293 cells. Collectively,
iptakalim, a cardiovascular KATP channel opener, closes rat islet beta-cell K(ATP)
channels, which may result from direct inhibition of the Kir6.2 subunit.
Therefore, iptakalim bi-directionally regulates K(ATP) channels in cardiovascular and islet tissues, and this unique pharmacological property suggests
iptakalim could be used as a new therapeutic strategy for the treatment of type 2
diabetes with the potential benefit in alleviating cardiac and/or vascular disorders
frequently associated with diabetes.
Plasma adiponectin and leptin levels in obese and insulin resistant
postmenopausal females with type 2 diabetes
Nona Adamia, Tea Tsotsonava & Ketevan Janberidze
Tbilisi State Medical University, Tbilisi, Georgia.
Adipocytokines appear to be important in regulating insulin sensitivity. The
objective of this study was to compare the levels of adiponectin and leptin in lean,
obese and obese diabetic (OD) postmenopausal female (PMF) subjects during 6
months follow-up of Metformin therapy (MT).
Endocrine Abstracts (2007) Vol 14
9th European Congress of Endocrinology, Budapest, Hungary, 2007
We examined plasma levels of adiponectin and leptin in 26 OD PMF with a mean
body mass index (BMI) of 36.6G1.8, 10 obese (BMIZ35.9G2.2) and 10 lean
(BMIZ22.3G1.9) individuals. The investigation was approved by the local ethics
committees. All participants gave informed, written consent before starting the trial.
Insulin resistance (IR) was assessed using the homeostasis model assessment.
Baseline characteristics of all groups shown that adiponectin was significantly
decreased and leptin is significantly elevated in OD PMF and obese subjects in
comparison with leans (P!0.001 and PZ0.003, respectively). There was a tendency
for adiponectin levels to be lower in OD PMF as compared with obese individuals
(PZ0.053). OD PMF were more insulin resistant than obese and lean subjects
(P!0.001). Results of MT shown that circulating adiponectin levels were significantly
increased (16.1G3.9 vs. 19.1G6.0 ng/ml, PZ0.008) with significant reduction of
BMI and IR (PZ0.005 and P!0.001, respectively). Leptin levels did not change
Circulating adiponectin levels is significantly reduced in OD PMF in comparison
with obese and lean subjects. Hypoadiponectinemia in PMF may be explained by
only IR because the amelioration of whole-body insulin action by MT causes the
increase of serum adiponectin levels. Leptin levels in OD PMF are not significantly
different from leptin levels of obese subjects, although they significantly differ from
leptin levels of lean individuals.
Pioglitazone modifies the effects of growth hormone on lipolysis and
insulin sensitivity
Morten B Krag1, Søren Nielsen1, ZengKui Guo2, Steen B Pedersen3,
Ole Schmitz1, Jens S Christiansen1 & Jens OL Jørgensen1
Medical Department M, Aarhus University Hospital, DK-8000 Aarhus C,
Denmark; 2Endocrine Research Unit, Mayo Clinic, Rochester, MN 55905,
United States; 3Medical Department C, Aarhus University Hospital, DK8000 Aarhus C, Denmark.
Thiazolidiones (TZD) improves insulin sensitivity in type 2 diabetes via effects on
fat metabolism, whereas growth hormone (GH) stimulates lipolysis and induces
insulin resistance.
To evaluate the effects of TZD on fat metabolism and insulin sensitivity in
GH-treated GH deficient (GHD) patients.
Randomized, placebo-controlled, double-blind parallel-group study including 20
GHD patients on continued GH replacement therapy. The patients were studied
before and after 12 weeks.
Patients received either tablet pioglitazone 30 mg (NZ10) or placebo (NZ10) once
daily for 12 weeks.
12 weeks of pioglitazone treatment in GH-replaced GHD patients was associated
with improved insulin sensitivity (PZ0.03) and increased basal glucose oxidation
(PZ0.004). Change in insulin-stimulated adiponectin level after pioglitazone
treatment was positive correlated to the change in insulin-stimulated total glucose
disposal (RZ0.69, PZ0.04). Pioglitazone significantly decreased basal free fatty
acid levels (PZ0.02) and lipid oxidation (PZ0.02). Adiponectin levels almost
doubled during pioglitazone treatment (PZ0.0001).
The impact of GH on lipolysis and insulin sensitivity is modified by administration
of PPARg agonists.
The metabolic syndrome and associated sexual dysfunction: psychobiological correlates
Giovanni Corona1, Edoardo Mannucci2, Luisa Petrone1, Riccardo Mansani1,
Giancarlo Balercia3, Valerio Chairini4, Gianni Forti1 & Mario Maggi1
Andrology Unit, University of Florence, Florence, Italy; 2Geriatric Unit,
Diabetes Section, University of Florence, Florence, Italy; 3Endocrinology
Unit, Polytechnic University of Marche, Ancona, Italy; 4Endocrinology
Unit, Maggiore-Bellaria Hospital, Bologna, Italy.
The aim of present study is to determine psychobiological characteristics of
sexual dysfunction (SD) associated with metabolic syndrome (MS; as defined by
Endocrine Abstracts (2007) Vol 14
National Cholesterol Education Program’s Adult Treatment Panel III, NCEPATP-III criteria) in a consecutive series of 803 male out-patients.
Several hormonal, biochemical and instrumental (penile doppler ultrasound,
PDU) parameters were studied, along with psychopathology scores (Middlesex
Hospital Questionnaire modified MHQ). The Structured Interview on Erectile
DYsfunction (SIEDY), was also applied.
Among subjects studied, 236 patients (29.4%) were diagnosed as having a
MS. Among them 96.5% reported ED, 39.6% hypoactive sexual desire,
(HSD) 22.7% premature and 4.8% delayed ejaculation. Patients with MS were
characterized by greater subjective (as assessed by SIEDY) and objective (as
assessed by PDU) ED and by greater somatizated anxiety than the rest of the
sample. The prevalence of overt hypogonadism (total testosterone !8 nM)
was significantly higher in patients with MS. Circulating TT decreased as the
number of MS components increased (BZK1.35G0.182 nmol/l; P!0.0001,
after adjustment for age). Accordingly, the relative risk for hypogonadism was
significantly higher in patients reporting 3 or more risk factors for MS.
Among MS components, waist circumference and hyperglycemia were the
best predictors of hypogonadism. Among patients with MS, hypogonadism
was present in 11.9% and 3.8% in the rest of the sample (P!0.0001) and it
was associated with typical hypogonadism-related symptoms, such as
hypoactive sexual desire, low frequency of sexual intercourses and depressive
Our data suggest that MS is associated with a more severe ED and induces
somatization. Furthermore, MS is associated with a higher prevalence of
hypogonadism in patients with SD. The presence of hypogonadism can further
exacerbate the MS-associated sexual dysfunction, adding the typical hypogonadism-related symptoms. (including HSD, 66.7%).
A comparison of NCEP-ATP-III and IDF metabolic syndrome
definitions with relation to metabolic syndrome associated sexual
Giovanni Corona1, Edoardo Mannucci2, Luisa Petrone1, Francesco Lotti1,
Alessandra D Fisher1, Giancarlo Balercia3, Valerio Chairini4, Gianni Forti1
& Mario Maggi1
Andrology Unit, University of Florence, Florence, Italy; 2Geriatric Unit,
Diabetes Section, University of Florence, Florence, Italy; 3Endocrinology
Unit, Polytechnic University of Marche, Ancona, Italy; 4Endocrinology
Unit, Maggiore-Bellaria Hospital, Bologna, Italy.
The aim of present study was to verify possible differences in the prevalence of
vasculogenic ED and hypogonadism comparing two distinct new definitions of
MetS, as National Cholesterol Education Program-Third Adult Treatment Panel
(NCEP-ATPIII) and International diabetes Federation (IDF) in patients with
sexual dysfunction.
Several hormonal, biochemical and instrumental (penile doppler ultrasound)
parameters were studied. ANDROTEST Structured Interview was also applied.
This a 12-item, recently validated, inventories, which assesses the degree of
androgenization in male.
We studied a consecutive series of 1086 patients. The prevalence of metabolic
syndrome was 32.0% and 44.7% according to NCEP-ATPIII and IDF criteria,
respectively. Patients with MetS according to both criteria reported lower PGE-1
stimulated penile flow (Vpmax). At multivariate analysis, only NCEP-ATPIII was
significantly associated with Vpmax (BZK7.7G3.8; P!0.05). Patients with MetS
defined according to both criteria reported lower total (13.6G6.0 vs. 17.4G7.2 and
14.7G7.4 vs. 18.2G6.0 nmol/l,) and free testosterone levels (34.8G14.0 vs. 40.8G
13.7 and 36.2G14.1 vs. 42.5G13.5 pmol/l), higher prevalence of hypogonadism
(34.3 vs. 11.9 and 25.3 vs. 8.7%), and higher ANDROTEST score (9.6G3.0 vs.
7.2G3.6 and 9.2G3.2 vs. 6.0G3.2) respectively for NCEP-ATPIII and IDF; all P!
0.0001. However, when IDF, but not NCEP-ATPIII, criteria were fulfilled, the
prevalence of hypogonadism was significantly lower than that observed in patients
fulfilling both criteria (15.6 vs.34.8% respectively; P!0.0001). Conversely, those
fulfilling NCEP-ATP-III, but not IDF, criteria did not show a significant different
prevalence of hypogonadism than those positive for both sets of criteria (30.8
vs.34.8%; PZNS).
In patients with ED, NCEP-ATPII criteria seem to be a better predictor of
hypogonadism and impaired penile blood flow than IDF.
9th European Congress of Endocrinology, Budapest, Hungary, 2007
Effect of supervised structured exercise program for 16 weeks on
metabolic, pulmonary and cardiovascular parameters in obese
Juan Guı́zar-Mendoza, Benigno Linares, Norma Amador, Gloria Barbosa &
Juan Malacara
Instituto Mexicano del Seguro Social, León/Guanajuato, Mexico,
Universidad de Guanajuato/Instituto de Investigaciones Médicas,
León/Guanajuato, Mexico, 3Universidad de Guanajuato/Facultad de
Medicina, León/Guanajuato, Mexico.
To investigate whether a supervised structured exercise program by 16 weeks
improves metabolic, pulmonary and cardiovascular parameters in obese
Material and methods
We included 38 obese adolescents between 12–15 years old. They participated in
a supervised exercise program by 90 minutes, 5 days a week during 16 weeks. At
baseline and at the end of the exercise program, we evaluated cardiorespiratory
fitness, anthropometric measurements, lipid profile, glucose, insulin, leptin,
adiponectin, and blood pressure levels. Pulmonary function was evaluated by
spirometry and heart sympathetic activity by spectral analysis of the R-R interval
during 60 minutes to obtain indices of heart autonomic function.
The exercise program increased exercise ability (P!0.001), maximal oxygen
uptake (PZ0.01), forced vital capacity (PZ0.004), and adiponectin levels (P!
0.001); while BMI (PZ0.001), body fat (!0.001), glucose, triglycerides (P!
0.001 in both), leptin (P!0.001), blood pressure levels (P!0.001), and heart
sympathetic activity expressed as LF/HF index (PZ0.005) significantly
decreased. The change in LF/HF index was correlated with the decrease in
leptin (rZ43; PZ0.007), diastolic (rZ0.33; PZ0.04) and systolic (0.35; PZ
0.03) blood pressure levels respectively.
A short-term supervised structured exercise decreased adiposity and improves
metabolic, pulmonary, and cardiovascular parameters in obese adolescents.
Continuous administration of dihydrotestosterone or letrozole to
immature female rats results in polycystic ovary syndrome characteristics at adult age
Louise Mannerås1, Theodore Lystig2, Agneta Holmäng1, Malin OttossonLönn2 & Elisabet Stener-Victorin1
Institute of Neuroscience and Physiology, Göteborg, Sweden; 2Insitute of
Medicine, Göteborg, Sweden.
Polycystic ovary syndrome (PCOS) is a complex endocrine and metabolic
disorder associated with ovulatory dysfunction, hyperandrogenism, abdominal
obesity and insulin resistance. Since hyperandrogenism is a PCOS key feature, the
aim was to evaluate the effects of androgen receptor activation in terms of
continuously administration, beginning pre-pubertal, of either the non-aromatizable androgen dihydrotestosterone (DHT) or the aromatase inhibitor letrozole (L),
on ovarian morphology, as well as on the endocrine and metabolic status were
At 21 days of age, the rats were implanted subcutaneously with a pellet releasing
DHT or L continuously during 90 days. Estrus cyclicity (vaginal smear), ovarian
morphology, sex steroid and leptin concentrations, body composition (DEXA,
MRI, and tissue dissection), mesenteric adipocyte size (computerized image
analysis), and insulin sensitivity (euglycemic hyperinulinemic clamp) were
DHT induced polycystic ovaries (PCO) and anovulation in 75% of the rats. DHT
rats also displayed increased body weight, fat mass and weight of individual
abdominal fat depots, as well as enlarged mesenteric adipocyte size with a right
shifted size distribution curve. Moreover, elevated leptin levels and insulin
resistance were observed in DHT treated rats. Almost all L rats developed PCO
morphology with similarity to human PCO, including hyperplastic theca cell
layer, and anovulation. Hyperandrogenism and increased body weight without
any body composition changes were other characteristics of the L group.
Typical PCO morphology was induced both by DHT and L treatment. In
particular DHT treatment also resulted in metabolic disorders of the syndrome,
while the endocrine features of the syndrome were mainly induced by L. Both
models can therefore be concluded as suitable for investigation of different
aspects of the human PCOS.
Neonatal sex steroid exposure of female rats results in insulin resistance
and enlarged mesenteric adipocytes
Camilla Alexanderson1, Theodore Lystig2, Elisabeth Stener-Victorin1,
Malin Lönn2 & Agneta Holmäng1
Instititute of Neuroscience and Physiology, Göteborg, Sweden; 2Institute of
Medicine, Göteborg, Sweden.
Neonatal events may contribute to the development of disorders such as type 2
diabetes and obesity at adult age. We have previously shown that neonatal
testosterone (T) programming of female rats is followed by insulin resistance and
changes in adipose tissue distribution with centralization of body fat. Therefore,
the aim of this study was to examine the effects of neonatal injection of T,
estradiol (E) or dihydrotestosterone (DHT) on insulin sensitivity and size
distribution of adipocytes in intra-abdominal and subcutaneous adipose tissue in
female rats.
Pups received one injection of T, E, DHT or vehicle within 3 hours after birth. At
14 wks of age the rats were exposed to a euglycemic hyperinsulinemic clamp.
Intra-abdominal (mesenteric) and subcutaneous (inguinal) adipose tissues were
dissected and weighed. Adipocyte size was analysed using a computerized image
analysis system.
All groups receiving steroids were insulin resistant in comparison with controls.
The mesenteric adipocyte size distribution was shifted to the right in T- and E-rats
compared with controls while adipocyte size in the inguinal depot was not
affected. T-rats also displayed increased mesenteric adipose tissue weight.
Analysis of all groups together showed a negative correlation between mesenteric
adipocyte size and glucose infusion rate.
Sex hormone exposure in early life may predispose to disturbances in insulin
sensitivity and adipose tissue at adult age. Directly after birth, in particular the
mesenteric adipose tissue depot seems to be vulnerable to T- and E exposure
which is seen as a shift to the right of the adipocyte size distribution in adulthood.
Evaluation of visceral protein malnutrition in morbid obese patients
operated on laparoscopic gastric bypass
Rosa Casañ, Carlos Morillas, Eva Sola, Katherinne Garcı́a, Jesus Yanini,
Ana Jover, Marcelino Gomez & Antonio Hernández
Endocrinology Department, Doctor Peset University Hospital, Valencia,
Morbid obesity is associated with a decreased life expectancy and a myriad of
serious medical problems. The Roux-en-Y gastric bypass (RYGBP) is the most
effective procedure for the treatment of these patients, but it can be responsible of
early and late complications. The aim of this prospective study was to evaluate the
rate of visceral protein malnutrition (VPM) in morbid obese (MO) patients two
years after laparoscopic RYGBP. Albumin (Alb), prealbumin (Prealb), transferrin
(Transf), retinol binding globulin (RBG), C3-complement factor (C3) plasma
levels, and lymphocyte count (Lymph) were measured before and 2 years after
RYGBP. Data were evaluated using paired Student t-test. Data were available for
46 patients (9 men and 37 women). Mean age: 38.5G11 years; mean follow-up
time: 24G 9 months.
No differences were observed in Prealb, RBG, Transf or Lymph count. Before
surgery, 1 patient (2.2%) had C3 values under normal levels, and after surgery 4
patients (8.7%) had C3 values under normal levels.
Weight (kg)
BMI (kg/m2)
Alb (mg/dL)
C3 (mg/dL)
24 months
Endocrine Abstracts (2007) Vol 14
9th European Congress of Endocrinology, Budapest, Hungary, 2007
1- There were no changes in main visceral protein plasma levels: Alb,
Prealb, Transf, and RBG in MO patients after 2 years of RYGBP. 2- A
significant decrease of C3 values was observed in these patients, without
changes in lymphocyte count. In spite of this decrease, C3 levels remained
in most patients between the normal range. 3- RYGBP seems to be an
effective procedure to treat morbid obesity which does not cause VPM, but
immunity should be assessed.
Overconsumption of salty and sweet foods increases blood pressure in
Vassilios Petrou1, Athanasia Tertipi1, Asteroula Papathanasiou1,
Ourania Zerva2, Vassiliki Skarpa1, Petros Papachilleos1,
Marina Anastasacou1, Panagiotis Nicolopoulos1 &
Charalambos Hadjiathanasiou1
Children’s Hospital “P. & A. Kyriacou” Department of Endocrinology,
Athens, Greece; 2Children’s Hospital “P. & A. Kyriacou” Department of
Nutrition, Athens, Greece.
To estimate the impact of overconsumption of salty and sweet foods on Body
Mass Index (BMI) and Blood Pressure (BP) in children.
We studied 208 children (105 girls), aged 9.2G3.0 yr, 57 (27.4%) of normal
weight, 37 (17.8%) overweight and 114 (54.8%) obese. Overconsumption of
NaCl was considered O5 g/day and of free sugar O0.5 g/Kg ideal Body
Weight/day. BP was measured as appropriate and BMI was estimated in all
Children overconsuming salty and sweet foods had significantly higher BMI SDS
than children consuming small amount of salty and sweet foods (2.1G1.5 vs
1.2G1.5, P!0.001 for salty foods and 2.1G1.5 vs 1.2G1.6, PZ0.002 for sweet
foods). Thirty-three (57.9%) of children of normal weight overconsumed salty
foods versus 23 (62.2%) of overweight and 98 (86.0%) of obese (c2Z18.8, P!
0.001). Thirty-five (61.4%) of children of normal weight overconsumed sweet
foods versus 32 (86.5%) of overweight and 99 (86.8%) of obese (c2Z16.5, P!
0.001). One hundred twenty nine children (83.8%) overconsuming salty foods had
Systolic BP (SBP)O50th percentile versus 35 (64.8%) of children consuming
small amounts of salty foods (c2Z8.6 PZ0.006). One hundred thirty six children
(81.9%) that overconsumed sweet foods had SBPO50th percentile versus 28
(66.7%) that consumed small amounts of sweet foods (c2Z4.6, PZ0.036). There
was no difference regarding diastolic BP (DBP) among children consuming large
or small amounts of salty and sweet foods respectively. BMI SDS emerged as the
most important determinant of SBPO50th percentile and DBPO50th percentile
in multivariate analysis.
Overconsumption of salty and sweet foods is related to a relatively increased BP
in children through the incremental effect on BMI SDS.
Expression of PKA regulatory subunits inversely correlates with BMI
and insulin resistance parameters in human adipocytes from lean and
obese subjects
Sara Bondioni1, Giovanna Mantovani1, Luisella Alberti2, Sabrina Corbetta3,
Luisa Gilardini2, Cecilia Invitti2, Marco Antonio Zappa4, Stefano Ferrero5,
Erika Peverelli1, Andrea G Lania1, Paolo Beck-Peccoz1 & Anna Spada1
Endocrine Unit, Dpt. of Medical Sciences, Fondazione Ospedale Maggiore
Policlinico Mangiagalli e Regina Elena IRCCS, University of Milan, Milan,
Italy; 2Lab. of Diabetologic Research, Istituto Auxologico Italiano IRCCS,
Milan, Italy; 3Endocrinology and Diabetology Unit, Dpt. of MedicalSurgical Sciences, University of Milan, Policlinico San Donato IRCCS, San
Donato Milanese, Milan, Italy; 4General Surgery Unit, Dpt. of Surgical
Sciences, University of Milan, Fondazione Ospedale Maggiore Policlinico
Mangiagalli e Regina Elena IRCCS, Milan, Italy; 5Pathology Unit,
Department of Medicine, Surgery and Dentistry, A.O. San Paolo and
Fondazione Ospedale Maggiore Policlinico Mangiagalli e Regina Elena
IRCCS, Milan, Italy.
Endocrine Abstracts (2007) Vol 14
In human adipocytes the cAMP-dependent pathway mediates signals
originating from the activation of beta-adrenergic receptors, thus playing a
key role in the regulation of important metabolic processes such as lipolysis
and thermogenesis. CyclicAMP effects are mainly mediated by cAMPdependent protein kinase (PKA), a tetrameric enzyme composed by two
catalytic subunits associated with two regulatory (R) subunits. There are
four different R subunit genes and proteins (R1A, R1B, R2A, R2B)
expressed with a tissue-specific pattern and exerting distinct roles in cell
differentiation and growth control. Recent studies indicate the R2B isoform
as the most expressed in mouse adipose tissue while its presence is limited
elsewhere. Moreover, R2B knock-out mice are genetically lean and
protected against developing diet-induced obesity and fatty-livers. The aim
of this study was to investigate the expression of the different PKA
regulatory subunits in 65 human subcutaneous and visceral adipose tissue
samples from 10 lean subjects (BMI!25) and 55 obese patients (BMIO30).
Real-time PCR showed that, as in mice, R2B is the most abundant
transcript, both in obese and normal subjects, with no differences between
visceral and subcutaneous adipose tissue. Moreover, a significant negative
correlation was observed between R2B expression levels and BMI, insulin
levels, HOMA-IR (rZK0.280, rZK0.269, rZK0.255, respectively; P!
0.05), with a positive correlation with adiponectin and adiponectin receptors
1&2 mRNA levels (rZC0.636, rZC0.582, rZC0.631 respectively; P!
0.001). Moreover, among obese patients, patients with metabolic syndrome
showed the lowest R2B levels. Immunohystochemistry and western-blot
analysis performed in 15 of the 55 samples from obese patients and in the
10 samples from lean subjects confirmed the same expression pattern. This
is the first study evaluating the relative expression of the different PKA
isoforms in human adipose tissue. Our results indicating important BMIrelated differences in R2B expression suggest that similar differences in
PKA activity may modulate the lipolytic response to beta-adrenergic
Insulin resistance and fasting leptin’s relationship in subjects with
metabolic syndrome
T Mokhort & E Shishko
Belarusian State Medical University, Minsk, Belarus.
Background and aims
The aim of our study is to investigate the possible associations between leptin and
fasting insulin and index HOMA-IR in patients with Metabolic Syndrome as
Leptin is involved in regulation of body weight.
Materials and methods
The study included 100 patients (32 m, 68 f) 25–65 years. They were divided into
2 groups matched by sex, age, weight, body mass index (BMI), waist-to-hip ratio
(WHR). Research group included 56 patients (24 m, 32 f) with Metabolic
Syndrome: abdominal obesity, insulin resistance, hyperinsulinemia, glucose
intolerance, hypertension and dyslipidemia. Control group included 44 patients
(16 m, 28 f) without clinical and biochemical findings of Metabolic Syndrome.
The average fasting plasma glucose, 2-hour plasma glucose concentrations
following a 75-g oral glucose tolerance test, total cholesterol, triglycerides,
systolic and diastolic blood pressure were also evaluated. Fasting serum leptin
(FL) and fasting insulin levels (FI) were detected by sensitive and specific ELISA.
Index HOMA-IR was calculated by standard formula. HOMA-IRZorO 2.7 were
considered as insulin resistance.
In patients of the research and control groups serum leptin levels were
higher in females (median 45.1 and 27.8 ng/ml respectively) than in males
(15.9 and 7.7 ng/ml respectively). But only in patients of the research group
correlations were between BMI and WHR (rZ0.91 P!0.001 vs rZ0.93
P!0.01 respectively). Correlation analysis showed that FL were significantly correlated with the FI (rZ0.56 P!0.01) and HOMA-IR (rZ0.52
P!0.01) in research group. In subjects of the control group leptin
concentration correlated with the HOMA-IR only in men (rZ0.91 P!
0.01) and not correlated in female. The strongest correlations were between
FL and total cholesterol (rZC0.49 ?!0.05 in men) and triglycerides
(rZC0.8 ?!0.05 in women) in research group.
Determine positive correlation of basal leptin and index insulin resistance
confirms hyperleptinemia and leptinresistance concern in formation of
metabolic syndrome.
9th European Congress of Endocrinology, Budapest, Hungary, 2007
Epicardial adipose tissue, hepatic steatosis and obesity
Ayse Sertkaya Cikim1, Ergun Topal2, Murat Harputluoglu3,
Lezzan Keskin1, Zeynep Zengin1, Kerim Cikim1, Ramazan Ozdemir2,
Murat Aladag3 & Saim Yologlu4
Inonu University Faculty of Medicine Department of Internal Medicine
Division of Endocrinology and Metabolism, Malatya, Turkey; 2Inonu
University Faculty of Medicine Department of Cardiology, Malatya,
Turkey; 3Inonu University Faculty of Medicine Department of Internal
Medicine Division of Gastroenterohepathology, Malatya, Turkey; 4Inonu
University Faculty of Medicine Department of Biostatistics, Malatya,
The measurement of epicardial adipose tissue (EAT) sonographically is reported
to be related with both obesity and insulin resistance. Hepatic steatosis is one of
the best known other coincidence with obesity. We aimed to evaluate the
relationships between EAT thickness, hepatic steatosis and insulin resistance in
obese patients.
Obese 63 subjects were enrolled into the study. Local ethical committee approval
was obtained. Patients were divided into three groups according to body mass
index (BMI) as follows: 20 patients with 30%BMI!35 kg/m2 (Group 1, mean
age 39.3G12.9 yrs), 25 patients with 35%BMI!40 kg/m2 (Group 2, mean age
41.7G9.3 yrs), and 18 patients with BMIR40 kg/m2 (Group 3, mean age 36.8G
13.9 yrs). EAT thickness and grade of hepatic steatosis were assessed
sonographically. Anthropometrical measurements were assessed with the footto-foot bioelectrical impedance analysis. Insulin resistance was assessed
according to basal insulin, QUICKI and HOMA equations.
hsCRP was the only metabolic parameter; which was higher in Group 3 than
Group 1 significantly (PZ0.02). EAT thickness was similarly higher in both
groups 2 and 3; but groups were found to be similar for grade of hepatic steatosis.
Both EAT thickness and grades of hepatic steatosis were positively and
significantly correlated with whole body fat mass and abdominal adiposity.
Waist circumference was the only factor affecting EAT thickness in linear
regression analysis.
Grade of hepatic steatosis is a lesser sensitive marker for closer obesity levels than
EAT, but with its significant correlations; hepatic steatosis can also be assessed as
a valuable predictor for reflecting increments of whole body fat mass and
abdominal adiposity as EAT thickness.
Decreased 11beta-hydroxysteroid dehydrogenase type 1 activity in
obese boys
Susanna Wiegand1, Anna Richardt1, Thomas Remer3, Stefan A Wudy4,
Jeremy W Tomlinson5, Annette Grüters1, Paul M Stewart5, Christian
J Strasburger2 & Marcus Quinkler2
Paediatric Endocrinology, Charite Campus Virchow, Universitaetsmedizin
Berlin, Berlin, Germany; 2Clinical Endocrinology, Charite Campus Mitte,
Universitaetsmedizin Berlin, Berlin, Germany; 3Department of Nutrition
and Health, Research Institute of Child Nutrition, Dortmund, Germany;
Steroid Research Unit, Center for Child and Adolescent Medicine, Justus
Liebig University, Giessen, Germany; 5Division of Medical Sciences,
Institute of Biomedical Research, University of Birmingham, Birmingham,
United Kingdom.
The incidence of childhood obesity and type 2 diabetes has reached epidemic
proportions. Glucocorticoid excess causes central obesity and diabetes mellitus as
seen in Cushing’s syndrome. The 11beta-hydroxysteroid dehydrogenase type 1
enzyme (11beta-HSD1), which is predominantly expressed in liver and adipose
tissue, regenerates active cortisol from inactive cortisone. Increased 11betaHSD1 may cause tissue-specific Cushing syndrome with central obesity and
impaired glucose homeostasis.
Design, patients and methods
Clinical and laboratory characteristics, and anthropometric measurements were
determined in 15 male (aged 12–18) and 6 female (aged 12–18) obese pubertal
children. In addition, analysis of 24 h excretion rates of glucocorticoids were
performed in obese and age- and sex-matched non-obese children using gas
chromatographic-mass spectrometric (GC-MS) analysis.
11beta-HSD1 activity (urinary THFC5alphaTHF/THE ratio) was lower in
obese compared to non-obese boys. In addition, obese children had a higher
total cortisol metabolite excretion than non-obese children. 11beta-HSD1
activity was significantly related to age, but not to waist-to-hip ratio, fat mass
(% of body mass), or insulin resistance index (HOMA). Standard deviation
score (SDS)-BMI did not correlate with 11beta-HSD1 or K2 (urinary free F/
free E ratio) activity, or with total cortisol metabolite excretion. We did
not find a gender difference regarding 11beta-HSD1 or K2 activity. 11betaHSD2 activity significantly correlated to abdominal circumference in obese
In conclusion, our findings strongly suggest that 11beta-HSD1 activity increases
with age and is reduced in obese boys. In addition, obese children have a higher
total cortisol metabolites excretion suggesting a stimulated HPA axis.
Clinical presentation of nonclassic congenital adrenal hyperplasia
(NC-CAH): from suspicion to diagnosis
Anna Casteràs Román, Ma Concepción Páramo Fernández, Javier De la
Fuente Aguado, Elena Hervás Abad, Laura Fajar Rodrı́guez, Beatriz
Mantiñán Gil, Reyes Luna Cano, Ma Antonia Rego Iraeta, Digna Rodrı́guez,
Domingo González Lestón & Ricardo Vı́ctor Garcı́a-Mayor
Hospital Xeral de Vigo, Vigo, Pontevedra, Spain; Hospital POVISA, Vigo,
Pontevedra, Spain.
Nonclassic congenital adrenal hyperplasia (NC-CAH) caused by mutations in
CYP21B gene is an inherited disorder with various clinical forms in relation to the
21-hydroxylase (21OH) activity. Classic forms are recognized early during
neonatal period as salt-wasting crisis or genital ambiguity, while non-classic form
presents later with wide hyperandrogenic spectrum. Genetic testing has proved to
be the definitive diagnostic method.
To observe the clinical presentation in relation to the genotype among subjects
with clinical suspect of NC-HAC.
Subjects and methods
Ninety-seven patients (90 female, 7 male) consulting with suggestive clinical data
of NC-HAC were genotyped and classified into groups (1: no mutation nZ54;
2: homozygotes nZ22; 3: compound heterozygotes nZ11; 4: simple
heterozygotes nZ10). Clinical presentation was correlated with the genetic
Mutations in CYP21B were present in 44,3% of patients and V281L in
homozygous state was the most frequent genotype in the studied population
(48,8%). In general, hirsutism and premature pubarche were the most common
symptoms (32,9 and 28,8% respectively).
Less than 50% of hyperandrogenic patients had genetic confirmation of 21OH
deficiency. We did not find clinical features associated with the genotype, but
precocious pubarche, which is more common in simple and compound
heterozygotes than in homozigotes or without mutation (P!0.05).
Daily and nightly urinary free cortisol ratio as a marker of the
hypothalamic-pituitary-adrenal (HPA) axis activity in abdominal
Valentina Vicennati1, Uberto Pagotto1, Bruno Ambrosi2, Mauro Maccario2,
Ettore Degli Uberti2, Marco Boscaro2, Francesco Cavagnini2,
Franco Mantero2, Decio Armanini2, Roberto Vettor2, Mario Marugo2 &
Renato Pasquali1
Endocrinology Unit, Bologna, Italy; 2“HPA axis and obesity” Group-SIE,
Bologna, Italy.
Abdominal obese (AO) women might have a hyperactivation of the HPA axis.
The limitations of previous studies have been often represented by the limited and
Endocrine Abstracts (2007) Vol 14
9th European Congress of Endocrinology, Budapest, Hungary, 2007
heterogeneous number of patients enrolled. Our aim was to asses urinary free
cortisol (UFC) output during daily and nightly hours in a large cohort of AO
women vs. normal weight controls (CT). 107 AO women and 37 CT were
enrolled in the study. In basal condition, each subject underwent OGTT,
biochemical determinations. Each subject collected daily (from 0800 AM to 0800
PM, dUFC) and nightly (from 0800 PM to 0600 AM of the day after, nUFC)
Cholesterol and triglycerides levels were significantly higher (P!0.001) in the
AO, whilst HDL were significantly (P!0.01) lower than in CT. AO had
significantly higher HOMA index than CT. There were no differences neither in
dUFC nor in the nUFC between the groups. On the contrary, AO had significantly
lower dUFC/nUFC than CT.
There was a negative and significant correlation between dUFC/nUFC and
waist and BMI in all subjects. When AO were analyzed separately, the
correlation between dUFC/nUFC and anthropometric variables was still
present. Moreover, the ratio was also positively correlated to HOMA index
In order to assess the linkage between HPA axis activity and metabolic
syndrome, a multiple regression was performed in AO. dUFC/nUFC was still
negatively and significantly correlated to BMI, while the correlation with
waist circumference was lost. Interestingly, dUFC/nUFC was still positively
and significantly correlated to HOMA index and systolic blood pressure. On
the contrary, a negative and significant correlation was found between
dUFC/nUFC and both HDL and diastolic blood pressure.
In conclusion, obesity by itself is characterized by high nightly UFC
excretion. The HPA axis dysregulation is strictly associated to the
abnormalities of the metabolic syndrome, particularly to glucose-insulin
homeostasis, dyslipidemia and hypertension.
Interaction of hypothalamic receptors involved in weight regulation
Anne Rediger1, Patrick Tarnow1, Annette Grüters1, Michael Schäfer2 &
Heike Biebermann1
Charité Universitätsmedizin Berlin, Inst. Exp. Ped. Endocrinology, Berlin,
Germany; 2Charité Universitätsmedizin Berlin, Inst. Pharmacology, Berlin,
Food intake is centrally regulated in hypothalamic nuclei where many
G-protein-coupled receptors (GPCRs) are expressed which are known to be
involved in weight regulation. Peripheral hormonal signals activate their
corresponding receptors in the arcuate nucleus. Orexigenic signals activate
POMC expression in one subset of neurons and inhibit AgRP and NPY
expression in a second subset. Cleavage products of POMC, a- and b-MSH
then stimulate melanocortin-4-receptors (MC4R) in the paraventricular
nucleus of the hypothalamus to inhibit food intake or stimulate the
melanocortin 3 receptor (MC3R) in the arcuate nucleus to activate a feedback
loop. Other neuropeptides or neurotransmitters are involved in hypothalamic
regulation of body weight, which also act through G-protein-coupled-receptors
co-expressed with melanocortin receptors (MCR) in hypothalamic nuclei. The
concept of homo and hetero-oligomerization of GPCRs today is well
accepted. Recently we could show homo-oligomerization of MC4R. In a
systematic approach we investigated the interaction of GPCRs that are
expressed on the same neurons.
We used two different methods to investigate GPCR oligomerization: a
sandwich-ELISA approach with differentially N- and C-terminal tagged
receptors in COS-7 cells and the FRET-acceptor-photobleaching-technique
which allows monitoring of GPCR interaction in living HEK-293 cells.
Furthermore we investigated receptor co-localization on the cell surface by
laser scanning microscopy.
Here we report data on interaction of the MC3R and ghrelin receptor (GHSR) that
are coexpressed on arcuate NPY/AgRP neurons. The usage of both methods
results in a strong signal of MC3R/GHSR oligomerization.
We could demonstrate for the first time that GPCR from different subfamilies, that
are expressed on the same neuron and are involved in weight regulation form
receptor oligomeres. These findings may provide a mechanistic basis of a
functional interaction between melanocortin and ghrelin receptors and thereby
widen our understanding of hypothalamic signalling pathways involved in weight
Endocrine Abstracts (2007) Vol 14
Association of estrogen receptor-alpha gene polymorphisms with
cerebrovascular disease in patients with metabolic syndrome
Nektaria Xita1, Sophia Markoula2, Leandros Lazaros3, Athanasios Kyritsis2,
Ioannis Georgiou3 & Agathocles Tsatsoulis1
Department of Endocrinology, University of Ioannina, Ioannina, Greece;
Department of Neurology, University of Ioannina, Ioannina, Greece;
Laboratory of Reproductive Genetics, University of Ioannina, Ioannina,
The vascular protective effects of estrogens are known to be mediated by their
binding to specific estrogen receptors (ER). However, the significance of genetic
variations of the ER in vascular diseases has not been reported. We have
examined the association between stroke and PvuII and XbaI polymorphisms of
the estrogen receptor-alpha gene in patients with metabolic syndrome.
Methods and subjects
The study population consisted by 84 male and 46 female patients with metabolic
syndrome compared with 100 healthy men and 140 healthy women respectively.
The body mass index was recorded and biochemical parameters were measured.
PCR-RFLP and genotyping of ER PvuII and XbaI polymorphisms were performed
in peripheral blood leucocytes. Multiple logistic regression analysis was used to
explore the risk factors for stroke. Local Ethical Committee approval was obtained.
Both polymorphisms were in Hardy Weinberg equilibrium in the study
population. Genotype distributions and allele frequencies of PvuII or XbaI
polymorphisms were not significantly different between control subjects and
patients. No association was found between the polymorphisms and the severity
of stroke. Total cholesterol, triglyceride, or HDL-cholesterol levels were not
significantly different among ER genotypes. However, men homozygous for A
allele of XbaI polymorphism had a stroke at a younger age compared to other
genotypes (53,3G8,1 years vs 56,9G9,4 years, P!0,05).
These findings suggest that PvuII and XbaI polymorphisms of ER are not
associated with the prevalence and severity of cerebrovascular disease. However,
the XbaI polymorphism seems to affect the age of developing cerebrovascular
disease in men with metabolic syndrome.
Bone mineral density and body composition in pubescent obese children
endangered by metabolic syndrome
Borbala Tobisch, Andrea Kozma, Zsuzsanna Nagy-Szakall, Ferenc Peter &
Laszlo Blatniczky
Buda Children’s Hospital, Budapest, Hungary.
The prevalence of type 2 diabetes due to insulin resistance is increasing in
puberty. Authors have investigated whether body weight excess arises only from
increased fat content of the body. Different anthropometrical data were also
analysed if they are able to predict degree of insulin resistance.
Materials and methods
108 obese children (50 female, 58 male, Tanner st-s1-5, mean age 12.06 years,
mean BMI: 30.97 kg/m2) with positive familiar anamnesis of metabolic syndrome
were in the study. Bone density by PQCT as well as body composition by
bioelectrical impedance analyser(inBody 3.0) were measured. Waist/hip-ratio and
body fat% based on skin-fold thicknesses measurement were calculated. HOMAindex and SC-peptide/SIRI ratio (SC/SIRI) during oral glucose tolerance test as
markers of insulin resistance were calculated
Total Z-score of bone mineral density in obese children exceeded by 0.2 SD and
trabecular density by 0.65 SD those of normal population of the same age. Obese
children’s muscle mass exceeded by 6.8 kg in average compared with same values of
“sample” population of the same age. There were slack correlations (rZ0.578 vs.
0.682) between measured and calculated body fat% as well as measured fat% and
BMI. There was no significant correlation between the anthropometrical values and
HOMA-index, nor the SC/SIRI. Waist/hip-ratio showed a mild correlation with
HOMA-index (rZ0.268) and a moderate one with SC/SIRI (rZ0.462).
Increased BMI-values in obese children are partially caused by both increased bone
mineral content and higher muscle mass. BMI-values are less helpful to estimate
inappropriate body composition. Differences between measured and calculated
body fat% can indirectly indicate the degree of visceral fat. Increased waist/hip
ratio predicts insulin resistance better. Anthropometrical data themselves do not
9th European Congress of Endocrinology, Budapest, Hungary, 2007
predict insulin resistance in youngsters, it has to be determined individually. The
SC/SIRI is a more exact indicator of insulin resistance than the HOMA-index.
Influence of gaining weight on metabolic syndrome in the menopause
Aleksandra Simoncig-Netjasov, Svetlana Vujovic, Milos Stojanovic,
Miomira Ivovic, Milina Tancic & Milka Drezgic
Institut of Endocrinology, Clinical Center of Serbia, Belgrade, Serbia.
Metabolic syndrome (MS) represents a prominent risk factor for cardiovascular disease. Parameters of MS were compared between obese women and
controls. I: 50 women (31.92G5.83 kg/m2; 54.4G3.64 y’s); Controls: 37
women (23.50G2.13 kg/m2; 53.92G3.95 y’s). Weight, height, waist and hips
circumference, sagital abdominal diameter (SAD) and blood pressure (BP)
were measured. Blood was taken at 8 am for: fasting glucose, triglycerides,
cholesterol, HDL, LD, Lp(a), FSH, LH, PRL, E2 and OGTT was performed.
Hormone analyses: RIA. Statistics: T test, Mann – Whitney U test, ANOVA.
MS: 66% in I and 22% in controls. Significant differences between groups
were found for: glycose (6.22G2.26 vs 5.49G2.43 mmol/l, P!0.05), weight
(86.20G17.82 vs 62.81G7.90 kg, P!0.01), waist (99.96G14.65 vs 79.9G
8.78 cm, P!0.01), hips circumference (114.31G11 vs 96.93G11.04 cm, P!
0.01), SAD (31.9G6.83 vs 24.9G9.86 cm, P!0.01), BMI (31.92G5.83 vs
23.5G2.13 kg/m 2, P!0.01), diastolic BP (93.08G13.41 vs 85.75G
10.54 mmHg, P!0.01), Lp(a) (0.50G0.36 vs 0.11G0.03 g/l, P!0.01), FSH
(54.35G27.16 vs 72.32G30.17 IU/L, P!0.01), LH (20.33G11.08 vs 28.77G
14.16 IU/L, P!0.01), PRL (251.52G142.60 vs 370.27G237.74 nmol/l, P!
0.05). There are positive correlations between menopausal duration and waist,
BMI and BP. Negative correlation was found for BMI, menopausal duration
and HDL.
Hypoestrogenic status in the menopausal women shows a shift to a central android
fat distribution and MS that can be counteracted by HRT.
Effects of physiological bell-shaped elevations of free fatty acids on
glucose metabolism and insulin sensitivity in humans
Lars Gormsen, Charlotte Nielsen, Niels Jessen, Esben Vestergaard,
Jens Christiansen, Jens Jørgensen & Niels Møller
Aarhus University Hospital, Aarhus, Denmark.
Physiological elevations of free fatty acids (FFAs) occur in a dynamic bell-shaped
fashion lasting some hours, e.g. nocturnally and during exercise. In order to define
the metabolic role of physiological elevations in relation to diurnal fluctuations in
insulin sensitivity, the present study was designed to identify the metabolic effects
of a dynamic 4 hour elevation of FFAs during a glucose clamp.
Materials and methods
8 lean, healthy men were examined twice in a cross-over design: 1) Control
(saline), and 2) 4 h graded infusion of intralipid (20%)/heparin. Insulin sensitivity
and EGP were assessed by the isotope dilution (3H-glucose) technique during an
8 h hyperinsulinemic-euglycaemic clamp (0.5 mU/kg/min). Before the study, the
protocol was approved by the Aarhus County Ethical Scientific Committee; the
purpose and potential risks of the study were explained to all subjects; and
informed, written consent was obtained from all participants.
Infusion of intralipid caused a significant increase of average FFA levels (Area under
the curve (AUC)) compared with saline reaching peak levels w1.9 mmol/L and
markedly impairing insulin sensitivity [iAUCglucose Rate of disappearance (Rd)
(mg/kg): 709G25 vs. 380G112, PZ0.04). There was a lag phase of 300 minutes
from initiation of intralipid infusion until glucose Rd was significantly reduced.
Glucose Rd returned to control levels after a further 150 minutes. Average insulin
sensitivity was negatively correlated with average FFA level (r2Z0.52, PZ0.002).
EGP was equally suppressed by hyperinsulinaemia regardless of treatment.
Our data suggest that physiological FFA elevations induce insulin resistance in the
periphery after a lag of 4–5 h and that normal insulin sensitivity is restored 1–2 h
after FFA values have returned to normal. It is therefore likely that FFA plays an
important role in circadian variations of insulin sensitivity (e.g. the Dawn
phenomenon and during exercise).
The metabolic changes induced by glucocorticoids: involvement of
AMP-activated protein kinase
Mirjam Christ-Crain1, Blerina Kola1, Francesca Lolli1, Csaba Fekete2,
Dalma Seboek3, Gabor Wittman2, Sharon Ajodha1, Judith Harvey-White4,
George Kunos4, Beat Mueller3, Giorgio Amaldi5, Gilberta Giacchetti5,
Marco Boscaro5, Ashley Grossman1 & Marta Korbonits1
Dept of Endocrinology, William Harvey Research Institute, Barts and
The London, Queen Mary School of Medicine, University of London,
EC1M 6BQ London, United Kingdom; 2Dept of Neurobiology, Institute of
Experimental Medicine, Hungarian Academy of Sciences, Budapest,
Hungary; 3Dept of Endocrinology, University Hospital Basel, Basel,
Switzerland; 4Laboratory of Physiological Studies, National Institute of
Alcohol Abuse and Alcoholism, National Institutes of Health, Bethesda,
United States; 5Dept of Internal Medicine, University of Ancona, Ancona,
Excess glucocorticoids result in Cushing’s syndrome (CS) which is characterised by
increased food intake, central obesity, dyslipidaemia and insulin resistance, leading
to the metabolic syndrome. AMPK is a regulator of energy homeostasis and plays an
important role in the regulation of appetite, glucose uptake, lipogenesis and
gluconeogenesis. We hypothesised that the effects of corticosteroids on metabolism
would be mediated by changes in AMPK activity in a tissue-specific manner.
Rats were implanted with corticosterone-containing pellets and consumed chow
and 30% sucrose for 2 weeks. Control animals were implanted with cholesterol
pellets consuming sucrose or saline only. AMPK activity (kinase assay), metabolic
enzyme expression (qRT-PCR) and hypothalamic endocannabinoid content were
measured. Human visceral fat tissue of patients with CS was analysed for AMPK
activity and compared to controls. In vitro experiments using human ex vivo
differentiated adipocytes and a human hepatoma cell line.
Corticosterone-treated rats demonstrated higher insulin, leptin, cholesterol and
triglyceride levels and an increase in visceral fat weight (to 129G5% of controls;
meanGSEM). The AMPK activity in the visceral fat of corticosterone-treated rats
and CS patients was significantly lower compared to controls. The gene expression
of gluconeogenic and adipogenic enzymes was increased in adipose tissue. The data
on AMPK were confirmed in human adipocytes treated with dexamethasone for
24 h. In the liver, fat content was increased concomitant with an increased AMPK
activity. In the heart a decrease in AMPK was observed, consonant with the
cardiomyopathy observed in humans. In the hypothalamus, AMPK and the
endocannabinoid content were increased concordant with the increased appetite
typical of CS.
We demonstrate that corticosteroids change AMPK activity in various tissues in a
manner that may explain the increase in food intake, lipid deposition in visceral
adipose and hepatic tissue and the peripheral cardiac effects of Cushing’s syndrome.
Net endogenous acid production and circulating leptin are associated
with potentially bioactive free glucocorticoids in healthy lean women
Christiane Maser-Gluth1, Triantifillia Dimitriou2 & Thomas Remer2
Dept of Pharmacology, University of Heidelberg, Heidelberg, Germany;
Research Institute of Child Nutrition, Dortmund, Germany.
Recent evidence suggests that endogenous glucocorticoids (GC) may be
suppressed by adipocyte-derived leptin and elevated by dietary acidity. Therefore
we examined whether these factors might be predictors of potentially bioactive
free glucocorticoids independently of adrenocortical activity.
Body composition, plasma cortisol, plasma leptin, 24-h urinary excretion rates of
net acid (NAE) reflecting daily diet-dependent acid load, total nitrogen, urinary
free cortisol (UFF), free cortisone (UFE), the main GC metabolites tetrahydrocortisone (THE), tetrahydrocortisol (THF) and 5alpha-tetrahydrocortisol
(alloTHF) were examined cross-sectionally in 30 healthy adults (15 females;
22–44 yr old; BMI: 20–25 kg/m). Adrenocortical activity (AA) was assessed by
the sum of the 3 major glucocorticoid metabolites (THECTHFCalloTHF),
reflecting overall daily cortisol secretion. As a measure of potentially bioactive
free GCs (bioactiveGCs) the sum of free cortisol and cortisone in urine (UFFC
UFE) was taken, reflecting the free fraction of circulating cortisol and cortisone.
Plasma leptin (meanGSD, 2.8G1.6 vs. 7.6G4.9 ng/mL) and percent body fat
(%BF, 16.8G4.2 vs. 26.9G4.9%) were lower (P!0.01) and body surface (BS)corrected AA higher (P!0.01) in males, whereas plasma cortisol and
Endocrine Abstracts (2007) Vol 14
9th European Congress of Endocrinology, Budapest, Hungary, 2007
BS-corrected bioactiveGCs were statistically undistinguishable between the
sexes. Both bioactiveGCs and AA correlated positively with %BF and leptin in
males (P!0.05), but not in females. After adjusting for AA, NAE was a positive
(PZ0.011) and leptin a negative (PZ0.046) predictor of bioactiveGCs in females
(total explained variability R2Z0.71). In males only AA explained variation of
bioactive-GCs (R2Z0.49, PZ0.004).
Our findings indicate that – at least in females – variability of potentially bioactive
glucocorticoids is not only explained by individual adreno-cortical activity, but may
also be affected by circulating leptin and diet-dependent daily acid load.
In the same cells, rimonabant reduced lipogenic gene expression, in particular of
FAS, ACC, LPL, SCD-1, DGAT-2 mRNAs, whereas WIN55,212 up-regulated these
genes suggesting a stimulatory role of endocannabinoids on fatty acids and
triglycerides biosynthesis.
All together, these results indicate that endocannabinoid system is able to stimulate
differentiation of pre-adipocytes towards adipocytes and to directly influence several
metabolic processes of these cells including their secretory profile.
Serum gamma-glutamiltransferase increases in type 2 diabetes mellitus
but it is not related with the body mass index
Juan Carlos Ferrer-Garcı́a, Xelo Garcı́a-Fabra, Raquel Albalat-Galera,
Patricia Sánchez-Llópez, Agustı́n Herrera-Ballester & Carlos Sánchez Juan
Unit of Diabetes and Endocrinology, Department of Internal Medicine,
University General Hospital, Valencia, Spain.
Absence of TSH-induced increase in leptin levels in patients with history
of differentiated thyroid carcinoma undergoing rhTSH testing
Francesca Cecoli1, Gabriella Andraghetti1, Carla Ghiara2, Lucia Briatore1,
Domenico Cavallero1, Michele Mussap2, Francesco Minuto1 &
Massimo Giusti1
Dipartimento di Scienze Endocrinologiche e Metaboliche, Azienda
Ospedaliera Universitaria San Martino, Genoa, Italy; 2U.O. Laboratorio
Analisi, Azienda Ospedaliera Universitaria San Martino, Genoa, Italy.
We have examined the relationship between the hepatic enzymes and type 2
diabetes. We have analyzed if the levels of hepatic enzymes are associated with
body weight, lipid profile and the treatment with metformin, thiazolidinediones or
318 patients with type 2 diabetes were included and they were compared with 100
healthy subjects. Alanine aminotransferase (ALT), aspartate aminotransferase
(AST) and gammaglutamiltranspeptidase (GGT) were measured. We studied the
lipid profile, the weight and the treatment with metformin, thiazolidinediones and
statins, analyzing possible differences in hepatic function.
Type 2 diabetic patients showed significantly increased levels of GGT that the
population control (48.3G5.2 vs 25.6G2.1 U/l respectively; P!0.01). The
difference was confirmed after adjustment for age, sex and body mass index
(BMI). There were no differences in the levels of ALT, AST. Levels of GGT
upper the normality were presented in 33.0% of type 2 diabetic patients and
13% of healthy subjects. The diabetic subjects showed higher triglycerides
and more reduced LDL-c and HDL-c levels. Lipid profile and body weight
were not correlated by the hepatic function. The diabetic patients treated with
metformin presented lower levels of ALT (31.3G2.7 vs 22.1G2.2 U/l; P!
0.05). There were no differences in patients treated with statins or
Increased levels of GGT are closely associated with type 2 diabetes, and this
association is independent of the BMI. Metformin has been associated with
reduced levels of ALT.
Some extra-thyroid effects of TSH have been described in vitro and in vivo.
TSH has recently been suggested to induce IL-6 secretion from adipocytes.
Leptin is the main secretory protein from adipose tissue. Our aim was to
evaluate the acute effect of rhTSH-induced TSH surge on serum leptin levels
in differentiated thyroid carcinoma (DTC) patients. Ten patients (2 m, 8 f; age
range 31–66 years) with stage 1-3 DTC were evaluated during scheduled
standard rhTSH testing. Leptin, thyroglobulin (Tg) and TSH were measured,
before and after rhTSH administration (0.9 mg i.m. for 2 consecutive days).
L-T4 therapy ranged from 575 to 1050 mg/week and f-T4 levels ranged from
8 to 23 pg/ml. According to BMI data, only 2 patients were obese. One
patient presented a high HOMA-IR (O4). LDL-cholesterol levels were over
130 mg/dl in 50% of patients. Baseline leptin levels were 8.4G1.3 ng/ml.
Only BMI correlated significantly (PZ0.05) with baseline leptin levels. After
rhTSH administration, TSH levels increased significantly (P!0.01), while
thyroid hormones remained unchanged. According to Tg-stimulated levels and
neck sonography, all but 2 patients were considered disease-free. Two patients
were considered partially ablated after post-surgical radioiodine therapy. On
average, leptin levels did not significantly change during rhTSH administration. Twenty hours after the last rhTSH administration, leptin levels were
8.6G1.4 ng/ml, maximal leptin levels being recorded after 1 week (8.9G
1.5 ng/ml). No correlation between maximal TSH and leptin levels after
rhTSH was noted. In conclusion our in vivo experimental model suggests that
acute TSH increase after rhTSH testing is uneffective on circulating leptin.
These results are in contrast with some literature data reporting an in vivo
correlation between leptin and TSH in hypothyroid, hyperthyroid and obese
Effects of pharmacological stimulation or blockade of cannabinoid
receptor type 1 (CB1) on gene expression in mouse cultured adipocyte
Luigi Bellocchio, Cristina Cervino, Flaminia Fanelli, Valentina Vicennati,
Renato Pasquali & Uberto Pagotto
Endocrine Unit and C.R.B.A. Hospital S.Orsola-Malpighi, Bologna, Italy.
Serum visfatin in relation to insulin resistance and markers of
hyperandrogenism in lean and obese women with polycystic ovary
Irina Kowalska, Marek Straczkowski, Agnieszka Nikolajuk,
Agnieszka Adamska, Monika Karczewska-Kupczewska,
Elzbieta Otziomek, Slawomir Wolczynski & Maria Gorska
Department of Endocrinology, Diabetology and Internal Medicine, Medical
University of Bialystok, Bialystok, Poland; Department of Reproduction
and Gynecological Endocrinology, Medical University of Bialystok,
Bialystok, Poland.
The endocannabinoid system has recently emerged as an important modulator of
several functions of adipose tissue by altering cell proliferation and gene expression.
In this work, we investigated the effects of CB1 activation/blockade in mouse 3T3L1 adypocite cells by using WIN55,212, a CB1/CB2 agonist and rimonabant, a
specific CB1 antagonist, in different experimental settings such as acute treatment on
pre-adipocytes and on mature adipocytes, and chronic treatment during differentiation process. The gene expression was first analyzed by semi-quantitative RT-PCR
and then confirmed by Real-TIME PCR for selected genes. We found that CB1 and
FAAH mRNAs were both up-regulated by WIN55,212 and down regulated by
SR141716, this effect was stronger in pre-adipocytes than in mature adipocytes.
Furthermore, in pre-adipocytes, rimonabant was able to down-regulate PPAR-g
expression, whereas WIN55,212 gave an opposite effect. Moreover, rimonabant was
also able to stimulate UCP1 and UCP2 mRNA expression.
Among adipokynes, adiponectin mRNA has been shown to be down-regulated by
WIN55,212 and up-regulated by rimonabant, whereas visfatin, apelin and IL-6
mRNAs resulted up-regulated by WIN55,212 and down regulated by rimonabant.
Endocrine Abstracts (2007) Vol 14
Visfatin is a newly discovered protein secreted by adipose tissue, which is
suggested to play a role in pathogenesis of insulin resistance. Polycystic ovary
syndrome (PCOS) is heterogeneous disorder, where insulin resistance might be
involved in the development of endocrine and metabolic abnormalities. The aim
of the present study was to asses the relation between serum visfatin and insulin
sensitivity and markers of hyperandrogenism in a lean and obese PCOS patients.
The study group consisted of 70 women with PCOS (23 lean and 47 overweight or
obese) and 45 healthy, normally menstruating women (25 lean and 20 overweight
or obese). Euglycemic hyperinsulinemic clamp and the measurements of serum
visfatin and sex hormones were performed. PCOS group had lower insulin
sensitivity (PZ0.00004) and higher serum visfatin concentrations (PZ0.026) in
comparison to controls. The decrease in insulin sensitivity was present both in
9th European Congress of Endocrinology, Budapest, Hungary, 2007
lean (PZ0.0053) and in obese (PZ0.017) PCOS subjects, whereas increase in
serum visfatin was observed only in lean PCOS (PZ0.013). In the whole studied
group, serum visfatin was negatively related to insulin sensitivity (rZK0.27, PZ
0.004). This relationship was also observed in the subgroup of lean (rZK0.30,
PZ0.038), but not obese women. Additionally, in lean women visfatin was
associated with serum testosterone (rZ0.47, PZ0.002) and free androgen index
(rZ0.48, PZ0.002), independently of other potential confounding factors.
Obtained results pointed out that visfatin could play a role in pathogenesis of
PCOS in lean women.
Relationship between serum adiponectin and oxidative and nonoxidative glucose metabolism in apparently healthy humans
Agnieszka Adamska, Marek Straczkowski, Irina Kowalska,
Agnieszka Nikolajuk, Monika Karczewska-Kupczewska,
Malgorzata Karolczuk-Zarachowicz, Elzbieta Otziomek & Maria Gorska
Department of Endocrinology, Diabetology and Internal Medicine, Medical
University of Bialystok, Bialystok, Poland.
The pathogenesis of insulin resistance is not completely understood, however,
there are data that it might be associated with altered tissue carbohydrate and
lipid oxidation. Adiponectin may be a key regulator of insulin sensitivity and
energy metabolism. The aim of the present study was to determine the
association of adiponectin, glucose metabolism (oxidation and storage) and
lipid oxidation by applying the euglycemic clamp technique and indirect
The study was carried out on 68 young (age 26.38G6.82 yr (meanGS.D.),
BMI: 29.15G7.24 kg/m2 (meanGS.D.)) people. Anthropometric and biochemical parameters were measured and oral glucose tolerance test was
performed. Plasma adiponectin was measured with radioimmunoassay (RIA)
kit. Insulin sensitivity was evaluated with the euglycemic hyperinsulinemic
clamp technique. Whole-body fat and carbohydrate oxidation was measured
by indirect calorimetry at baseline (in the fasting state) and during last
30 minutes of the clamp. Nonoxidative glucose disposal rate was calculated
by subtracting glucose oxidation rate from GDR.
Plasma adiponectin was positively related to insulin sensitivity (rZ0.477, PZ
0.000038), glucose oxidation at the steady state (rZ0.326, PZ0.006) and nonoxidative glucose metabolism (rZ0.424, PZ0.0003) and was negatively
associated with FFA at the end of the clamp and fat oxidation during
hyperinsulinemia (rZK0.0309, PZ0.0137 and rZK0.260, PZ0.031). Insulin
sensitivity was positively related to fat oxidation during fasting (rZ0.241, PZ
0.04) and carbohydrate oxidation during last 30 minutes of the clamp (rZ0.308,
We conclude that adiponectin modulates insulin sensitivity probably through
influencing both oxidative and non-oxidative glucose metabolism.
Muscle ceramide, sphingosine and sphinganine content and the activities of the
enzymes: neutral and acid sphingomyelinase, neutral and alkaline ceramidase and
serine palmitoyltransferase were measured. Muscle free fatty acid (FFA),
diacylglycerol (DAG) and triacylglycerol (TG) content was also assessed.
Insulin sensitivity was related to circulating cytokines (adiponectin, rZ0.38,
PZ0.021; IL-10, rZ0.47, PZ0.0034; IL-18, rZK0.37, PZ0.023) and to
muscle lipids (ceramide, rZK0.45, PZ0.024; DAG, rZK0.43, PZ0.031;
TG, rZK0.52; PZ0.01). It was also associated with the activities of
the enzymes regulating ceramide metabolism (serine palmitoyltransferase,
rZK0.58, PZ0.002; alkaline ceramidase, rZK0.37, PZ0.025). Adiponectin
was negatively related to muscle ceramide content (rZK0.44, PZ0.027) and
to serine palmitoyltransferase activity (rZK0.35, PZ0.032). IL-10 and IL-18
were associated, in an opposite manner, with muscle DAG (IL-10, rZK0.46,
PZ0.022; IL-18, rZ0.40, PZ0.049) and muscle TG (IL-10, rZK0.50, PZ
0.014; IL-18, rZ0.46, PZ0.026). IL-10 was also related to muscle FFA pool
(rZK0.51, PZ0.026).
We conclude that there are multiple associations between circulating
cytokines and muscle lipid pool, which possibly might influence insulin
sensitivity. Adiponectin is related to muscle ceramide content, mostly through
an association with de novo synthesis pathway. IL-10 and IL-18 are
associated with muscle FFA-DAG-TG pathway.
Prevalence of metabolic syndrome in old men and its relation to ghrelin
Sergio Rueda Alfaro1, Mateu Serra-Prat2, Cristián Fernández Fernández1,
Elisabet Palomera2, Roser Casamitjana1 & Manel Puig Domingo1
Hospital Clinic i Provincial de Barcelona, Barcelona, Spain; 2Hospital de
Mataró, Mataró, Spain.
To study the prevalence of metabolic syndrome (MS) and its relation with ghrelin
in old men.
Material and methods
Prospective-population based study (2002–2005) in which 153 independently
living men older than 70 y were included. Comorbidities, physical exam, BMI,
blood pressure were recorded and blood sample taken for biochemical and
hormonal determinations. Metabolic syndrome was defined using IDF criteria.
MS was found in 54.9%; BMI in non-MS individuals was 25.8G3.3 and in MS
was 28.3G3.7 (P!0.001). No association was found between ghrelin and MS at
basal evaluation (non-MS 1185G445 vs MS 1106G368; p:ns), even after weight
At 3 years follow-up ghrelin level in MS were lower than in non-MS individuals
(non-MS 1165.8G356.0 vs MS 988.4G245.8; P:0.004). Differences between
ghrelin levels at the two time-points was only statistical significant in MS group
(P:0,006). Ghrelin correlated with BMI (rZK0.22; PZ.023) in subjects between
70–80 years and with creatinina !1.5 mg/dl. Also a correlation was found with
HDL (rZ0.21; PZ.012). Multiple lineal regression analysis showed than age
(betaZK12.1; PZ.049), BMI (betaZK22.0; PZ.021) and creatinine (betaZ
407.7; PZ.002) had an independent effect on circulating ghrelin.
MS in old men is associated to a decrease in circulating ghrelin over time.
Relationships between serum adiponectin, interleukin 10 and interleukin 18 concentrations and muscle lipid fractions in healthy humans
Marek Straczkowski1, Irina Kowalska1, Agnieszka Nikolajuk1,
Marcin Baranowski2, Agnieszka Adamska1, Malgorzata Karolczuk-Zarachowicz1, Monika Karczewska-Kupczewska1, Piotr Zabielski2,
Agnieszka Blachnio2, Jan Gorski2 & Maria Gorska1
Department of Endocrinology, Diabetology and Internal Medicine,
Medical University of Bialystok, Bialystok, Poland; 2Department of
Physiology, Medical University of Bialystok, Bialystok, Poland.
Intramuscular lipids, including ceramide, might be responsible for the
development of insulin resistance. Insulin action is also inversely associated
with circulating proinflammatory cytokines, like interleukin (IL)-18 and
positively related to antiinflammatory factors, like adiponectin and IL-10. The
aim of the present study was to estimate the relationships between serum
adiponectin, IL-10 and IL-18 concentrations and muscle lipid fractions in healthy
The study group consisted of 37 male subjects with normal glucose tolerance,
without morbid obesity or other serious medical problems. Euglycemic
hyperinsulinemic clamp and a biopsy of vastus lateralis muscle were performed.
Antipsychotic drugs and associated metabolic disorders
Kolcsár Melinda, Nagy Réka, Nagy Imre, László Annamária &
Kun Imre Zoltán
U.M.Ph – Department of Pharmacology and Endocrinology, Tg.Mures,
Obesity is a major contributor to a range of metabolic disorders responsible
for much of the medical morbidity and mortality. Increasing numbers of
reports concerning not only obesity, but diabetes, hyperglycaemia and lipid
dysregulation in patients treated with antipsychotics have raised concerns
about a possible association between these metabolic effects and treatment
with these medications. The objective of our study was to investigate the
prevalence of obesity and other metabolic disorders in young patients treated
with different antipsychotics and in the age matched general population.
Endocrine Abstracts (2007) Vol 14
9th European Congress of Endocrinology, Budapest, Hungary, 2007
Antropometric and metabolic data of the patients treated with psychotropics,
hospitalized in the Endocrinology Clinic, Tg. Mures, between years 2001–
2005 were compared with the data of persons selected among patients
hospitalized in the same clinic and period, without psychotropic drug use. The
frequency of patients treated with antipsychotics was 10.92% (4.33% typical
antipsychotics and 6.59% atypical antipsychotics) with 43.1G13.6 years of
mean age. In this patients the prevalence of obesity, elevated total cholesterol
and triglyceride level was significantly higher than in the control group. The
blood sugar didn’t present difference between the two groups, but measuring
HOMA-IR in 25 patients treated with atypical psychotropics and 20 other
persons without treatment with psychotropic drug we found a significant
difference between them. We concluded that a complete metabolic syndrome
(MS) was present in 34.2% of the patients treated with antipsychotic drugs,
while the frequency of MS was only 18.7% in the age matched patients group
without any psychotropic drug use. Atypicial antipsychotics causes the most
severe metabolic disorders in association with a significantly elevated
prolactin level, when compared with the control group. The choice of a
second generation antipsychotic for a given patient depends on many factors.
The likehood of developing severe metabolic disease should also be an
important consideration.
Associations between thyroid function parameters and adipokines in
euthyroid individuals
Laszlo Bajnok1, Ildiko Seres2, Zsuzsa Varga2, Sara Jeges1, Attila Peti1,
Zsolt Karanyi2, Attila Juhasz2, Eva Csongradi2, Emese Mezosi1,
Endre V Nagy2 & Gyorgy Paragh2
School of Medicine, University of Pécs, Pécs, Hungary; 2University of
Debrecen, Medical and Health Science Center, Debrecen, Hungary.
Adipose tissue secreted hormonal mediators, adipokines play pivotal roles in the
regulation of, among others, central nervous and immune systems influencing
body weight, insulin action and inflammatory responses. The aim of our present
study was to investigate possible associations of thyroid function with plasma
levels of three of known adipokines, i.e. leptin, adiponectin and resistin in 74
Caucasian subjects without any endocrine diseases or related therapy. In order to
create broad adipokine ranges, 3 age-, and sex-matched groups were formed:
Group 1 and 2 consisted of non-diabetic obese patients (nZ25 with BMI: 28–
39.9 kg/m2, nZ25 with BMI R40 kg/m2, respectively), while Group 3 of 24
healthy, normal weight control subjects. Level of TSH was correlated negatively
with leptin (rZK0.26, P!0.05), while positively with adiponectin (rZ0.28,
P!0.05). Both were independent predictors of TSH level in a multiple regression
model including BMI, age, gender, FT3 or FT4. But when both leptin and
adiponectin were included into the model, only the latter remained significant.
In opposite to TSH, level of FT3 was negatively associated with adiponectin
(rZK0.27, P!0.05) and showed a positive trend with leptin (rZ0.26, PZ0.06)
of which the latter was independent predictor in multivariate analyses, beside age,
BMI and FT4. FT4 was not correlated with any of adipokines. In univariate
analysis, neither BMI, nor resistin was significantly correlated with thyroid
function parameters.
In conclusion, in individuals without thyroid illness, leptin and adiponectin
plasma levels are associated with TSH and FT3 concentrations in opposite ways,
and partly independently of anthropometric parameters. Adipokines may
participate in the regulation of thyroid hormone axis.
10 yrs, nZ18). Isolated AbdSc adipocytes were treated with 1–100 nM rhNPY
with and without DPP-IV inhibitors; a glycerol release assay was used as an index
of lipolysis and DPP-IV mRNA expression assessed in AbdScAT. Treatment with
NPY reduced glycerol release which was further blunted by co-incubation with
DPP-IV inhibitors (baseline 234(meanGS.E.)G23 mmol/l, NPY100: 187G
30mmol/l*; NPY100 with DPP-IV: 121G14 mmol/l**, *P!0.01, **P!0.01,
nZ8). Relative DPP-IV mRNA expression was reduced in AbScAT taken from
obese subjects versus lean subjects (obese: 77G6 SU versus lean: 186G29 SU*,
In conclusion, paracrine effects of NPY may be modulated by AT-derived DPPIV. Thus DPP-IV inhibitors may have little effect on tissue mass regulation in the
obese where endogenous DPP-IV from AT is reduced, but may enhance fat
accumulation in the lean through enhanced antilipolytic effects of NPY, which
requires further study.
The role of nitric oxide in pathogenesis of development of arterial
hypertension during obesity
Diana Giorgadze1, Ellen Giorgadze1, Tamar Doliashvili1,
Tamar Sanikidze2, Ketevan Asatiani1, Ketevan Bochorishvili1 &
Arkadi Surmava1
N4 clinical hospital, Tbilisi, Georgia; 2State Medical University, Tbilisi,
The cardiovascular complication is the main cause of morbidity and mortality in
obese patients. Endothelial dysfunction and atherosclerosis have the goal role in
development of these diseases. The aim of our study was to reveal the role of
nitric oxide during obesity associated arterial hypertension.
Subject and method
200 obese patients (age 35–55) were investigated. Control group comprised 25
healthy subjects. We calculated BMI, determined lipid profile, concentration of
nitric oxide, activity of antioxidant enzymes – superoxiddismutase and katalaze,
evaluated arterial pressure.
Systolic arterial pressure insignificantly increased in overweight group (nZ50)
compared to control group (124.3G5.6 mm/hg), but significantly (P!0,05) – in
patients with obesity of I (nZ50) (134.4G11.7 mm/hg), II (nZ50) (142.6G
12.6 mm/hg) and III (nZ50) (145.7G10.3 mm/hg) degree. Diastolic arterial
pressure significantly (P!0.05) increased in patients with obesity of II (91.8G
9.4 mm/hg) and III (95.6G7.2 mm/hg) degree compared to control group (81.4G
6.2 mm/hg). According to weight gain the whole lipid profile (Chol, Trig, HDL,
LDL) was damaged. Concentration of nitric oxide significantly reduced in obese
subjects compared to control group. Significant decrease of nitric oxide in different
BMI groups was revealed (overweight-11.875G0.427, I degree-11.2154G0.3113,
II degree-10.2364G0.381, III degree-9.5G0.2823 P!0,001). Changes in concentration of NO correlated with decrease of antioxidant enzymes activity (enzymes
activity decrease compared to control group and increase according to weight gain).
Hyper generation of oxygen causes inactivation of antioxidant enzymes and
disorders in redox-status. NO oxidative degradation, stimulated by dyslipidemia,
has the main role in the pathogenesis of arterial hypertension development during
Human adipose tissue derived DPP-IV regulates lipolysis through NPY
in cultured abdominal subcutaneous adipocytes
Katarina Kos, Adam Baker, Alison Harte, Philip McTernan, Paul O’Hare &
Sudhesh Kumar
University of Warwick, Coventry, United Kingdom.
Effects of PGC-1a on endothelial function and apoptosis
Joong-Yeol Park1, Jong Chul Won1, Ki-Up Lee1, Woo Je Lee2, Kyung
Soo Ko2, Kee-Ho Song3 & In-Kyu Lee4
University of Ulsan College of Medicine, Seoul, South Korea; 2Inje
University College of Medicine, Seoul, South Korea; 3Konkuk University
School of Medicine, Seoul, South Korea; 4Kyungpook National University,
Daegu, South Korea.
We have previously shown that the orexigenic hormone NPY is secreted by
human adipocytes. The orexigenic hormone NPY(1–36) is truncated by the
dipeptidyl-inhibitor IV (DPP-IV) to NPY(3–36) as consequence its affinity
changes from receptor Y1 to Y4 and 5. The aim was to investigate whether DPPIV is expressed in adipose tissue (AT) where it could modulate adipose tissue
growth through modulation of NPY activity. This is relevant in light of DPP-IV
inhibitors utilised as therapeutic agents and their use for treatment in Type 2
diabetes. For this purpose ex vivo human abdominal AT was taken from women
undergoing elective surgery (BMI: 27.5(meanGS.D.)G5 kg/m2, Age: 43.7G
Endocrine Abstracts (2007) Vol 14
Central obesity is associated with increased cardiovascular morbidity and
mortality. It has been proposed that increased lipid accumulation in vascular
tissue and the consequent increase in oxidative stress may be a missing link
between obesity and atherosclerosis. The peroxisome proliferators-activated
receptor (PPAR)-g coactivator 1-a (PGC-1a) is a transcriptional coactivator
playing an important role in energy metabolism. PGC-1a is present in vascular
9th European Congress of Endocrinology, Budapest, Hungary, 2007
cells, but its role in vascular endothelial cells has not been established. In this
study, we examined the effect of adenoviral overexpression of PGC-1a (Ad-PGC1a) in human aortic endothelial cells (HAECs) on apoptosis induced by linoleic
acid (LA).
Effect of PGC-1 on HAECs apoptosis was evaluated by ELISA, WST-1 assay,
and caspase activity. Using Ad-PGC-1 and ANT-1 siRNA, effect of PGC-1 and
ANT-1 on reactive oxygen species (ROS) production, fatty acid oxidation (FAO)
and mitochondrial membrane potential (Djm) were analyzed.
PGC-1a prevented LA-induced endothelial apoptosis. PGC-1a also reduced
LA-induced increases of antioxidant enzyme expression and ROS accumulation
at basal state. LA decreased the activity of adenosine nucleotide translocase
(ANT), and increased Djm. In the Ad-PGC-1a-infected HAECs, activity and the
mRNA expression of ANT-1 were increased and LA did not increase Djm.
siRNA against ANT-1 reversed the changes induced by PGC-1a.
These data suggest that PGC-1a functions as a physiologic regulator of ROS
generation in endothelial cells and that part of this effect is mediated by ANTdependent increase in FAO.
Changes in serum glucose metabolism and growth hormone, cortisol,
prolactin, ghrelin, leptin concentrations in normal weight patients with
schizophrenia before treatment with atypical antipsychotics
Mirjana Doknic1, Nadja Maric2, Sandra Pekic1, Aleksandar Damjanovic2,
Dragana Miljic1, Marko Stojanovic1, Marina Djurovic1, Miroslava JasovicGasic2, Carlos Dieguez3, Felipe Casanueva4 & Vera Popovic1
Institute for Endocrinology, Diabetes and metabolic Diseases, Belgrade,
United States; 2Institute for Psychiatry, Belgrade, United States; 3Departement of Physiology, School of Medicine, and Comlplejo Hospitalario
Universitario de Santiago, Santiago de Compostela, Spain; 4Departement of
Medicine, School of Medicine, and Complejo Hospitalario Universitario de
Santiago, Santiago de Compostela, Spain.
Schizophrenia is a devastating mental illness associated with obesity and diabetes
mellitus rates that far exceed those of the general population.
The aim was to evaluate changes in positive energy balance (serum insulin, leptin
and ghrelin) and hormones involved in neuroendocrine regulations (serum
cortisol, growth hormone and prolactin) before treatment with atypical
antypsyhotics (SGA) in normal weight patients with schizophrenia.
Thirty patients with schizophrenia (13 males, mean age 28.9G1.3 years and BMI,
23.3G0.6 kg/m2) treated with antypsyhotics first generation were investigated in
this study. They had neither other diseases. The control group included 27 healthy
subjects (9 males, mean age 30.7G1.9 years, BMI od 22.8G0.6 kg/m2). Positive
family history for diabetes mellitus was similar between groups.
A oral glucose tolerance test (OGTT) with measuring glycemia, insulin, growth
hormone and ghrelin was performed in all patients. Fasting samples for leptin,
cortisol and prolactin were taken. Patients had normal fasting glucose levels but
significantly higher peak glucose levels during OGTT as well as glucose area
under the curve (AUC) than control subjects (746G25 vs 650G
26 mmol/L/120 min; P!0.01). Fasting insulin levels, as well as insulin AUC
did not differ from control subjects at baseline (PO0.05) but peak insulin values
were significantly higher in patients with schizophrenia (95.1G14.8 vs 52.2G
6.5 mU/L, P!0.05). Growth hormone (GH) and ghrelin levels during OGTT, and
leptin concentrations did not differ between patients and control subjects (PO
0.05). Cortisol levels (513.3G29.1 vs 441.9G24.3 nmol/L; P!0.05) were higher
in patients. Prolactin levels were higher in patients with schizophrenia than in
control subjects (821G135 vs 353G45 mU/L; P! 0.01).
Normal weight patients with schizophrenia have already some abnormalities
in glucose metabolism therapy and neuroendocrine responses (cortisol,
prolactin) before SGA. Thus, shizophrenia could be per se risk factor for
diabetes mellitus.
The aim of our study was to determine the frequency of hypogonadism (H) in
males with type 2 diabetes (T2D) and its relation with erectile dysfunction (ED)
and obesity.
We studied 107 diabetic males who came successively to an Endocrine
consultation. The presence of H was determined by total testosterone (T) with
an immunofluerescence method and free testosterone (fT) calculated with
Vermeulen’s equation, defining H if T!2 ng/ml or fT!250 pmol/l, with LH,
FSH and prolactine in the normal range. We studied ED by means of the
International Index of Erectile Dysfunction (IIEF) (questions 1 to 5 and 15 that
determine ED). We excluded patients taking drugs that cause ED and those
diagnosed of severe autonomic neuropathy. The anthropometic parameters
analyzed were weight, height, waist perimeter and the calculated body mass index
We included 107 patients, aged 55.1G7.8 years (range 39–70) with an average of
duration of T2D of 8.2G8.1 years (range 1–32). The frequency of H was 22.4%.
The average of LH was 3.7G1.7 mU/ml (range 1.1–9.5), FSH 5.1G2.3 mU/ml
(range 1.2–13.3) and prolactine 8.5G2.9 ng/ml (range 2.9–16.5). ED was present
in 66.7% of hypogonadal males and 66.7% of patients not presenting H. Patients
with H had more weight (93.2G11.9 vs 84.8G13.8 kg, PZ0.016), more BMI
(31.8G3.8 vs 29.6G3.8 kg/m2, PZ0.025) and more waist perimeter (111.1G9.2
vs 104.7G10.7 cm, PZ0.028), compared to patients without H. The table below
show the means of T and fT according to BMI:
BMI (kg/m2)
T (ng/ml)
fT (pmol/l)
The frequency of H is 22.4%. ED appears in the same proportion in patients with
and without H. Hypogonadal patients are more obese and there is an inverse
relation between BMI and T and fT.
Acute phase reactants and soluble cell adhesion molecules are
associated to plasma leptin levels in obese nondiabetic children
Barbara Garanty-Bogacka, Malgorzata Syrenicz, Anhelli Syrenicz,
Aneta Gebala, Grazyna Dawid & Mieczyslaw Walczak
Pomeranian Medical University, Szczecin, Poland.
There are increasing evidences that leptin, a protein secreted by adipose tissue,
may be an important factor contributing to the development of atherosclerosis.
In this study, the relationship between plasma leptin levels and markers of
inflammation and endothelial activation was investigated in 214 obese
nondiabetic children and adolescents. Fasting levels of leptin, C-reactive
protein (CRP), fibrinogen (FB), interleukin-6 (IL-6), interleukin-1b (IL-1b),
intercellular cell adhesion molecule-1 (ICAM-1), vascular cell adhesion
molecule-1 (VCAM-1), von Willebrand factor (vWF), glucose and insulin
were determined. Insulin resistance was assessed by the homeostasis model. At
multiple regression analysis leptin predicted IL-6, FB, ICAM-1, VCAM-1 and
vWF independently of obesity measures and HOMA IR. There was a trend for
association between leptin and CRP concentrations. Therefore, our findings
showed that leptin levels is associated with inflammation and endothelial
activation markers and in such way may promote the development of
attherosclerosis relatively early in life
Frequency of hypogonadism in males with type 2 diabetes and its
relation with erectile dysfunction and obesity
Katherinne Garcı́a-Malpartida, Rosa Casañ-Fernández, Jesús Yanini-Garcı́a, Ana Jover-Fernández, Marcelino Gómez-Balaguer, Eva Solá-Izquierdo,
Carlos Morillas-Ariño & Antonio Hernández-Mijares
Hospital Universitario Dr. Peset, Valencia, Spain.
Relationship between homocysteine level and low-grade systemic
inflammation in obese children with metabolic syndrome
Justyna Syrenicz & Barbara Garanty-Bogacka
Pomeranian Medical University, Szczecin, Poland.
Obesity is an independent risk factor for the development of cardiovascular
disease, frequently associated with various metabolic disorders defined as
metabolic syndrome. High plasma total homocysteine (Hcy) concentration is
Endocrine Abstracts (2007) Vol 14
9th European Congress of Endocrinology, Budapest, Hungary, 2007
now well established as a powerful risk indicator for a wide range of vascular
The aim of this study was to investigate total Hcy levels in obese children and
their possible association with both metabolic syndrome and various
inflammatory biomarkers.
The study group consisted of 61 obese children, (aged 6–18 y.) with metabolic
syndrome, defined according to NCEP-ATP III criteria and 122 obese
counterparts without metabolic syndrome. Both group were comparable
regarding to age, sex, and pubertal development.
The obese subject with metabolic syndrome presented significantly higher
values for fasting insulin (P!.001), HOMA IR (P!.001), C-reactive proteine
(P!.01), interleukin-6 (P!.001), interleukin-1ß (P!.01), and WBC (P!
.001). In the group with metabolic syndrome plasma Hcy concentration was
positively correlated with insulin (P!.001), HOMA IR (P!.01), C-reactive
protein (P!.001), interleukin-6 (P,.01) and WBC (P,.05), but not in the group
without metabolic syndrome.
Elevated plasma Hcy level in obese children with metabolic syndrome, may be
causally involved in the pathogenesis of cardiovascular disease.
Obesity and metabolism – presented on Tuesday
Oxidative stress and antioxidant defense is associated with adiposity in
men among the urban population of south Iran
Fariborz Haghparast & Jaffar Nourooz-Zadeh
Islamic Azad University-Larestan Branch, Larestan, Fars, Iran.
Changes in lifestyle have resulted in an increased number of boese subjects, and
obesity is currently an important causative factor of health-related problems in
To investigate the direct relationship of oxidative stress and antioxidant status
with obesity in men.
Materials and methods
We measured the plasma levels of malondialdehyde (MDA) as a marker of
oxidative stress and vitamin E, glutathione and superoxide dismutase as
antioxidants in 44 obese and 47 no obese men and evaluated their
relationship with body mass index (BMI); body fat weight; waist-to-hip
ratio (WHR).
Compared with controls, obese men had a significantly higher body mass index
(28.97G2.42 vs. 16.03G1.88 kg/m2; PZ0.0002) and waist-to-hip ratio (WHR)
(0.89G0.03 vs. 0.80G0.01; PZ0.0004); vitamin E, glutathione, superoxide
dismutase, vitamin C levels were significantly decreased (all P!0.05), whereas
MDA was significantly increased (114.9G21.4 vs. 64.3G14.2 nmol/L; PZ
0.001). MDA significantly correlated with BMI (rZK0.34 (PZ0.004)) and
WHR (rZK0.63 (PZ0.0001)). We calculated the amount of vitamin E per
LDL-cholesterol, total cholesterol and total lipids, we found all of them,
significantly lower levels in obese men as compared to controls. There was also
a significant correlation between the plasma levels of MDA and vitamin E,
vitamin C, glutathione and superoxide dismutase in obese men and all men (all
In brief, these findings showed that the circulating levels of oxidative stress
are related to adiposity in men. Although correlation does not prove
causation, the results of this study suggest that obesity is an important factor
for enhanced oxidative stress and important role of oxidative stress
deleterious impact.
Ghrelin basal levels in metabolic syndrome
Tatiana Mokhort
Belarusian State Medical University, Minsk, Belarus; State Research Center
for Radiation Medicine and Human Ecology, Gomel, Belarus.
Ghrelin is known to play an important role in overweight formation and glucose
metabolism regulation. The aim was to assess ghrelin basal secretion features in
persons with metabolic syndrome (MS).
Endocrine Abstracts (2007) Vol 14
We examined 39 patients (age 35–55years) with MS (IDF criteria) and 28 healthy
persons of comparable age. Ghrelin, insulin and C-peptide serum concentrations
were measured by immunoenzyme method, lipid spectrum parameters - by
spectrophotometry. For IR assessment we used HOMA-IR and Reciprocal of
HOMA-IR indexes.
Basal insulinemia and C-peptide levels in S significantly exceeded the ones
in healthy persons: 21.3G3.86 vs 9.96G1.18 mU/l and 2.86G0.56 vs 1.28G
0.76 ng/ml. HOMA-IR in MS significantly exceeded the value of control
group (5.03G1.03 vs 2.06G0.23). Reciprocal of HOMA-IR showed the
opposite results. Ghrelin level was significantly lower in MS 61.06G11.9 vs
88.76G16.9 ng/ml in control group. Progressive decrease of ghrelin from
71.59G7.09 to 50.34G6.58 ng/ml was marked at BMI increase that is
confirmed at correlation analysis: ghrelin levels negatively correlated with
BMI (rZ0.41; P!0.05), waist-to-hip ratio (rZ0.37; P!0.05) and waist
circumference (rZ0.39; P!0.05). Ghrelin levels also showed negative
correlation with systolic (rZ0.40; P!0.01) and diastolic blood pressure (rZ
0.39; P!0.01).
We observed significant negative correlation of ghrelin and insulin (rZ0.18),
C-peptide (rZ0.15), HOMA-IR (rZ0.23) and positive with Reciprocal of
HOMA-IR (rZ0.22). We revealed significant negative correlation of ghrelin
and atherogenecity index (rZ0.32), while there was no significant connection
with other parameters of lipid spectrum.
Progressive decrease of basal ghrelin levels with increase of BMI, waist-to-hip
ratio and waist circumference was revealed that can testify to ghrelin influence on
formation of visceral obesity. Obtained results are proved by negative correlation
of ghrelin level with basal insulinemia, HOMA-IR and positive one with
Reciprocal of HOMA-IR that confirms ghrelin role in formation of insulin
resistance in MS and dictates essential necessity for further studies.
Pioglitazone treatment significantly decreases 5-alpha reductase
activity and improves metabolic risk factors in PCOS
Dorte Glintborg1, Anne Pernille Hermann1, Claus Hagen1,
Johannes Veldhuis2, Anne Schmedes3, Jan Frystyk4, Allan Flyvbjerg4 &
Marianne Andersen1
Department of Endocrinology and Metabolism, Odense University
Hospital, DK-5000 Odense C, Denmark; 2Division of Endocrinology and
Metabolism, Department of Internal Medicine, Mayo Clinical Research
Center, Rochester, United States; 3Department of Clinical Chemistry, Vejle
Hospital, DK-7100 Vejle, Denmark; 4Medical Research Laboratories,
Clinical Institute and Medical Department M (Diabetes and Endocrinology),
Aarhus University Hospita, DK-8000 Aarhus, Denmark.
To investigate the effect of pioglitazone on cortisol metabolism in PCOS.
Thirty insulin resistant PCOS patients were randomized to either 16 weeks
of pioglitazone (30 mg/day) or placebo treatment. Before and after
intervention, patients underwent 24 h 20 min.-integrated blood sampling for
measurement of cortisol and 24 h excretion of cortisol, cortisone and steroid
metabolites (cortisol, corticosteron, androgen, and 17-hydroxyprogesteron)
were measured in urine. Fasting insulin, adiponectin, testosterone, dihydrotestosterone (DHT), and dehydroepiandrosteronsulfate (DHAS) was
measured. 5-alfa reductase activity was evaluated by alloTHF/THF and
androsteron/ethiocholanolon ratios. Delta values (D) denoted changes during
the treatment period.
Pioglitazone treatment was followed by significantly decreased 5-alfa reductase
activity as evaluated by alloTHF/THF levels. D-androsteron/ethiocholanolon
showed a significant negative correlation with D-IGF-I and D-peak GH level
during PD-GHRH test. Furthermore, a significant negative correlation was found
between D- alloTHF/THF and D- adiponectin levels.
No significant changes were measured in 24 h mean cortisol levels or urine
excretion of cortisol, cortisone or steroid metabolites.
Insulin sensitivity, GH, adiponectin, and IGF-I was significantly increased during
pioglitazone treatment.
Pioglitazone treatment was followed by significantly decreased 5-alfa
reductase activity which was inversely correlated with IGF-I, GH, and
adiponectin levels. These results suggest important relations between
5-alfa reductase activity and the GH/IGF-I system as well as metabolic
risk factors.
9th European Congress of Endocrinology, Budapest, Hungary, 2007
Plasma adiponectin and leptin levels in menopausal metabolic
David Virsaladze1, Nona Adamia1, Nino Charkviani1,
Ketevan Khitarishvili1, Tea Giorgadze1 & David Tananashvili2
Tbilisi State medical University, Tbilisi, Georgia; 2E. Andronikashvili
Institute of Physics, Tbilisi, Georgia.
Association of sex hormone-binding globulin (shbg) levels with
measures of adiposity and metabolic profile in apparently healthy
Katerina Saltiki2, Paraskevi Voidonikola3, Kimon Stamatelopoulos3,
Emily Mantzou1, Eleftheria Chryssohoou3, Christos Papamichael3 &
Maria Alevizaki2
Endocrine Unit, Evgenidion Hospital, Athens University School of
Medicine, Athens, Greece; 2Dept Medical Therapeutics, Alexandra
Hospital, Athens University School of Medicine, Athens, Greece; 3Vascular
Laboratory, Dept of Medical Therapeutics, Alexandra Hospital, Athens
University School of Medicine, Athens, Greece.
The aim of our investigation was the study of blood adiponectin and leptin levels
in patients with menopausal metabolic syndrome (MMS) and their correlation
with the parameters of MMS features.
40 females with menopausa have been investigated. In 38 cases diabetes mellitus
type 2 has been registered, and in 2 – impaired glucose tolerance. Mean duration
of postmenopausal period was 11.1G7.4. Control group consisted of 10 females
of postmenopusal age. The blood content of adiponectin and leptin was measured
by ELISA. For MMS diagnostics WHO classification (2002) was applied.
In basic group MMS was revealed in 37 patients, in control group – in 3 cases
(c2Z19.53, P!0,001). It was not observed significant difference in blood
adiponectin levels of basic and control groups (16.4G7.6 vs. 16.3G6.1, PZNS),
but blood leptin level was significantly higher in investigated group in comparison
with control (166.7G105.3 vs. 60.3G51.0, P!0.001). It was revealed significant
correlations of blood adiponectin and leptin levels with the parameters of MMS
Obtained results show that blood adiponectin level in MMS does not differed from
control value. Blood leptin level is significantly higher than control one. They
significantly correlated with the parameters of MMS features.
Serum interleukin 6 and soluble form of interleukin 6 receptor
concentrations in obese subjects with impaired glucose tolerance
Agnieszka Nikolajuk, Marek Straczkowski, Irina Kowalska,
Agnieszka Adamska, Ida Kinalska & Maria Gorska
Department of Endocrinology, Diabetology and Internal Medicine, Medical
University of Bialystok, Bialystok, Poland.
Obesity is associated with an increased risk of impaired glucose tolerance and
type 2 diabetes. Insulin resistance is the link between obesity and disturbances of
glucose metabolism. It is suggested that some substances secreted by adipose
tissue might play a role in the pathogenesis of insulin resistance. One of these
substances is interleukin-6 (IL-6), cytokine, which regulates synthesis of the
acute-phase proteins in the liver. The aim of the present study was to estimate
serum IL-6, soluble form of IL-6 receptor (sIL6-R) and C-reactive protein
concentrations (hs-CRP) in obese subjects with normal and impaired glucose
The study group consisted of 107 subjects, 28 obese with impaired glucose
tolerance (IGT), 44 obese with normal glucose tolerance (obese-NGT) and
35 lean healthy controls. Insulin sensitivity was measured with euglycemic
hyperinsulinemic clamp technique. The protocol was approved by Ethics
Committee of Medical University, and informed consent was obtained from
each subject.
IGT subjects had lower insulin sensitivity index in comparison to obese-NGT and
controls (both P!0.000001), and obese-NGT subjects had lower insulin
sensitivity in comparison to controls (PZ0.00043). We found higher IL-6 and
hs-CRP concentrations in IGT group in comparison to obese-NGT (PZ0.042 and
PZ0.041 respectively) and to controls (PZ0.00056 and P!0.000001
respectively). Differences in sIL-6R concentration between IGT subjects and
the remaining groups were approaching the level of significance (obese-NGT,
PZ0.087, control, PZ0.066). We found significant correlations between insulin
sensitivity index and IL-6 (rZK0.21, PZ0.029), sIL-6R (rZK0.19, PZ0.049)
and hs-CRP (rZK0.34, PZ0.001). IL-6, sIL-6R and hs-CRP were also
associated with fasting insulin and with post load glucose and insulin
concentrations. IL-6 and hs-CRP were also related to triglycerides and HbA1c
and IL-6 was related to HDL-cholesterol.
Our data indicate that IL-6/sIL-6R system might play a role in the development of
insulin resistance in obese subjects with IGT.
The association of SHBG levels with obesity, hyperinsulinemia and metabolic
abnormalities is well recognized in both men and women. Recent data suggest
that SHBG levels are an important predictor of cardiovascular disease (CVD) risk.
Several methods have been used for the measurement of adiposity including
ultrasonography (U/S) which is a reliable and low-cost method. We used U/S to
assess regional adiposity and investigated possible associations with SHBG
309 apparently healthy individuals (124 men and 185 women, mean age 43.9G9)
without a history of diabetes or hypertension were examined for indices of the
metabolic syndrome. None of the subjects was taking hormone therapy. The
thickness of abdominal subcutaneous and peritoneal fat layer was estimated by
U/S. Clinical parameters of obesity such as waist and hip circumference and BMI
were recorded and SHBG, insulin, glucose and lipid levels were measured.
SHBG levels were inversely correlated with peritoneal fat (PZ0.003) whereas
there was no significant association with subcutaneous fat. Lower SHBG levels
were associated with increased waist circumference, decreased hip circumference, increased BMI, higher HOMA - Insulin Resistance Index and insulin levels
(P!0.02). Step multivariate analysis showed that peritoneal fat, hip
circumference and insulin levels were independently associated with SHBG
levels. Significant associations were also found with age (PZ0.047).
Peritoneal but not subcutaneous adiposity, as assessed by U/S, is inversely
associated with SHBG levels. U/S seems to be a simple, low-cost method for the
assessment of central adiposity in apparently healthy individuals. SHBG levels,
which have been recognized as a risk factor for CVD, are highly correlated with
indices of either protective type (hip) or high-risk type (peritoneal and waist)
regional adiposity, indirectly supporting the importance of regional adiposity to
the risk for metabolic syndrome and cardiovascular disease.
Comparative analysis of adiponectin, leptin and C-peptide levels in
obese non-diabetic, type 1 diabetic and lean non-diabetic children
Olga Sysoyeva, Nataly Karlovich & Tatiana Mokhort
State Rehabilitation Centre, Department of Endocrinology, Minsk, Belarus.
A range of hormones which regulate energy metabolism are secreted by adipose
tissue, among which adiponectin and leptin are the main adipokines regulating
insulin sensitivity.
The aim of our study was to estimate and compare levels of adiponectin, leptin,
C-peptide and adiponectin-to-leptin ratio (A/L) in obese non-diabetic, Type 1
diabetic (T1D) children and lean non-diabetic controls.
BMI and SDS BMI were calculated in 88 children (46f, 42m, age 14.8G
3.6 yrs): 32 pts with obesity, 34 pts with T1D, 22 lean non-diabetic persons.
Serum levels of C-peptide, adiponectin and leptin were measured by ELISA.
Median adiponectin levels were higher in control group (22.1 mcg/ml;
PZ0.0001) and T1D pts (21.1 mcg/ml; PZ0.0002) as compared with obese
pts (12.6 mcg/ml). Leptin levels were higher in pts with obesity (41.2 ng/ml)
as compared with control (1.8 ng/ml; P!0.000001) and T1D pts (2.8 mcg/ml;
P!0.000001). Leptin levels in T1D pts were higher than in control group
(PZ0.027), while adiponectin levels were practically the same.
Highest A/L ratio was in lean controls (11.6), lowest – in obese nondiabetic children (0.5), whereas in T1D pts A/L ratio was 6.6. Differences
between groups were significant (P!0.05).
We did not find significant correlation of adiponectin and leptin levels,
adiponectin-to-leptin ratio with age at observation, BMI, C-peptide. At the
same time adiponectin level and adiponectin-to-leptin ratio negatively
correlate with BMI in T1D (rZK0.37, PZ0.032; rZK0.35, PZ0.049)
and obese non-diabetic children (rZK0.55, PZ0.001; rZ0.45, PZ0.011).
Endocrine Abstracts (2007) Vol 14
9th European Congress of Endocrinology, Budapest, Hungary, 2007
Surprisingly, in obese non-diabetic pts we find significant correlation of
adiponectin and age at observation (rZK0.59, PZ0.0004).
We concluded that the older obese pts are, the lower adiponectin level is.
Adiponectin-to-leptin ratio is a more useful marker of impaired adipokines
secretion than adiponectin or leptin levels alone, though further study is
necessary to prove reliability of this test for assessment of insulin
significant difference between Group A and B in BMI (34.85G1.12 vs.
34.65G0.87), age (36.00G4.64 vs. 37.07G1.81), basal glucose (4.91G0.26
vs. 4.73G0.09), basal insulin (14.73G1.82 vs. 17.43G1.67), adiponectin
(5.90G3.19 vs. 10.97G2.94), leptin (34.66G6.34 vs. 33.09G3.45), peak
glucose (8.96G1.10 vs. 7.85G0.36), insulin at peak glucose (80.54G20.78
vs. 105.97G16.46) neither in insulin sensitivity (5.51G0.87 vs. 4.81G0.64).
Our data demonstrate existence of two type of visfatin response during OGTT
in obese women. It is still not clear which influence determines different type
of visfatin response during OGTT and further studies are necessary to
elucidate these mechanisms.
Effects of pioglitazone and metformin on body weight and the insulin
resistance parameters in young patients with obesity
Olya OLeksyk, Alexander Serhiyenko & Victoria Serhiyenko
Medical University, Lviv, Ukraine.
Background and Aims
The aim of this study was to evaluate the effects of pioglitazone (PGZ) and
metformin (MET) plus Hypocaloric Diet (HD) in young patients with obesity and
impaired oral glucose-tolerance test (75 g glucose).
Materials and methods
49 patients (17.1G1.2 yrs) were allocated in groups: A (nZ14) received PGZ
30 mg tid plus HD, B (nZ12) - MET 1000 mg tid plus HD, C - PGZ 30 mg plus
MET 1000 mg plus HD (nZ11), D (nZ12) were only on HD. The duration of the
study was 3 months. We investigated Body Mass Index (BMI), triglyceridaemia
(TG), Systolic (SBP), Diastolic Blood Pressure (DBP), insulin resistance (IR)
parameters: Homeostasis Model Assesment (HOMA) - IR index; HOMA - b-cell
function (HOMA-b-CF). Statitics: ANOVA.
The increase of BMI, W/H, pre- and postprandial TG, HOMA-IR index (P!0.05),
SBP and DPB (P!0.05) parameters, the decrease of HOMA-b-CF (P!0.05) were
observed. PZG lead to the decrease of postprandial TG, HOMA-IR (P!0.05),
some increase of BMI, improvement of HOMA-bCF and did not significantly
influence SBP, DBP. MET was accompanied by the decrease of BMI (P!0.05),
postprandial TG (P!0.05), SDP, DBP (P!0.05), but in a smaller degree, than
PZG. The combined administration of PZG and MET lead to more expressed
positive dynamics of investigated parameters. In particular, BMI made 26.4G3.6
(P!0.05), HOMA IR index, HOMA-bCF 0.28G0.004 (P!0.01), postprandial
TG 1.77G0.03 (P!0.01), SBP (P!0.05), DBP 85.4G2.5 (P!0.05). The use of
HD only lead only to some decrease of BMI (P!0.05).
The administration of PZG and MET in young patients with obesity and impaired
OGTT is accompanied with more expressed positive dynamics of IR parameters,
that allows to recommend their use in such patients.
Plasma visfatin levels during oral glucose tolerance test in obese women
Dragan Micic1, Mirjana Sumarac-Dumanovic1, Aleksandra Kendereski1,
Goran Cvijovic1, Danica Stamenkovic-Pejkovic1, Maja Georgiev1,
Svetlana Zoric1, Jagoda Jorga1, Carlos Dieguez2 & Felipe Casanueva2
Institute of Endocrinology, Diabetes and Diseases of Metabolism, Clinical
Center of Serbia, Belgrade, Serbia; 2Department of Endocrinology,
University of Santiago De Compostela, Santiago de Compostela, Spain.
Visfatin is expressed in visceral adipose tissue and is up regulated in some
animal models of obesity. Insulin-mimetic actions of visfatin may be part of
the feedback regulation of glucose homeostasis, so plasma glucose or insulin
may have effect on visfatin levels in humans. The aim of study was to
investigate plasma glucose, insulin and visfatin during oral glucose tolerance
test (OGTT, 75 gr) in obese women. 22 obese women (age: 36.73G1.88 yrs;
BMI 34.72G0.67 kg/m2) were studied. Plasma visfatin (EIA Phoenix, ng/ml),
adiponectin and leptin (Linco RIA, ng/ml), insulin (RIA Inep, mU/l) and
glucose (mmol/l) were measured in basal state, while additional visfatin and
insulin were measured at the peak glucose during OGTT. Insulin sensitivity
(M index:mg/kgBW/min) was measured using euglycemic 2 hr clamp.
Basal glucose was 4.78G0.10 and peak glucose during OGTT 8.20G0.42
(P!0.005). There were no significant differences in visfatin between
basal sample and at the peak glucose levels (72.26G3.34 vs. 79.46G7.15,
PO0.05). Basal insulin was 16.57G1.28 and at the peak glucose 97.88G
13.01 (P!0.05). After analysis of the individual data we found that 7
obese women (Group A) had significant decrease (44.77G3.87 vs.36.19G
8.42, P!0.05) and 15 women (Group B) had significant increase in visfatin
during OGTT (69.85G4.49 vs. 99.66G2.59, P!0.05). There were no
Endocrine Abstracts (2007) Vol 14
The association of high sensitivity C-reactive protein levels with body
fat mass and body fat distribution
Deniz Gokalp1, Alpaslan Tuzcu1, Hatice Akay2, Senay Arikan1 &
Mithat Bahceci1
Dicle University School of Medicine Department of Endocrinology,
Diyarbakir, Turkey; 2Dicle University School of Medicine Department of
Radiology, Diyarbakir, Turkey.
Background and aim
C-reactive protein (CRP) is a sensitive marker for systemic inflammation. In this
study we aimed to investigate the relationship between high-sensitivity C-reactive
protein (hs-CRP) levels and BMI, body fat mass and fat distribution in healthy
Subjects and methods
A total 117 healthy subjects aged with 20–68 yr [normal weight (BMI
18.5–25.0 kg/m2, n:35), overweight (BMI: 25–30 kg/m2, n:27) and obese (BMI
R30.0, n: 55)] were included to the study. Body weigt, BMI, waist and hip
circumferences, skinfolds (biceps, triceps, suprailiac and subscapular region) with
skinfold caliper and ultrasonography and body fat mass with bioelectric
impedance of all subjects were measured. Hs-CRP concentrations were measured
with immunometric assay. Analysis of variance, post hoc Benferoni test and
Pearson correlation test were used for statistical analysis.
Mean serum hs-CRP levels of obese group determined with BMI were higher than
overweight and normal weight groups (7.3G5.46, 2.5G3.13, 0.66G1.1,
respectively, PZ0.0001). Mean serum hs-CRP levels of overweight group was
not different normal weight groups. In addition hs-CRP levels were positively
correlated with BMI, waist and hip circumferences, fat mass and skinfold
thickness of all 4 regions. Al data were shown in Table 1.
1-Hs-CRP level is high in obese patients and there was close relationship between
BMI and HS-CRP serum levels. 2-Both waist and hip circumference positively
correlated with hs-CRP level, these data suggest that not only android obesity but
also gineoid obesity increased hs-CRP levels. 3-Skinfold thicknesses were useful
methods in clinical practice and they were also positively correlated hs-CRP
BMI (kg/m2)
Waist crcum. Cm
Hip circum. (cm)
Thickness (cm)
Fatmass (kg)
Innervation of white and brown adipose tissue: dual viral transneuronal
tracing study
Ádám Dénes1, Miklós Darida1, Zsolt Boldogkoi2 & Krisztina Kovacs1
Institute of Experimental Medicine, Budapest, Hungary; 2Dept. Biology,
University of Szeged, Szeged, Hungary.
9th European Congress of Endocrinology, Budapest, Hungary, 2007
Central control of body weight involves coordinated regulation of food intake
and energy metabolism. White (WAT) and brown (BAT) adipose tissue
represent functionally distinct compartments of lipid storage and fuel
consumption, respectively. Both adipose tissues are innervated by the
sympathetic nervous system. Tyrosine hydroxylase positive fibers were found
in between fat cells. To determine the extent to which the control of different
fat compartments is provided by the same pre-autonomic neurons, the central
circuit innervating WAT and BAT was compared by dual viral transneuronal
tracing using isogenic recombinant strains of the pseudorabies virus. BDL,
expressing beta galactosidase was injected to the epididymal WAT and BDG,
expressing green fluorescent protein was inoculated into the intrascapular BAT
of male rats and virus reporter proteins were revealed by
immunocytochemistry. In the spinal cord, BDG infected neurons were found
in the intermediolateral and central autonomic nuclei of the upper thoracic
segments, while BDL infection appeared in the lower thoracic and lumbar
levels. Several brainstem pre-autonomic areas (C1, A5) and the gigantocellular
reticular nucleus contained BDG and BDL infected neurons, but relatively few
neurons were infected by both viruses. In the dorsal motor nucleus of the
vagus, the periaqueductal gray matter, as well as in the dorsomedial,
ventromedial, paraventricular hypothalamic nuclei and in the lateral hypothalamic area, anatomically distinct sub-regions were infected by the two
recombinant viruses. Following administration of the mixture of BDG and
BDL into the WAT, over 70% of the infected neurons contained both
recombinant viruses. Our data suggest that neurons involved in the regulation
of WAT and BAT coexist in all areas involved in the control of sympathetic
outflow, although the relative proportion of these neurons vary across the
regions. Double-labeled neurons may represent central command neurons that
direct coordinated responses of WAT and BAT to metabolic challenges.
Waist circumference and BMI as predictors of arterial hypertension in
childhood and adolescence in Latvia
Inese Madrevica, Juris Krikis & Renate Ligere
Latvian University, Riga, Latvia.
Child and adolescent adiposity is a problem of major concern not only for
Europe, but also for the world at large. Increase of waist circumference, BMI
and arterial blood pressure are metabolic syndrome risk factors which
contribute to the development of cardiovascular disease, hypertension and
diabetes mellitus.
To determine whether changes in arterial blood pressure are related to the
increase of waist circumference and BMI in childhood and adolescence.
We examined 1049 schoolchildren (aged 7–18), 535 of whom were
included in the study. In the risk group 41 schoolchildren were observed. For
the study special questionnaires including 25–28 metabolism parameters were
used. The obtained data were processed with the SPSS software packages
(BMDP and Systat 9) adapted for biological and medical studies. We also
determined the insulin resistance (Caro et al., 1991) and the insulin resistance
index (Dunkan et al., 1995).
In our study elevated arterial blood pressure for boys and girls rather correlated
with BMI (nZ532; rZ0.449; PZ0.000) than with the increase of waist
circumference (nZ532; rZ0.427; PZ0.000), whereas in the risk group arterial
blood pressure for both boys and girls more closely correlated with waist
circumference (nZ39; rZ0.403; P!0.05). In the child and adolescent risk group
both waist circumference and BMI have a negative correlation with the blood
glucose level (nZ39; rZK0.432; PZ0.000). BMI also negatively correlates with
insulin resistance in the risk group (nZ39; rZK0.339; P!0.05).
Elevation of arterial blood pressure in children and adolescents strongly
correlates with increase of both waist circumference and BMI. In assessing the
metabolic syndrome risk factors for children and adolescents both waist
circumference and BMI should be taken into account when working out early
metabolic syndrome criteria for children and adolescents.
Identification of orexin receptors in brown adipocytes: functional effects
of orexin-B
Janet Digby1, Jing Chen1, Danijela Markovic1, Say Viengchareun2,
Marc Lombes2, Hendrik Lehnert1 & Harpal Randeva1
University of Warwick, Medical School, Coventry, United Kingdom;
INSERM, Paris, France.
Orexin-A and orexin-B and their G-protein coupled receptors (orexin receptor-1 &
-2: OX1R, OX2R) have divergent effects on physiological behaviour,
cardiovascular regulation, glucocorticoid and insulin release. Furthermore, orexins
have been shown to affect both brown adipose tissue energy expenditure and
thermogenesis through stimulation of sympathetic nerve activity. Despite in vivo
studies demonstrating a role for orexins acting centrally on adipose tissue, there are
no data on the expression of orexin receptors in brown adipose tissue. We therefore
analyzed the expression and localization of OX1R and OX2R in mouse brown
adipocytes and in the T37i brown adipocyte cell line. Furthermore, the effects of
exposure to orexin-A and orexin-B were measured on the expression of key
genes involved in thermoregulation and insulin sensitivity; leptin, uncoupling
protein-1 (UCP-1), adipocyte-specific fatty acid binding protein-2 (AP2) and
Quantitative real time RT-PCR was performed using a Roche Light Cyclere
system, and genes of interest were standardised against the housekeeping gene
b-actin. OX1R and OX2R were detected in differentiated T37i brown
adipocytes using immunocytochemistry and confocal microscopy.
mRNA expression was detected for OX1R and OX2R in mouse mature
interscapular brown adipocytes, as well as in differentiated T37i brown
adipocytes in vitro. Furthermore, mRNA expression of both receptors increased
as a function of the degree of differentiation. Confocal analysis revealed intense
localised staining for OX1R around intracellular lipid droplets, whereas more
membrane-localised staining was observed for OX2R. T37i brown adipocytes
treated with orexin-B (100 nM, 4 h), resulted in significant increases in leptin,
UCP-1, AP2 and PPARg mRNA (P!0.05).
These novel findings indicate a direct role for orexin-B in brown adipocyte
tissue metabolism and thermogenesis and the potential to affect insulinsensitivity. Furthermore, the differing cellular receptor localisation suggests
divergent roles for orexins in brown adipocytes.
Uric acid is an important predictor of metabolic disturbances in obese
Ayse Sertkaya Cikim, Taner Bayraktaroglu, Adil Dogan Azezli &
Yusuf Orhan
Istanbul University, Istanbul Faculty of Medicine, Endocrinology and
Metabolism, Capa, Fatih/Istanbul, Turkey.
It was shown that a relationship between uric acid and cardiovascular diseases,
and hyperuricemia is associated with systemic inflammation. But, determination
of uric acid is widely available and inexpensive, it has been overlooked as a
marker of systemic inflammation and metabolic disturbances. In this study, we
aimed to evaluate uric acid value and its association with inflammation and
metabolic disturbances in overweight and obese Turkish women.
Material and methods
The study population consisted of 3975 women with BMI of 25 kg/m2 or greater,
classified as overweight (BMIOZ25 kg/m2, nZ771) or obese (BMIOZ
30 kg/m2, nZ3204) by National Institutes of Health and WHO criteria. They
divided two groups according to median uric acid levels. Demographic and
anthropometric characteristics, blood glucose, insulin and lipid concentrations,
and the indices of insulin resistance and inflammation were determined and
compared between groups.
Median uric acid level was 4.40 mg/dl. Therefore, our patients were divided two
groups according to median uric acid levels; i.e. 4.40 mg/dl, group 1(women with
low uric acid levels; ‹ 4.40 mg/dl) and group 2 (women with high uric acid levels;
› 4.40 mg/dl). And metabolic parameters in group 2 having higher uric acid levels
were significantly different and disturbed than group 1 with lower uric acid levels.
In this study, we found a significant difference in various metabolic and
inflammatory parameters among different uric acid levels groups. The women
with high uric acid groups have had high metabolic and inflammatory markers.
These findings suggest that the relationship between uric acid and inflammatory
markers. However. The nature of such a relationship remains unknown. These
findings support the hypothesis that uric acid may negatively impact on metabolic
Endocrine Abstracts (2007) Vol 14
9th European Congress of Endocrinology, Budapest, Hungary, 2007
Fasting and postprandial plasma obestatin levels are reduced in obesity
Christina Maier1, Dominik Haider2, Greisa Vila1, Michaela Riedl1,
Anton Luger1 & Michael Wolzt2
Department of Internal Medicine III, Division of Endocrinology and
Metabolism, Medical University of Vienna, Vienna, Austria; 2Department
of Clinical Pharmacology, Medical University of Vienna, Vienna, Austria.
Growth hormone Reduces Inflammation in Postmenopausal Women
with Abdominal Obesity: a 12-month randomized placebo-controlled
Celina Franco1, Björn Andersson2, Lars Lönn3, Bengt-Åke Bengtsson1,
Johan Svensson1 & Gudmundur Johannsson1
Research Center for Endocrinology and Metabolism, Sahlgrenska
University Hospital, SE-413 45, Göteborg, Sweden; 2Department of
Medicine, Sahlgrenska University Hospital, SE-413 45, Göteborg, Sweden;
Department of Diagnostic Radiology, Sahlgrenska University Hospital,
SE-413 45, Göteborg, Sweden.
Obestatin has recently been identified as a peptide derived from pre-proghrelin
that opposes ghrelin effects on appetite and body weight in rodents. We studied
the effect of food intake on both these hormones in obese and lean subjects and
recorded in parallel the subjective sensations of satiety and hunger. Eight obese
(two males and six females, BMIZ31–52 kg/m2) and eight age- and sex-matched
lean subjects (BMIZ19–23 kg/m2) were randomized to 1) take a standard
breakfast and 2) time control studies after an overnight fast in a prospective crossover study design. Obestatin and ghrelin plasma concentrations were quantified
by radioimmunoassays, satiety and hunger by visual analogue scales.
Basal circulating obestatin was significantly decreased in obese as compared to
lean humans and stable in both study groups during an observation period of
90 minutes. Thirty minutes after food intake, obestatin levels were markly
reduced in obese subjects, but increased in lean controls. There was no correlation
between ghrelin and obestatin postprandial plasma concentrations. Subjective
ratings of satiety and hunger were significantly related to obestatin plasma
concentrations only in lean subjects.
We conclude that obestatin concentrations are much lower in obese subjects
and inversely regulated by food intake, as compared to lean subjects. Both fasting
and postprandial suppression of the anorexigenic obestatin might be of relevance
in the pathophysiology of the positive energy balance associated with obesity.
Insulin resistance and insulin secretion in morbidly obese patients
before and six months after bariatric surgery
Miriam Promintzer1, Gerhard Prager2, Marietta Stadler3,
Christian Anderwald1, Martina Mandl1, Soheila Shakeri Manesch2,
Peter Nowotny1, Martin Georg Bischof1, Bernhard Ludvik1, Anton Luger1
& Michael Krebs1
Division of Endocrinology and Metabolism, Department of Internal
Medicine III, Medical University of Vienna, Vienna, Austria; 2Department
of Surgery, Medical University of Vienna, Vienna, Austria; 3Thrid Medical
Department of Metabolic Diseases and Nephrology, Lainz Hospital, Ludwig
Boltzmann Institute of Metabolic Diseases and Nutrition, Vienna, Vienna,
Recent case reports describe hyperinsulinemic hypoglycemia after gastric bypass.
The aim of this study was the assessment of insulin resistance and insulin
secretion in non-diabetic morbidly obese patients before and six months after
bariatric surgery.
In 8 non-diabetic morbidly obese patients (OB:6f/2 m, age:42G3a,
BMI:47.29G2.2 kg/m2) and 6 controls (CON:4f/2 m, age:43G0a, BMI:23.8G
0.5 kg/m2) we performed a frequently sampled oral glucose tolerance test (75 g,
3-hOGTT). The OGTT was repeated in 4 patients (3 Roux-en-Y gastric bypass, 1
gastric band) 6 months after surgery. Before bariatric surgery fasting plasma
levels of glucose were comparable between OB and CON while fasting insulin
and c-peptide were higher in OB (insulin:OB:27.0G5.6/CON:7.0G0.6 mU/ml,
PZ0.01; c-peptide:OB:4.3G0.7/ CON:1.3G0.1 ng/ml, PZ0.003). During the
OGTT peak plasma glucose and insulin concentrations were significantly higher
in OB (glucose: OB:196.1G15.6/CON:130.5G9.6 mg/dl, PZ0,006; insulin:OB:119.7G21.6/CON:58.6G9 mU/ml, PZ0.039). 6 months after bariatric
surgery fasting and early postprandial glucose concentrations were unchanged,
while insulin and c-peptide were lower at fasting and higher after glucose load.
Insulin resistance, assessed by HOMA-IR and OGIS, improved after bariatric
surgery. After glucose load insulin and c-peptide secretion was adapted to insulin
resistance prior surgery but was excessively elevated after bariatric surgery
(adaptation index: before:119G16/after surgery:228G53, P!0.05,
CON:114.5G19.6 total-nmol*m-2, PZ0.8, for before surgery vs. CON).
Conclusion: Non-diabetic morbidly obese patients exhibit preserved adaptation
of insulin secretion to severe insulin resistance. Six months after bariatric surgery
elevated fasting insulin and c-peptide were normalized. In the early postprandial
state, however, hyperglycemia remained unchanged, while secretion of insulin
and c-peptide was excessive and not adapted to improved insulin resistance. Thus,
this dissociation between increase of insulin secretion on the one hand and
amelioration of insulin resistance on the other hand might put patients at risk for
late postprandial hypoglycemia.
Endocrine Abstracts (2007) Vol 14
Abdominally obese individuals have relative hyposomatotropism, elevated serum
markers of inflammation, and increased risk of cardiovascular disease (CVD).
The aim was to study the effect of GH treatment on serum levels of inflammatory
markers and vascular adhesion molecules in postmenopausal women with
abdominal obesity.
Forty postmenopausal women aged 51–63 yrs with abdominal obesity received
GH (0.67 mg/d) in a randomized, double blind, placebo controlled 12-month trial.
Measurements of inflammatory markers in serum: interleukin-6 (IL-6), highly
sensitive C-reactive protein (CRP), and amyloid polypeptide A (SAA), and
markers of endothelial function: selectin, vascular adhesion molecule-1
(VCAM-1), intercellular molecule-1 (ICAM-1) were performed at baseline and
after 6 and 12 months of treatment.
The GH and placebo group were comparable at baseline in terms of age, BMI,
waist circumference, IGF-1, smoking habits and antihypertensive treatment. After
12 months, mean IGF-I SD score was 0.9G1.5 and – 0.8G0.6 in the GH and
placebo groups, respectively. The 12-month GH treatment reduced serum levels
of CRP and IL-6 as compared with placebo (PZ0.03 and PZ0.05, respectively),
whereas the markers of endothelial function were unaffected. Within the GH
treated group, serum CRP level showed a reduction from 4.3G4 at baseline to
3.0G3 mg/L after 12 months (PZ0.05) and serum IL-6 level was reduced from
4.4G2 to 3.3G2 ng/L (P!0.01).
GH treatment in postmenopausal women with abdominal obesity reduced serum
levels of inflammatory markers, suggesting that the risk of CVD was reduced.
There was no detectable effect of the GH treatment on endothelial function
evaluated using measures of vascular adhesion molecule levels in serum.
Hyperactivity of the hypothalamic-pituitary-axis and adrenal hyperandrogenism in polycystic ovary syndrome: a consequence of 5
b-reductase hyperfunction
Alessandra Gambineri, Laura Patton, Giulia Forlani, Alessandra Munarini,
Federica Tomassoni, Uberto Pagotto & Renato Pasquali
Endocrinology Unit, Department of Internal Medicine, S. Orsola-Malpighi
Hospital, University of Bologna, Bologna, Italy.
Among the uncertainties surrounding the etiology of polycystic ovary syndrome
(PCOS) the role of increased peripheral cortisol metabolism has become
interesting, particularly in relationship to the pathogenesis of adrenal
hyperandrogenism. The patways of cortisol metabolism include irreversible
inactivation of cortisol by 5a- and 5b-reductase. To evaluate the association of
5a- and 5b-reductase activity with adrenal hyperandrogenism in PCOS, we
recruited 90 PCOS women (age range: 18–45 years) classified into three groups
accordingly to the responsiveness of androstenedione (A) and DHEA to
1–24ACTH: group of low responders (LR) (nZ27), defined by A and DHEA
responsiveness to 1–24ACTH within 2 SD of mean of a group of controls; group of
medium responders (MR) (nZ43), defined by A or DHEA responsiveness to
1–24ACTH over 2 SD; group of high responders (HR) (nZ20), defined by A and
DHEA responsiveness to 1–24ACTH over 2 SD. Excretion of cortisol and its
metabolites was measured by electron impact gas chromatography-mass
spectrometry in a 24-h urine collection. Relative 5a- and 5b-reduction of cortisol
was assessed by 5a-tetrahydrocortisol (5a-THF)/cortisol, and 5b-THF/cortisol
and 5b-tetrahydrocortisone (THE)/cortisone, respectively. The three groups were
similar for age, body weight and body fat distribution. Testosterone, A and 17OHprogesterone basal levels were also similar among the three groups, whereas
DHEA-S was significantly higher in MR (P!0.05) and more in HR (P!0.01)
respect to NR. HR presented also basal cortisol levels significantly lower and
cortisol responsiveness to 1–24ACTH significantly higher than MR (P!0.01) and
9th European Congress of Endocrinology, Budapest, Hungary, 2007
NR (P!0.001, P!0.05). 5b-THF/cortisol and 5b-THE/cortisone were significantly higher in HR respect to MR and NR (P!0.05). No differences in
5a-THF/cortisol were observed among the three groups. These data open up the
intriguing possibility of 5 b-reductase hyperfunction as a new pathogenetic
mechanism of adrenal hyperandrogenism in a subgroup of PCOS women.
An examination of the prevalence of IDF and ATPIII defined metabolic
syndrome: towards population based screening
Deirdre Waterhouse, Jayant Sharma, Frances Sheehan & Donal O’Shea
St Vincent’s University Hospital, Dublin, Ireland.
Despite the significant associated cardiovascular morbidity, as well as the
significant economic implications, little consideration has been given towards
population screening for the Metabolic Syndrome (MetS). Therefore, we wished
to estimate the prevalence of MetS, using both the recently published IDF, as well
as the previously defined Cholesterol Education Program Adult Treatment Panel
III (ATPIII), criteria. Additionally, we hypothesised that simple, inexpensive
anthropometric measurements offer an effective means of population based
assessment for MetS.
1716 participants (1026 males, 690 females) underwent full cardiovascular
assessment over a twelve month period, including detailed questionnaire,
measurement of waist circumference, BMI calculation, sphygomanometry and
fasting glucose and lipid profiling. Subsequently, the prevalence of the MetS was
defined in accordance with both the IDF and ATPIII definitions.
The prevalence of the MetS was 21.4% (nZ368) and 13.2% (nZ227) in
accordance with IDF and ATPIII criteria respectively. Subjects identified using
IDF criteria had significantly lower waist circumference (PZ0.006) as well as
significantly increased HDL cholesterol (PZ0.008) when compared to the
ATPIII cohort.The prevalence of IDF defined central obesity in our cohort was
56.8% (nZ975); of these 37.5% (nZ368) had MetS. The prevalence of MetS
within this obese hypertensive cohort was 57.3% (nZ328). Thus, concurrent
central obesity and hypertension would identify 89.1% of the total IDF defined
MetS in the population.
When compared to the previous ATPIII criteria, the IDF definition identifies an
additional cohort of individuals with metabolic risk factor clustering despite a
significantly leaner waist circumference. This leads to a higher prevalence of IDFdefined MetS. Finally, the coexistence of central adiposity and hypertension was
noted in the majority of patients with MetS. This simple dysanthropometric
phenomenon may potentially be used as an inexpensive means of population
assessment for MetS.
Neuroendocrine and genetic aspects of metabolic disturbances in
women with simple obesity, polycystic ovary syndrome (PCOS) and
eating disorders
Agnieszka Baranowska-Bik1, Wojciech Bik1, Ewa Wolinska-Witort1,
Pawel Gaj2, Michal Mikula2, Piotr Bragoszewski2, Jerzy Ostrowski2 &
Boguslawa Baranowska1
Medical Centre of Postgraduate Education, Neuroendocrinology Department, Warsaw, Poland; 2Medical Centre of Postgraduate Education,
Department of Gastroenterology, Warsaw, Poland.
Neuropeptides and adipocytokines influence metabolic homeostasis and food
intake. Deregulation in their secretion leads to insulin resistance or metabolic
syndrome. Adiponectin possesses anti-diabetic and insulin sensitizing properties.
Expression of this gene remains under control of nuclear peroxisome proliferatoractivated receptor (PPAR)-gamma. Ghrelin, an endogenous ligand for GH
secratagogue receptor (GHSR), modulates metabolic homeostasis. A high aminoacid homology and transmembrane localization of G-protein coupled receptor 39
(GPR39) and GHSR suggest that ghrelin secretion can be modified by GPR39.
Genetic variation found in genomic DNA sequences is a potentially important
factor regulating expression level of mentioned genes. We evaluated the role of
genetic factors and relationship between metabolic alterations and plasma
adiponectin, ghrelin and leptin levels in women with simple obesity, PCOS (nonobese) and anorexia nervosa (AN).
The study consisted of 142 women (109 patients and 33 healthy lean controls)
in similar age and was approved by the Local Ethics Committee. For SNP (single
nucleotide polymorphism) analyses we genotyped all women for: (PPAR)gamma, TNF-alpha, GPR39, GHSR, and ADIPOQ. We compared the distribution
of alleles according to different clinical course vs. healthy controls. Our main
findings are that in lean PCOS women insulin and HOMA-IR were higher
comparing to controls but adiponectin and ghrelin did not differ significantly.
Furthermore, in AN adiponectin and ghrelin were higher and leptin was lower
compared with controls. The correlations between adiponectin, leptin and
metabolic parameters were found. Genetic variant correlation was shown only for
(PPAR)-gamma (Pro12Ala-rs1801282) locus comparing AN to healthy controls
with a preference of higher level of heterozygosity among these patients.
Decreased adiponectin and ghrelin levels in obesity cannot be explained by
variations loci we examined. We conclude that lean PCOS women show
increased insulin resistance. An evidence of genetic correlation of (PPAR)gamma (Pro12Ala-rs1801282) locus in the group of AN patients was found.
The effect of body composition and iron status on insulin resistance in
hemodialysis patients
Zorica Rasic, Gordana Perunicic, Jelena Tica, Vesna Popovic,
Marina Vujovic & Zoran Gluvic
University hospital Zemun, Belgrade, Serbia.
High level of inflammatory cytokines was present within malnourished and
chronic renal failure maintenance hemodialysis (MHD) patients, but there were
conflicting data about the role of inflammation on development of insulin
resistance (IR) in non-obese and overweight MHD patients.
We selected 23 well-nourished and 20 middle- to moderate-malnourished, sex
and age-matched, stable MHD patients, 23 male and 20 female, with median
dialysis duration of 48 months (IQR 24.5–82.0). All patients were treated at the
Hemodialysis Unit. To determine the nutritional status, body composition and the
presence of inflammation of MHD patients we used: subjective global assessment
(SGA), anthropometrics measurements (BMI and waist circumference),
bioelectrical impedance analysis (BIA) which was performed to quantify body
fat and lean body mass, and biochemical parameters measurements [with serum
iron, ferritin, intact parathormone (i-PTH), TNF-alpha, IL-6 and high sensitivity
C-reactive protein (hs-CRP)]. All parameters were evaluated by comparisons
between HOMA-IR tertiles. By backward multivariate regression analysis we
identified independent variables for IR.
As the tetiles of HOMA-IR increased, dialysis duration, systolic blood pressure,
serum levels of glucose, insulin, and waist circumference increased, whereas
HDL-cholesterol level decreased. Serum iron value was increased also. As we
expected, the prevalence of the metabolic syndrome were increased significantly
across the tertiles of HOMA-IR. HOMA-IR correlated with the levels of iron,
ferritin, adipokine TNF-alpha, waist circumference, and total fat percentages.
After adjustment for gender, age, hemodialysis duration, ferritin, BMI and total
fat percentages, multivariate regression analysis was performed and the
association with HOMA-IR was still strong only for serum levels of iron, TNFalpha and waist circumference. That explains 17% of the total variation in
HOMA-IR (Adjusted R2Z0.166, PZ0.04).
Our study demonstrated that 1) serum iron had participated as independent
predictor in the pathogenesis of IR on long-term MHD patients, together with 2)
adipokine TNF-alpha and 3) visceral adiposity.
Relationship between obesity, insulin resistance and adipokines in
morbidly obese women
Rana Madani1, Nazar Miheisi2, Majid Hashemi1 & Vidya Mohamed-Ali2
University College London, Department of Surgery, London, United
Kingdom; 2University College London, Department of Medicine, London,
United Kingdom.
Several cytokines and chemokines are released by adipose tissue and
associated with insulin resistance. We investigated the systemic and in vitro
Endocrine Abstracts (2007) Vol 14
9th European Congress of Endocrinology, Budapest, Hungary, 2007
release of RANTES(Regulated upon Activation Normal T-cell Expressed
and Secreted), MCP-1(Monocyte Chemo-attractant Protein-1), adiponectin,
leptin and IL-6 from three human adipose tissue depots and their
relationship to insulin sensitivity.
Fasting blood samples were taken from obese female patients undergoing
surgery(nZ7, mean age 39 years, mean BMI 46 kg. m2). Glucose, insulin
and lipid profiles and circulating adipokines named above were measured.
Subcutaneous(Sc), omental(Om) and Gastric Fat Pad(GFP) adipose tissue
organ culture were set up for determining in vitro adipokine release.
Haemostasis Model Assessment for Resistance(HOMA-R) was calculated.
Body fat content was measured using bioelectrical impedance. The study
was approved by the hospital ethical committee.
Unlike for leptin no significant correlation was observed between % body
fat and other adipokines. Production rates of adipokines in vitro per gram
adipose tissue per hr were: RANTES(Sc medianZ67, OmZ29, GFPZ
62 pg/ml), MCP-1(Sc medianZ5, OmZ6, GFPZ4 ng/ml), leptin (Sc
medianZ971, OmZ212, GFPZ447 pg/ml), adiponectin(Sc medianZ23,
OmZ25 ng/ml) and Il-6(Sc medianZ9, OmZ12, GFPZ10 ng/ml). Depot
specific differences in adipokine release were not apparent except in leptin
which was mainly subcutaneous. There was a direct significant correlation
between % body fat and Sc leptin production and an inverse relationship
with Om adiponectin. GFP release of RANTES had a negative and MCP-1 a
positive relationship with % body fat. Obese subjects were significantly
more insulin resistant. Serum MCP-1 was elevated in patients with
worsening insulin resistance. There was a negative correlation between
HOMA-R and serum adiponectin and HDL.
RANTES, MCP-1 and adiponectin were released in vivo from adipose tissue.
Local production of adipokines varies between depots. Insulin sensitivity and %
body fat can alter local production of the adipokines.
Somatostatin receptor subtype 2 inhibits glucagon secretion and
regulates glucose homeostasis
Mathias Strowski, Vandana Singh, Carsten Grötzinger, Sylvia Zacharias,
Bertram Wiedenmann & Ursula Plöckinger
Hepatology & Gastroenterology, Berlin, Germany.
Somatostatin (SST) inhibits glucagon and insulin secretion. Five receptor
subtypes for SST are known (SSTR1-SSTR5), all of which are expressed in the
endocrine pancreas. SSTR2 inhibits glucagon secretion in vitro, however its role
in vivo is not well understood. Here, we characterize the role of SSTR2 in
regulating glucose homeostasis in mice with diet-induced obesity.
SSTR2-deficient (SSTR2K/K) and control mice (SSTR2C/C) were fed high-fat
diet (HFD) for 14 weeks and the parameters of endocrine pancreas function were
determined. Hepatic glycogen and lipid content was evaluated enzymatically and
by histomorphology. Expression of enzymes regulating glycogen synthesis and
breakdown were measured by a real-time PCR and Western blot. Insulin,
somatostatin and glucose tolerance tests were performed. Glucagon secretion
from isolated islets was measured by RIA, and glycogenolysis in isolated
Postprandial glucagon and glucose concentrations were increased in SSTR2deficient mice. Glucose disappearance rate following administration of glucose,
insulin or SST was delayed in SSTR2K/K mice. SSTR2-deficient mice had
decreased hepatic glycogen content and decreased glucokinase mRNA. Glycogen
synthase of SSTR2K/K mice was decreased while glycogen synthase kinase-3
was increased. Glycogen phosphorylase, phosphorylase-kinase, and CREB were
increased. The hepatic lipid content of SSTR2-deficient mice was decreased.
Glucose was unable to suppressglucagon secretion from pancreatic islets isolated
from SSTR2-deficient mice. Hepatic glycogenolysis was inhibited by an SSTR2selective agonist.
We demonstrate here that SSTR2 inhibits glucagon secretion in mice with dietinduced obesity. Deletion of SSTR2 accounts for the postprandial hyperglucagonemia. Increased glucose concentration may be due to decreased hepatic
glucose utilization, lipid accumulation, and increased glycogen breakdown.
SSTR2 may provide a valuable therapeutic target at improving hyperglycemia in
patients with peripheral insulin resistance and obesity.
Obesity in pre-school children –new epidemic problem?
Ewa Barg, Chmielarska Joanna, Adamska Barbara, Begar Inna,
Konieczna Agnieszka & Skarzynska Malgorzata
Wroclaw medical University, Wroclaw, Poland.
In the opinion of the World Health Organization the obesity will become one of
four major epidemics of the 21st century. The most important factor for its
occurrence is the lifestyle.
The aim of the research was to analyse the body mass index (BMI) of preschool children and their parents and the components of their lifestyle, such as
diet, sports and free time activities.
Material and Methods
The two-stage study included 537 children (265 boys and 272 girls) aged 3 and 6
(5.63G1.1). The anthropometric measurements of the children were made and the
BMI was counted and referred to the percentiles. The parents were questioned
about their height and weight and life style.
82 (15%) children fulfilled the criteria of obesity. The fathers’ overweight was
stated in 54.6%, whereas obesity in 10.7%; mothers’ overweight in 14.4%,
obesity in 1.34%.
Children eat their first meal around 8.00 a.m., the last at 7.00 p.m.
The average number of main meals is 3.9G0.9. Up to 87% of parents state
that their child eats extra food (fruit, yoghurts, sandwiches) between the
main meals. A major part in the diet plays the sweets. Up to 48% of
children consume sweets everyday, 8.2% of them a few times daily and
only 1% once a week.
Only 33% of children regularly do sports. A child spends up to a
100 minutes daily in front of a TV or a computer.
1. The occurrence of obesity in over 15% of pre-school children should keep
parents and pediatrists alert because of the possible health consequences.
2. The incorrect nourishment and improper lifestyle may result in obesity
becoming an epidemic.
3. It is vital to popularize a healthy lifestyle not only among children but also
their parents.
Endocrine Abstracts (2007) Vol 14
The role of combined treatment of arterial hypertension in patients with
Doliashvili Tamar, Giorgadze Ellen, Asatiani Ketevan & Surmava Arkadi
N4 clinical hospital, Tbilisi, Georgia.
The aim of our study was to assess the advantage of combinative therapy with
lisinopril and moxonidin for the treatment of arterial hypertension in group of
obese patients in comparison to the single-drug therapy with lisinopril.
26 obese patients were divided in 2 groups. They underwent a 24-hour monitoring
of the arterial pressure and were diagnosed as arterial hypertension II degree
(ESH-ESC). In the I group for the purpose of stabilization of arterial hypertension
lisinopril was given in the daily dose of 10 mg for 2 times, in the II group we gave
a combination of lisinopril in the same dose as in the I group plus moxonidinin the
daily dose of 0.4 mg for 1 times. The evaluation of state of health and the
ambulatory registration of the arterial pressure data were carried out every week.
After 3 weeks from the beginning of the treatment repeatedly the monitoring was
done and the data were compared in both of the groups.
At the beginning of the treatment the mean daily indices of the arterial pressure in
the groups were 165/100 mmHg and 166/98 mmHg. After 2 weeks from the
treatment in both groups the data of the pressure stabilized, however in the group
of combinative therapy the decrease of the daily dose of lisinopril was required on
5 mg because of more expressed lowering of the arterial pressure data, and after 3
weeks of the treatment according to repeated monitoring the mean daily indices
were 142/87 mmHg and 136/85 mmHg. The state of the health was improved
markedly in both of the groups.
Adding the agonist of imidazoline receptor in the standard antihypertension
therapy significantly improves the state of the health and tolerance of the therapy,
as well as enables the lowering of the other antihypertensive medications.
9th European Congress of Endocrinology, Budapest, Hungary, 2007
A registry of GDM in portugal
Luı́sa Ruas, Tiago Rocha, Jorge Dores & Manuela Carvalheiro
Pregnancy Study Group of the Portuguese Diabetes Society, Coimbra,
A retrospective study of the year 2003, of 1314 women with GDM, was
Patients and methods
Two groups according to pre-pregnancy BMI: Go - BMIS30 Kg/m2; Gno BMI!
30 Kg/m2. Mean age 32.9G5 years, A1c!6% in both groups. Influence of BMI
in different variables was analysed: family history of DM, weight gain during
pregnancy; blood pressure, need of insulin, gestation age at the beginning of
insulin, time and type of delivery, new-born weight and re-evaluation postpartum.
Mean BMI was 26.7G5.1, 76.3%ZBMI!30 and 23.8%ZBMIS30. Family
history of DM - BMI 26.93 Kg/m2, without family history K26.19 Kg/m2;
PZ0.01. Weight gain was adequate in 41.4%, reduced in 29.9% and excessive in
28.7%. Normal arterial blood pressure K86.5%, hypertension worsened by
pregnancy K6.9% and pregnancy induced hypertension K6.6%, BMI in these
three groups 26.1, 30.51 and 29.33, respectively (P!0.05). There was statistical
significant difference (P!0.05) between the two groups in these parameters:
Insulin therapy 75.2% in Go vs 52.5% in Gno and its need earlier in Go
K28.83 wks vs Gno K30.97 wks; time of delivery 38.1 wks in Go vs 38.4Kwks
in Gno; caesarean section 49.8% in Go vs 35% in Gno; new- born weight 3324.8 g
in Go vs 3167.9 g in Gno; macrosomic babies 8.3% in Go vs 4.4% in Gno. In the
re-evaluation post-partum higher BMI was related with severe degrees of
carbohydrate intolerance (P!0.05). We didn’t find any difference in the
re-evaluation between the women with adequate and excessive weight gain.
Obesity in GDM is a risk factor for maternal and fetal outcomes, with the risk of
early development in the mother of glucose intolerance.
The effects of glucocorticoids on the expression of gluconeogenic and
lipogenic enzymes in a rodent model of Cushing’s syndrome
Francesca Lolli1, Mirjam Christ-Crain1, Blerina Kola1, Csaba Fekete2,
Gábor Wittman2, Ashley B Grossman1 & Márta Korbonits1
Department of Endocrinology, William Harvey Research Institute, Barts
and the London, Queen Mary School of Medicine, London, United
Kingdom; 2Department of Endocrine Neurobiology, Institute of Experimental Medicine, Hungarian Academy of Sciences, Budapest, Hungary.
Cushing’s syndrome results from chronic exposure to excessive levels of
glucocorticoids (GC). The clinical manifestations associated with hypercortisolaemia are variable and differ widely in severity, including hypertension, apparent
obesity and metabolic aberrations such as diabetes, dyslipidaemia, ultimately
leading to changes similar to the metabolic syndrome. We hypothesised that GC
might influence the expression of the genes involved in lipogenesis and
gluconeogenesis in adipose tissue and liver.
Rats were implanted with corticosterone-containing pellets, and consumed chow
and 30% sucrose for two weeks according to a well-established model of
glucocorticoid excess. Animals implanted with cholesterol (placebo) pellets
consuming sucrose or saline only served as controls. RNA was extracted from
mesenteric and subcutaneous adipose tissue and liver. Gene expression was
analyzed by reverse transcription followed by real time quantitative PCR with
primers specific for phosphoenolpyruvate carboxykinase (PECPK), sterol
regulatory element-binding protein (SREBP1c and SREBP2), fatty acid synthase
(FAS), glucose-6-phospatase (G6P) and b-actin as housekeeping gene.
In the mesenteric adipose tissue GC significantly increased PEPCK mRNA
expression (PZ0.01), SREBP1c and FAS mRNA expression (PZ0.02 and
PZ0.035, respectively). No significant changes were observed in subcutaneous
fat tissue. In the liver GC significantly increased FAS mRNA expression
(P!0.0001) and decreased PEPCK mRNA (PZ0.027), without changes in the
expression of G6P or SREBP1c.
GC increase the expression of lipogenic and glyceroneogenic genes in visceral
adipose tissue and this could explain the increased fat storage observed in the
visceral fat of Cushing’s syndrome. The changes in the liver would lead to
increased fat deposition with less gluconeogenesis, and this was reflected in the
massive fatty liver observed experimentally. We suggest that there may be a
common factor leading to these changes secondary to the excess of
HRT in treatment of dislipidemia in women with hypogonadotropic
Vita Zektser, Irena Ilovayskaya, Aleksandr Iliyn, Nikolay Goncharov &
Galina Melnichenko
Research Centre for Endocrinology, Moscow, Russia.
Hypoestrogenemia is associated with dislipidemia and is an independent risk
factor for cardiovascular diseases in postmenopausal women. However, there is a
cohort of young women with gonadal steroid deficit caused by the disorders of
central regulation. Twenty women with hypogonadotropic hypogonadism (HH)
were included in group 1. (median age - 29 years and 3 months, median duration
of amenorhea - 5 years 3 months, mean BMI - 24.6G6.05 kg/cm2. Women were
examined before and after the 12 months treatment with 2 mg of 17-b-estradiol
and 10 mg of dydrogesteron in sequenced manner. Twenty three healthy women
were included in the group 2 (control), median age 27 years, Mean BMI - 24.0G
4.37 kg/cm2.
Dislipidemia was found in all patients with HH before the treatment. The levels
of total cholesterol was 5.65G1.26 mmol/l and tryglycerides 1.63G1.0* mmol/l;
HDL 1.34G1.0 mmol/l and LDL 3.9G1.1* mmol/l. In the control group total
cholesterol was 4.85G0.36 mmol/l, tryglycerides 0.78G0.07 mmol/l, HDL
1.77G0.33 mmol/l and LDL 1.8G0.7 mmol/l (*P!0,05). All of the parameters
were higher in group 1, but the significant difference was in LDH and tryglyceride
After 12 months treatment BMI didn’t change in all of the patientes with HH,
there was small but not significant reducing of cholesterol 5.2G1.23 mmol/ l and
tryglycerides 1.16G0.78 mmol/l leveles and the LDL 2.96G1.1* mmol/l level
reduced significantly (*P!0.05).
It is important to notice that hypoestrogenemia in women of reproductive age
with HH leads to dislipidemia and HRT taking can somehowe correct this
unpleasant changes.
Rare polimorphism in the intron of human Agouti- related protein gene
is associated with obesity
Ivo Kapa1, Ineta Kalnina1, Valdis Pirags1, Helgi Schioth2 & Janis Klovins1
Latvian Biomedical Centre, Riga, Latvia; 2Uppsala University, Uppsala,
Agouti related protein (AGRP) as a endogenous antagonist of melanocortin 4
receptor plays an important role in regulation of food intake and energy balance
being one of the most potent orexigenic factors. We have determined complete
sequence of AGRP gene and upstream promoter region in 100 patients with
severe obesity (BMIO35). Three previously described polymorphisms were
identified: silent mutation G538A in second exon, non-synonymous mutation
G772A (rs5030980) and C662T located in second intron. Association of C662T
mutation with obesity this far has not been studied. We further screened this SNP
in the cohort of 1173 patients from Latvian Genome database. Carriers of C662T
polymorphism had significantly higher BMI when analyzed in all subjects (PZ
0.017) and in men separately (PZ0.028). Mean BMI levels were adjusted for
other non-genetic factors including age, status of type 2 diabetes cardiovascular
disease and other diseases. After adjustment BMI levels remained significantly
higher in men carriers of C662T polymorphism (PZ0.035): mean BMI value
(with 95% confidence interval) was 29.768 (26.738–33.572) for CT genotype
compared with 26.816 (26.432–27.208) for CC genotype. The association of
C662T with higher BMI in women was not significant (PZ0.051). The present
study presents for the first time the association of AGRP polymorphism C662T
with obesity in men. The possible functional effects of polymorphism are unclear
and may involve splicing defects. Present study has been approved by Latvian
Central Committee of Medical Ethics.
Endocrine Abstracts (2007) Vol 14
9th European Congress of Endocrinology, Budapest, Hungary, 2007
The relationship between plasma androgens (testosterone and dehydroepiandrosterone sulfate), insulin resistance and visceral obesity in
elderly men
Michal Rabijewski, Lucyna Papierska & Wojciech Zgliczynski
Department of Endocrinology; Medical Center for Postgraduate Education,
Warsaw, Poland.
In elderly men testosterone and DHEAS deficiency is often observed, also
changes of body composition and metabolic disturbances are common disorders.
The aim of this study was to analyze the association between testosterone and
DHEAS deficiency and waist/hip ratio (WHR) and also levels of glucose, insulin,
HOMA and FG/FI ratio in elderly men as well as analysis, whether these sex
hormones influent on measured parameters separately.
Material and methods
Together 85 men with age from 60 to 70 years men (mean 66.3G1.5 years) was
analyzed. Testosterone levels!4 ng/ml or DHEA levels!2000 ng/ml and
BMI!30 kg/m2 were including criteria. Patients were divided into three groups:
52 with testosterone deficiency (L-T), 32 with DHEA deficiency (L-DHEA-S)
and 67 with deficiency of both sex hormones (L-T/DHEA-S).
Testosterone levels in L-T, L-DHEA and L-T/DHEA groups were
respectively 3.19G0.23 ng/ml, 4.89G0.45 ng/ml and 3.25G0.34 g/ml (P!
0.002). While DHEA-S levels were respectively: 2498G98 ng/ml, 1435G
1010 ng/ml and 1501G89 ng/ml). BMI values do not deferent between
groups. WHR ratio values were the highest in L-T/DHEA-S group (P!0.05
vs. L-T) group, significant lower in L-T group (P!0.005 vs. L-DHEA-S)
and the lowest in L-DHEA-S group. Insulin fasting levels were lowest in
L-DHEA-S group, higher in L-T group (P!0.01) and highest in LT/DHEA-S group (P!0.001 vs, L-T group). FG/FI values were highest in
L-DHEA-S group, lower in L-T group (NS) and lowest in L-T/DHEA group
(P!0.002 vs. L-T group). HOMA ratio values similarly did not change
significantly between L-T (6.6G3.21) and L-DHEA-S group (5.5G2.92),
although tendency to higher values in L-T group was noticed, while WHR
ratio values were significant higher in L-T/DHEA group (7.3G2.45; P!
0.002 vs. L-T group).
DHEAS and testosterone deficiency were independently associated with higher
insulin resistance and obesity and also WHR ratio is more sensitive then BMI
ratio reflects androgen deficiency influence on obesity and body composition in
elderly men.
Prevalence of metabolic syndrome in a cohort of young Mediterranean
women with polycystic ovary syndrome and association with clinical
and biochemical parameters
Laura Patton, Alessandra Gambineri, Andrea Repaci, Giulia Forlani,
Uberto Pagotto & Renato Pasquali
Endocrine Unit, Internal Medicine Department, S. Orsola-Malpighi
Hospital, Bologna, Italy.
The purpose of the study was to evaluate the prevalence of the metabolic
syndrome (MS) in a cohort of young Mediterranean women with PCOS in
reproductive age and to evaluate the association of the MS with clinical and
biochemical parameters.
Among 200 PCOS (17-31 years) criteria of MS in accordance with the “NCEPATPIII” were used to construct 3 groups: no one criteria, 1 or 2 criteria and 3 or
more criteria (affected by MS). All patients underwent clinical, hormonal and
metabolic assessments.
36 women had no criteria, 101 women had 1 or 2 criteria, 63 women had 3 or more
criteria. We found a prevalence of the MS of 31.5%. The women with MS had
higher BMI, waist circumference and WHR than the other two groups. Among the
3 groups we found no differences in severity of hirsutism and menses
abnormalities. However, the women with more criteria had more frequently
acanthosis nigricans and less frequently acne. The group with MS respect the
group without any criteria had higher levels of fasting insulin (PZ0.014),
Endocrine Abstracts (2007) Vol 14
glucose-stimulated insulin and glucose levels (P!0.001) and HOMA (PZ0.039)
and lower levels of HOMAOGTT (P!0.001) and QUICKI (P!0.001). Moreover,
we found higher levels of cortisol and androstenedione responsiveness to 1–24
ACTH (PZ0.004, PZ0.040). There were no differences for the levels of
androgens at baseline except for the Free Androgen Index (FAI) which was higher
in the group with MS (PZ0.023). Finally, the levels of SHBG were lower in
patients with the MS respect to patients without any criteria (P!0.001).
Young women of the Mediterranean area present a higher prevalence of the MS
respect to the general population. Moreover, the MS is associated with a more
severe insulin resistance state and hyperandrogenemia and with a hyperactivity of
the hypothalamic-pituitary-adrenal axis.
Obesity: diffusion weighted imaging features of brain
Alpay Alkan1, Ibrahim Sahin2, Lezzan Keskin2, Hakki Muammer Karakas1,
Ayse Sertkaya Cikim2, Zuhal Karaca3, Nedim Turhan3, Ahmet
Kemal Firat1, Ahmet Sigirci1 & Ozkan Ulutas3
Inonu University Faculty of MedicineDepartment Of Radiology, Malatya,
Turkey; 2Inonu University Faculty of Medicine, Department Of Endocrinology and metabolism, Malatya, Turkey; 3Inonu University Faculty of
Medicine, Department Of Internal Medicine, Malatya, Turkey.
Homeostasis of the body weight is maintaining by the interactions between the
different sections of the brain and peripheral tissues. Diffusion weighted magnetic
resonance imaging (DWI) is a method that investigates the microscopic motion of
the water particules in tissues and also depends on measurement of the signal
variations in tissues which is connected with the kinetic energy of the molecules
called; molecular diffusion. The purpose of this work was to detect brain diffusion
abnormalities in obese patients by DWI.
Eighty one obese patients (68 obese (group 1),13 morbid obese (group 2)) and 29
healty control were included. ADC (Appearance Diffusion Coefficience) values
were measured with DWI in the hyppocampus, corpus amygdala, insular cortex,
orbifrontal cortex,middle temporal cortex and cerebellum, and compared with
healty controls.
The ADC values obtained from hypothalamus, hippocampal gyrus,
amygdala, insula, cerebellum and midbrain were significantly increased in
patients compared to controls.There were statistically significant differences
for ADC values that obtained from insula between group 1 (obesity, n: 68)
and controls.There were statistically significant differences for ADC values
that obtained from insula, thalamus, hippocampal gyrus, orbitofrontal cortex,
midbrain, and occipital cortex between group 2 (morbid obesity, n: 13) and
controls. The ADC values were significantly increased in group 2. The ADC
values obtained from orbitofrontal and occipital cortex were significantly
increased in group 2 (n:13) compared to group 1 subjects.The body weight
were positively correlated with hippocampal gyrus, insula, orbitofrontal and
middle temporal cortex ADC values. The BMI were positively correlated
with amygdala, insula, orbitofrontal and middle temporal cortex ADC
Increased ADC values in the hypothalamus, hippocampal gyrus, amygdala,
insula, cerebellum and midbrain. suggest development of the extracellular water
accumulation similar to vasogenic edema in these location.
Key Words: Obesity, Diffusion magnetic resonance imaging.
Hepatic and brain metabolism in young adults with glycogen storage
disease type 1
Martina Mandl1, Daniel Weghuber2, Martin Krssak1, Michael Roden3,
Peter Nowotny1, Atilla Brehm3, Michael Krebs1, Kurt Widhalm2 &
Martin Bischof1
Division of Endocrinology and Metabolism, Department of Internal
Medicine III, Medical University of Vienna, Vienna, Austria; 2Division of
Clinical Nutrition, Department of Pediatrics, Medical University of Vienna,
Vienna, Austria; 3Department of Internal Medicine I, Hanusch Hospital
Vienna, Vienna, Austria.
Glycogen storage disease type 1 (GSD1) is a rare inherited defect of endogenous
glucose production. While children present with severe hypoglycemia the
9th European Congress of Endocrinology, Budapest, Hungary, 2007
propensity for hypoglycemia may decrease with age in these patients. It was the
aim of this study to elucidate the mechanisms for milder hypoglycemia symptoms
in grown up GSD1 patients. Four patients with GSD1 (BMI: 23.2G6.3 kg/m2,
age: 21G3 yr) and four healthy controls matched for BMI (23.1G3.0 kg/m2) and
age (24G3 yr) were studied. Combined 1H/31P-nuclear-magnetic-resonancespectroscopy was used to assess brain metabolism. Before and after
administration of 1 mg glucagon endogen glucose production (EGP) was
measured with D-[6,6-2H2]glucose while hepatic glucose metabolism was
examined by 1H/13C/31P-NMRS. At baseline GSD1 patients exhibited significantly lower rates of EGP (0.53G0.04 vs. 1.74G0.03 mg$kgK1$min-1, P!0.01
vs. control) but an increased intrahepatic glycogen (502G89 vs. 236G11 mmol/l,
PZ0.05 vs. control) and lipid content (16.3G1.1 vs. 1.4G0.4%, P!0.001 vs.
control). After glucagon challenge, EGP did not change in GSD1 patients
(0.53G0.04 vs. 0.59G0.24 mg$kgK1$min-1; PZn.s.) but increased in healthy
controls (1.74G0.03 vs. 3.95G1.34, P!0.0001). In GSD1 patients we found an
exaggerated increase of intrahepatic phosphomonoesters (PME) (0.23G0.08 vs.
0.86G0.19AU, P!0.001) while inorganic phosphate (Pi) even decreased
(0.36G0.08 vs. K0.43G0.17AU, P!0.01). Intracerebral ratios of glucose,
glutamate, and myo-inositol:creatine were higher in GSD1 patients (at least
P!0.05 vs. control, respectively). Hepatic defects of glucose metabolism persist
in grown up GSD1 patients. Upregulation of the glucose and lactate transport at
the blood-brain barrier could be responsible for the amelioration of hypoglycemic
Sex hormone binding globulin (SHBG) levels have been associated with the
development of the metabolic syndrome. In particular, low SHBG levels have
been proposed as an indicator of increased risk for metabolic syndrome in men.
The (TAAAA)n repeat polymorphism SHBG gene is believed to affect SHBG
levels. In vitro experiments have shown that the allele with 6 TAAAA repeats is
associated with decreased transcriptional activity of SHBG gene. The aim of this
study was to examine the possible role of this polymorphism in the metabolic
Subjects and methods
The study population consisted of 44 men with metabolic syndrome aged 51.6G
9.9 years and 100 healthy men. The body mass index was recorded and blood
samples were obtained after overnight fasting for biochemical and hormonal tests.
The fasting glucose to insulin ratio was calculated as an indicator of insulin
resistance. The SHBG (TAAAA)n polymorphism was genotyped in peripheral
blood leucocytes.
Genotype analysis for the (TAAAA)n polymorphism of the SHBG gene in the
patients and controls revealed six alleles having 6–11 TAAAA repeats. The
distribution of the alleles between patients and the control group did not show
statistically significant differences. However, the 6/6 genotype was more frequent
in patients with metabolic syndrome compared to healthy men (22.7% vs 11%,
PZ0.05). The small number of patients did not allow any association between
polymorphism and biochemical parameters.
The (TAAAA)n polymorphism of SHBG gene appears to be associated with
metabolic syndrome
Body composition and GH status in morbidly obese females before and
after laparoscopic silicone adjustable-gastric banding
Silvia Savastano1, Annamaria Colao1, Francesca Rota1, Laura Vuolo1,
Maria Cristina Savanelli1, Teresa Cascella1, Francesco Orio1,
Luigi Angrisani2, Gaetano Lombardi1 & Carolina Di Somma1
Department of Molecular and Clinical Endocrinology, Federico II
University, Naples, Italy; 2Department of Surgery, S.Giovanni Bosco
Hospital ASL NA1, Naples, Italy.
The GH/IGF-I axis function are reported to ameliorate after weight-loss. Bariatric
surgery leads to a significant weight loss in morbidly obese patients. We
investigated the relationships between GH/IGF-I axis and body composition in 20
morbidly obese females (BMI: 44.8G4.7; waist circumference (W) 119.5G7.2
cm, age 33.7G11.7 yrs) with a normal glucose tolerance, before and after
laparoscopic silicone adjustable-gastric banding (LASGB). The GH axis was
evaluated by GH response after GHRHCarginine test and IGF-I levels. Patients
were evaluated 6 months after surgery and a well balanced mildly hypocaloric
diet. Fat Mass (FM), Free Fat Mass (FFM) were evaluated by bioimpedance
analysis. Before surgery, 8 (40%) subjects were GH deficient (peak GH!4.2
mg/l), while 7 (35%) had IGF-I levels below the normal values for age and sex.
Postoperatively, GH response was persistently impaired in 3 (15%) subjects,
while IGF-I levels were still reduced in 9 (45%). After 6 months BMI, W, FM
(P!0.001) and FFM (PZ0.03) were significantly reduced. The percent
decrement of FM was greater than that of FFM (22.4G16% vs 5.6G2.3%;
P!0.001). GH response was persistently impaired in 3 (15%) subjects, while
IGF-I levels were still reduced in 9 (45%). In addition, a significant correlation
was found between the decrement of FFM (rZ0.81; P!0.001) and that of FM
(rZ0.47; P!0.04) and the decrement of IGF-I. At the multiple regression
analysis, the percentage of FM and W at baseline were the major determinants of
IGF-I. In conclusion, both the nutritional status and a relative malabsorption
might affect IGF-I and FFM. After bariatric surgery and after the initial acute
negative energy balance, a persistent deficiency in GH/IGF-I axis is present and
this particular endocrine profile is also associated to unfavourable body
composition changes. The low IGF-I levels might represent a possible marker
of an underlying persistent catabolic state in these subjects.
The importance of (TAAAA)n polymorphism of SHBG gene in the
metabolic syndrome
Nektaria Xita1, Charalambos Milionis2, Ioannis Georgiou3, Moses Elisaf2 &
Agathocles Tsatsoulis1
Department of Endocrinology, University of Ioannina, Ioannina, Greece;
Department of Medicine University of Ioannina, Ioannina, Greece;
Laboratory of Reproductive Genetics, University of Ioannina, Ioannina,
Exophthalmos and its relation to adipokines in obese men
Sinan Caglayan1, Gokhan Ozisik2, Melih Unal3, Omer Ozcan4 &
Metin Ozata2
Kasimpasa Military Hospital, Division of Endocrinology and Metabolism,
Istanbul, Turkey; 2GATA Haydarpasa Teaching Hospital, Division of
Endocrinology and Metabolism, Istanbul, Turkey; 3GATA Haydarpasa
Teaching Hospital, Division of Ophthalmology, Istanbul, Turkey; 4GATA
Haydarpasa Teaching Hospital, Division of Biochemistry, Istanbul, Turkey.
Up to date, many studies were performed regarding the relationship between
obesity and inflammation, and exophthalmos which is developed in thyroidassociated ophthalmopathy (Graves’ ophthalmopathy). Several studies suggest
that transforming orbital preadipocytes into adipocytes may cause exophthalmos because of the inflammation. Therefore, we examined the relationship
exophthalmos and obesity which is also called low-grade systemic
inflammation. We investigated the relationship between Hertel exophthalmometry values and plasma leptin, adiponectin, TNF-a, IL-6 and IL-1b levels in
52 obese and 34 healthy men who don’t smoke and have any systemic
Plasma leptin, adiponectin, TNFa, IL-6 and IL-1b levels were 25.28G
8.98 ng/mL, 0.41G0.24 mg/mL, 305.53G153.82 pg/mL, 63.99G20.30 pg/mL
ve 95.22G69.54 pg/mL respectively, in obese group, whereas these levels
were 2.66G1.81 ng/mL, 1.17G0.98 mg/mL, 69.31G50.22 pg/mL, 18.84G
11.12 pg/mL ve 21.77G6.84 pg/mL respectively, in control group. Hertel
exophthalmometry values were found as 18.90G1.63 mm in obese group and
16.88G1.69 mm in control group. When obese group’s variables compared to
control group’s variables, plasma adiponectin levels were found significantly
lower whereas the other variables were found significantly higher in obese
group (P!0.05). In multiple regression models using backwards stepwise
regression, we only found that the dependent variable, BMI, was predicted by
leptin and TNF-a (PZ0.004 ve PZ0.052, respectively).
Our results suggest that the inflammation which is resulted by secreted
adipokines and cytokines from adipose tissue might be associated with
exophthalmos in obesity. Nevertheless, the lack of correlation between Hertel
exophthalmometry values and BMI, plasma leptin, adiponectin, TNFa, IL-6
and IL-1b levels shows that there is no directly relation between
exophthalmos and adipokines which causes inflammation in obesity.
Endocrine Abstracts (2007) Vol 14
9th European Congress of Endocrinology, Budapest, Hungary, 2007
Influence of orlistat on adiponectin levels in obese women
Marianthi Tzoitou1, Evridiki Papadopoulou1, Athanasios Papageorgiou1,
A Galactidou2, Marina Kita1, Anargyros Kourtis1, Pavlos Poulakos1 &
Avraam Avramidis1
Endocrinology Clinic Ippokratio General Hospital, Thessaloniki, Greece;
Research Department Theagenio Hospital, Thessaloniki, Greece.
The polymorphism of PPAR and susceptibility to atherosclerosis in
children with low birth weight (below 2500 g)
Ewa Barg, Anna Skoczynska, Beata Wikiera, Dorota Chacka, Ewa Glab,
Arleta Lebioda & Barbara Turczyn
Wroclaw Medical University, Wroclaw, Poland.
Adiponectin is secreted by adipocytes and has been linked to glucose and lipid
regulation. Obesity, diabetes and atherosclerosis have been associated with
reduced adiponectin levels. Orlistat lowers lipids and improves insulin sensitivity
but its effect on other metabolic parameters is not known.
The purpose of this study is to evaluate the influence of orlistat on metabolic
and hormonal parameters of the adipose tissue.
Materials and methods
Thirty obese female patients with Body Mass Index O30 kg/m2 and mean aged
48.7G12.9yrs and mean weight 92.47G12.5 kg were included. Patients with
diabetes and thyroid disorders were excluded. All patients were on a low calorie
diet one month before treatment with orlistat.Blood samples for glucose, total
cholesterol triglycerides, HDL,LDL,FT4, TSH, insulin and adiponectin were
obtained before and three months after orlistat treatment.
19/30 female (63.3%) have lost over five kilos after three months of treatment and
diet. Mean body weight was 92.47G12.5 kg and 85.45G11.2 kg p!0.05 after
treatment. Statistical signigicant differences between glycose triglycerides,
cholesterol HDL,LDL were observed after treatment with orlistat(101G31.2 vs
85G14.5 mg/dl P!0.05, 207.5G29.8 vs 196.1G25.5 mg/dl P!0.004, 127.5G
50.9 vs 119.2G41.4 mg/dl P!0.001).Insulin levels decreased significantly after
three months of treatment (11.3G2.4 mU/ml vs 9.19G2.7 mU/ml P!0.00).In
contrast adiponectin levels seemed to be increased significantly after treatment
with orlistat.(16.284.5G21.640.6 vs 41.798.5G64.776.1 P!0.00)
In this study it seems that orlistat could effectively manage obesity. It decreases
insulin and increases adiponectin when obese patients reduced caloric intake and
lost weight after three months of treatment.
Children, who are born with low birth weight (less 2500 g) are known to have an
increased risk of developing lipid disturbances and atherosclerosis in later live.
PPAR alpha activity could play a regulatory role in the pathogenesis of
hyperlipidemia and a modulatory role in the control of inflammatory response.
The aim of this study was to determine whether the presence of polymorphism
in gene of peroxisome proliferators-activated receptor(PPAR) alpha is associated
with lipid disturbances and susceptibility to apoptosis in children with low birth
The associations between L162V polymorphism in the gene for PPAR alpha and
lipid peroxidation, lipid profile, activity of caspase3 and apoptosis activation was
examined in 155 children with low birth weight aged 4–11 years, and in 30
children born with normal weight as a control group.
The frequency of the V allele of the L162 polymorphism gene in PPAR alpha
gene in children(0.07) was similar to that in general population(0.06 in controls).
In the group with polymorphism gene 4 children with LBW have the 50 Kb
domain on the DNA electrophoretic profiles, but 7 children with LBW and control
children haven’t it.
The effect of the l162V polymorphism within PPAR alpha gene on the serum total
HDL levels are observed (P!0.001).The levels of HDL and triglycerides and
lipid peroxides were statistically higher in children with gene PPAR
polymorphism (P!0.05) than in those children without polymorphism. Among
all the children with the polymorphism, the group born with LBW presented
higher level of lipid peroxides (P!0.05).
The linear correlations between caspasa 3 and serum cholesterol (rZK0.999,
P!0.05), lipid peroxides and susceptibility of infection (rZK0.769, P!0.05),
In children more susceptible for atheroscerosis in adulthood due to low birth
weight the L162V mutation in PPAR are connected with a protective effect on
lipid pattern
Effect of omega-3 fatty acids on plasma adiponectin levels in Metabolic
syndrome subjects
Dimiter Dimitrov
Medical University Varna, Varna, Bulgaria.
Increased consumption of fish and fish oil as a source of n-3 long chain
polyunsaturated fatty acids (nK3 LC-PUFA), mainly eicosapentaenoic acid
(EPA, 20:5 n-3) and docosahexaenoic acid (DHA, 22:6 n-3) is often associated
with decreased mortality (as well as morbidity) from cardiovascular disease.
Treatment with n-3 LC-PUFA augments circulating adiponectin levels via a
PPARg-dependent mechanism in animal models. Given that adiponectin is
known to exert antiinflammatory effects and enhance insulin sensitivity, it is
conceivable that n-3 LC-PUFA could impede the adipose tissue switch to an
inflammatory gene expression profile in response to obesity via a PPARg- and
adiponectindependent mechanism.
To evaluate the effect of n-3 LC-PUFA on plasma adiponectin levels and
components of the Metabolic syndrome (Met-S).
35 overweight and obese adults (28!BMI!36 kg/m2), aged 18–65 years, having
developed the features of Met-S (IDF definition, 2005) were randomized to 2 gr.
n-3 LC-PUFA daily or placebo for 3 months. All subjects were instructed to
follow ad libitum diet without change in dietary lifestyle during that period.
Metabolic parameters, plasma adiponectrin, insulin resistance (HOMA-IR) and
CRP were measured before and after treatment.
After 3 months, plasma adiponectin concentrations were increased by 44% (P!
0.001). HDL cholesterol concentrations were increased by 10% (P!0.001)
.Triglycerides was decreased by 39%, HOMA –IR decreased with 34% and CRP
decreased with 20%. There were no significant complications resulting from
treatment with n-3 LC-PUFA.
n-3 LC-PUFA may contribute to decreasing the burden of the metabolic
syndrome, such as modulating inflammation, lipid abnormalities, endothelial
function, and blood pressure via adiponectindependent mechanism.
Endocrine Abstracts (2007) Vol 14
Visfatin, adiponectin, leptin and insulin sensitivity in severe obese
women with normal and impaired glucose tolerance
Mirjana Sumarac-Dumanovic1, Dragan Micic1, Maja Georgiev1,
Danica Stamenkovic-Pejkovic1, Jagoda Jorga1, Aleksandra Kenedereski1,
Goran Cvijovic1, Svetlana Zoric1, Carlos Dieguez2 & Felipe Casanueva2
Institute of Endocrinology, Diabetes and Diseases of Metabolism, Clinical
Center of Serbia, Belgrade, Serbia; 2Department of Endocrinology,
University of Santiago de Compostela, Santiago de Compostela, Spain.
Visfatin, a new adipokine, facilitates adipogenesis and has insulin-mimetic
properties. There are data that hyperglycemia causes an increase in plasma
visfatin levels in people with T2DM this increase gets more prominent as the
glucose intolerance worsens. The aim of the study was to investigate plasma
visafatin, leptin and adiponectin in obese women with normal and impaired
glucose tolerance. Thirteen obese women (age: 34.50G2.57 yrs; BMI 35.05G
0.57 kg/m2) with normal glucose tolerance (NGT) and 11 age and BMI matched
obese women (age: 37.0 2.4734.50G2.57 yrs; BMI 38.20G1.81 kg/m2) with
normal fasting and impaired glucose tolerance during oral glucose tolerance test
(OGTT) (IGT) were included in the study. Fasting plasma visfatin (EIA Phoenix,
ng/ml), adiponectin (Linco RIA, ng/ml), leptin (Linco RIA, ng/ml) and insulin
(RIA Inep, mU/l) were measured. OGTT (75 gr of glucose) were performed in all
obese women. Insulin sensitivity (M index: mg/kgBW/min) using hyperinsulinemic euglycemic 2hr clamp was measured before and after weight reduction.
There was no difference in fasting visfatin between NGT and IGT (68.65G4.78
vs. 73.14G5.22, PO0.05), fasting leptin (36.75G3.79 vs. 32.06G3.79, PO0.05)
fasting adiponectin (6.82G1.84 vs. 10.76G4.14, PO0.05) and fasting insulin
(17.34G1.44 vs. 19.08G2.65, PO0.05). Insulin sensitivity was reduced in obese
women with IGT (5.36G0.63 vs. 2.81G0.39, P!0.05) while waist circumference were greater in the same subgroup of obese women (101.07G3.12 vs.
113.18G3.60, P!0.05). There was significant correlation between M index and
waist in obese women (rZK0.67, P!0.05). In conclusion, decreased insulin
sensitivity is confirmed in severe obese women with IGT. Our data suggest that
impairment in insulin sensitivity precede change in adipocytokines during
development of type 2 diabetes in obesity.
9th European Congress of Endocrinology, Budapest, Hungary, 2007
Signal transduction – presented on Sunday
Characterization of the rat homologue of the human neuroendocrine
marker secretagogin – new functional implications by in vitro studies
Wolfgang Gartner1, Greisa Vila4, Teodora Daneva2, Felic Koc-Saral1,
Otto Majdic3, Anastasia Nabokih1, Anton Luger4 & Ludwig Wagner1
Medical University Vienna, Department of Medicine III, Vienna, Austria;
Bulgarian Academy of Sciences, Institute of Molecular Immunology, Sofia,
Bulgaria; 3Medical University Vienna, Department of Immunology, Vienna,
Austria; 4Medical University Vienna, Department of Endocrinology and
Metabolism, Vienna, Austria.
Establishment of rodent in vitro cell systems for the extension of the functional
data about the recently cloned neuroendocrine marker secretagogin.
1. DNA-cloning; 2. Antibody generation; 3. Immunoblotting and Immunohistochemistry; 4. Cell-transfection; 5. Luciferase Reporter Assays; 6. ELISA.
1. We characterized the rat homologue of human secretagogin (rat secretagogin)
and demonstrated the homologous tissue expression pattern of both proteins. 2.
Highest rat secretagogin expression levels were found in rat pancreatic islets and
in the rat insulinoma cell lines Rin-5F and INS-1. 3. There exists a considerable
degree of sequence homology between human and rat secretagogin, indicating
comparable functional properties. 4. Overexpression of rat secretagogin in Rin-5F
and in INS-1 cells induced an increase in insulin secretion and expression, which
is mediated mainly via the promoter elements AP-1 and CRE. 5. Insulin and rat
secretagogin are secreted in an inverse ratio by Rin-5F and INS-1 cells upon
incubation with dexamethasone and other agents kno