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Role of Somatostatin Signalling in Neuroendocrine Tumours
Authors:Olesja Rogoza  Kaspars Megnis  Marija Kudrjavceva  Aija Gerina-Berzina  Vita Rovite
Affiliation:1.Latvian Biomedical Research and Study Centre, Ratsupites Str 1-k1, LV-1067 Riga, Latvia; (O.R.); (K.M.);2.Pauls Stradins Clinical University Hospital, Pilsonu Str 13, LV-1002 Riga, Latvia; (M.K.); (A.G.-B.)
Abstract:Somatostatin (SST) is a small peptide that exerts inhibitory effects on a wide range of neuroendocrine cells. Due to the fact that somatostatin regulates cell growth and hormone secretion, somatostatin receptors (SSTRs) have become valuable targets for the treatment of different types of neuroendocrine tumours (NETs). NETs are a heterogeneous group of tumours that can develop in various parts of the body, including the digestive system, lungs, and pituitary. NETs are usually slow growing, but they are often diagnosed in advanced stages and can display aggressive behaviour. The mortality rate of NETs is not outstandingly increased compared to other malignant tumours, even in the metastatic setting. One of the intrinsic properties of NETs is the expression of SSTRs that serve as drug targets for SST analogues (SSAs), which can delay tumour progression and downregulate hormone overproduction. Additionally, in many NETs, it has been demonstrated that the SSTR expression level provides a prognostic value in predicting a therapeutic response. Furthermore, higher a SSTR expression correlates with a better survival rate in NET patients. In recent studies, other epigenetic regulators affecting SST signalling or SSA–mTOR inhibitor combination therapy in NETs have been considered as novel strategies for tumour control. In conclusion, SST signalling is a relevant regulator of NET functionality. Alongside classical SSA treatment regimens, future advanced therapies and treatment modalities are expected to improve the disease outcomes and overall health of NET patients.
Keywords:neuroendocrine tumour   somatostatin   somatostatin receptor   somatostatin analogue   octreotide   lanreotide   PRRT
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