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¹ Endocrine Unit, Department of Clinical and Experimental Medicine and Surgery and ² Endo-Surgery Unit, Second University of Naples, 80131 Naples, Italy ³ Pathology Section, Department of Surgical Science, University of Foggia, 71100 Foggia, Italy Departments of ⁴ Molecular and Clinical Endocrinology and Oncology and ⁵ Radiology, ‘Federico II’ University of Naples, Naples, 80131 Italy

(Correspondence should be addressed to D Pasquali who is now at Cattedra di Endocrinologia, Seconda Università di Napoli, Via Pansini 5, Building 16, 80131 Napoli, Italy Email: daniela.pasquali{at}unina2.it)

Surgery is the primary therapy for pheochromocytoma (PHEO), a catecholamine-producing tumor. Benign and malignant PHEO could develop recurrences, and the intraoperative risk of recurrent PHEO is an important unresolved issue. Non-surgical treatments of PHEO recurrence would therefore better prepare patients for reintervention as well as provide them with palliative management. We investigated the effects of the new somatostatin analog (pasireotide) SOM230 versus octreotide (OCT) in primary PHEO cell cultures (Pheo-c). Pheo-c from six benign surgical samples were set up and characterized by immunocytochemistry. Real-time PCR, using both PHEO tissues and Pheo-c, showed different levels of somatostatin receptor_1–5 mRNA expression. Cells treated with various doses of OCT or SOM230 for 48 and 72 h were analyzed to assess their effects on cell proliferation and apoptosis and catecholamine levels. Even if reduction of cell viability was observed in Pheo-c treated for 48 h with either OCT or SOM230 and this effect increased after 72 h, a more significant inhibition of cell growth as well as a significantly higher induction of apoptosis was seen in Pheo-c treated with SOM230 versus OCT. In particular, apoptosis in Pheo-c was detected after 48 h and was associated with increased expression and activation of caspase-3 and cleaved poly(ADP-ribose) polymerase. OCT 10^–6 M and SOM230 10^–7 M significantly reduced catecholamine levels. Our results indicate that while both OCT and SOM230 modulate cell growth and apoptosis and catecholamine levels in Pheo-c through specific receptors, SOM230 is more effective. This improves our knowledge on the mechanism of SOM230 action in PHEO and supports a possible therapeutic use in benign PHEO recurrence.

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