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Featured researches published by Claudia Teti.


Journal of Molecular Endocrinology | 2009

The clinical-molecular interface of somatostatin, dopamine and their receptors in pituitary pathophysiology

Diego Ferone; Federico Gatto; Marica Arvigo; Eugenia Resmini; Mara Boschetti; Claudia Teti; Daniela Esposito; Francesco Minuto

The role of somatostatin and dopamine receptors as molecular targets for the treatment of patients with pituitary adenomas is well established. Indeed, dopamine and somatostatin receptor agonists are considered milestones for the medical therapy of these tumours. However, in recent years, the knowledge of the expression of subtypes of somatostatin and dopamine receptors in pituitary adenomas, as well as of the coexpression of both types of receptors in tumour cells, has increased considerably. Moreover, recent insights suggest a functional interface of dopamine and somatostatin receptors, when coexpressed in the same cells. This interaction has been suggested to occur via dimerisation of these G-protein-coupled receptors. In addition, there was renewed interest around the concept of cell specificity in response to ligand-induced receptor activation. New experimental drugs, including novel somatostatin analogues, binding to multiple somatostatin receptor subtypes, as well as hybrid somatostatin-dopamine compounds have been generated, and recently a completely novel class of molecules has been developed. These advances have opened new perspectives for the medical treatment of patients with pituitary tumours poorly responsive to the present clinically available drugs, and perhaps also for the treatment of other categories of neuroendocrine tumours. The aim of the present review is to summarise the novel insights in somatostatin and dopamine receptor pathophysiology, and to bring these new insights into perspective for the future strategies in the medical treatment of patients with pituitary adenomas.


European Journal of Endocrinology | 2013

Vitamin D increases circulating IGF1 in adults: potential implication for the treatment of GH deficiency

Pietro Ameri; Andrea Giusti; Mara Boschetti; Marta Bovio; Claudia Teti; Giovanna Leoncini; Diego Ferone; Giovanni Murialdo; Francesco Minuto

OBJECTIVES Previous studies suggested that vitamin D modulates circulating IGF1. We investigated this effect in adults and its clinical relevance in the management of GH deficiency (GHD). DESIGN AND METHODS IGF1 levels were prospectively measured before and after 12 weeks of treatment with oral vitamin D3 (5000 or 7000 IU/week) vs no intervention in 39 subjects 61.9±7.9 years old. The frequency of IGF1 values ≥50th age- and sex-specific percentile in relation to vitamin D status, as determined by the concentration of 25-hydroxyvitamin D (25(OH)D), was retrospectively assessed in 69 GHD patients (57.4±16.6 years) on stable hormone replacement and with 25(OH)D and IGF1 concurrently measured. RESULTS Treatment with 5000 and 7000 IU vitamin D3/week significantly raised 25(OH)D by 12.7±8.4 and 13.1±6.5 ng/ml respectively (both P<0.001 vs baseline). In the 7000 IU group, IGF1 levels also significantly increased by 31.3±36.7 ng/ml (P=0.01). Neither 25(OH)D nor IGF1 significantly varied in controls. IGF1 was ≥50th percentile more frequently in GHD patients with 25(OH)D levels ≥15 than <15 ng/ml (65.9 vs 40.0%, P<0.05). Logistic regression with adjustment for recombinant human GH (rhGH) dose, vitamin D supplements, gender, use of thyroid hormones, corticosteroids or estrogen/testosterone, and season revealed a significant positive association between ≥15 ng/ml 25(OH)D and IGF1 ≥50th percentile (OR 4.4, 95% CI 1.0-18.8, P<0.05). A significant negative correlation between 25(OH)D concentrations and rhGH dose was found after correcting for age and IGF1 (β -0.042, P<0.01), but not after further adjusting for sex, thyroid, adrenal or gonadal replacement, and season (β -0.037, P=0.06). CONCLUSIONS Vitamin D increases circulating IGF1 in adults. As a result, a better vitamin D status may ease the achievement of normal IGF1 values in GHD.


Clinical Endocrinology | 2013

Role of pituitary dysfunction on cardiovascular risk in primary empty sella patients

Annamaria Colao; Oana Ruxandra Cotta; Diego Ferone; Maria Luisa Torre; Francesco Ferraù; Carolina Di Somma; Mara Boschetti; Claudia Teti; Maria Cristina Savanelli; Angela Alibrandi; Francesco Trimarchi; Salvatore Cannavò

Primary empty sella (PES) is a frequent anatomical condition rarely causing pituitary dysfunction. We assessed cardiovascular risk in a cohort of PES patients referred to Endocrine Units.


Hormones (Greece) | 2014

Autonomic nervous system and cardiovascular risk assessment during one year of growth hormone replacement therapy in adults with growth hormone deficiency

Mara Boschetti; Massimo Casu; Sara Moretti; Claudia Teti; Valeria Albanese; Manuela Albertelli; Giovanni Murialdo; Francesco Minuto; Diego Ferone

OBJECTIVE: This prospective study aimed to evaluate the impact of growth hormone deficiency (GHD) on cardiac autonomic tone and on cardiovascular risk and the changes after 12 months of GH replacement therapy (GHRT). GHD is associated with increased cardiovascular morbidity and mortality. This has been attributed to increased markers of cardiovascular risk and to abnormalities of both the cardiac and peripheral autonomic nervous systems. The autonomic cardiac nervous system (ACNS) can be indirectly evaluated by analysis of heart rate variability (HRV) in clinostatism and orthostatism. DESIGN: We compared 14 GHD patients at baseline and after 12 months of GHRT and 17 healthy controls. We analyzed a number of cardiovascular risk factors and we used analysis of HRV during the Tilt Test that identified high frequency (HF) and low frequency (LF), representing parasympathetic and sympathetic activity, respectively. RESULTS: Compared with the control group, in either clinostatism or in orthostatism our patients showed a significantly lower value of LF (P=0.047; P=0.004, respectively), whereas HF was significantly reduced in orthostatism (P=0.037), and indicatively in clinostatism (P=0.065). These values remained unchanged after 12 months of GHRT. No statistically significant differences were found between the LF/HF ratio in untreated and treated patients. In GHD patients, there was a significant reduction of cardiovascular risk in 12 months of replacement therapy (P=0.002). CONCLUSIONS: Our study highlights the absence of sympathovagal imbalance in GHD patients; GHRT does not change ACNS during the first year of GH treatment but it reduces the absolute cardiovascular risk in these patients.


Pituitary | 2015

Pituitary image: pituicytoma

Claudia Teti; Lara Castelletti; Luca Allegretti; Miryam Talco; Gianluigi Zona; Francesco Minuto; Mara Boschetti; Diego Ferone


Endocrine | 2017

One-year GH replacement therapy reduces early cardiac target organ damage (TOD) in adult GHD patients.

Mara Boschetti; Sergio Agosti; Valeria Albanese; Laura Casalino; Claudia Teti; Gian Paolo Bezante; Claudio Brunelli; Manuela Albertelli; Diego Ferone


HORMONES | 2015

THE AUTONOMIC NERVOUS SYSTEM AND CARDIOVASCULAR RISK ASSESSMENT DURING ONE YEAR OF GH REPLACEMENT THERAPY IN ADULTS WITH GH DEFICIENCY

Mara Boschetti; Massimo Casu; Sara Moretti; Claudia Teti; Valeria Albanese; Manuela Albertelli; Giovanni Murialdo; Francesco Minuto; Diego Ferone


Reviews in Endocrinology and Metabolism | 2013

Adult GH deficiency - the value of IGF-I estimation

Mara Boschetti; Claudia Teti; Manuela Albertelli; Francesco Minuto; Diego Ferone


F1000 - Post-publication peer review of the biomedical literature | 2013

Faculty of 1000 evaluation for Radiation-induced hypopituitarism.

Francesco Minuto; Claudia Teti


F1000 - Post-publication peer review of the biomedical literature | 2011

Faculty of 1000 evaluation for Rathke cleft cysts: a review of clinical and surgical management.

Francesco Minuto; Claudia Teti

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Diego Ferone

University of Naples Federico II

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