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Citations to this article

A physiologic role for somatostatin 28 as a regulator of insulin secretion.
D A D'Alessio, … , C Beglinger, J W Ensinck
D A D'Alessio, … , C Beglinger, J W Ensinck
Published September 1, 1989
Citation Information: J Clin Invest. 1989;84(3):857-862. https://doi.org/10.1172/JCI114246.
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A physiologic role for somatostatin 28 as a regulator of insulin secretion.

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Abstract

Somatostatin 28 (S-28) is a peptide produced in the intestinal tract which rises in the circulation during nutrient absorption. We tested the hypothesis that S-28 regulates B-cell function by (a) studying the effects on insulin secretion of "physiologic" infusions of S-28 and (b) measuring insulin responses during elevated nutrient-stimulated endogenous S-28 levels. (a) Synthetic S-28 was infused on separate days into six healthy men at rates of 25 and 50 ng/kg per h which mimicked postprandial levels. Subjects were given a bolus of glucose (0.1 g/kg) after 120 min. Insulin responses during S-28 infusions were compared to a control study using a saline infusion in the same individuals. Glucose-stimulated insulin secretion was inhibited during the infusion of 50 ng/kg per h S-28 when compared to control (P less than 0.05). (b) Insulin secretion during elevations of endogenous S-28 was studied in healthy men who received a bolus of 2.5 g arginine (n = 14) or 25 U of secretin (n = 8) 120 min after swallowing 50 g fat, or, on a separate day, an equivalent volume of water. S-28 levels rose significantly after fat ingestion but did not change after water. Arginine and secretin-stimulated insulin secretion was inhibited following ingestion of fat compared with intake of water (P less than 0.05). Arginine-enhanced glucagon secretion was not changed by fat ingestion. We conclude that elevations in plasma S-28 levels, occurring during the postprandial state, attenuate B-cell secretion and this peptide may be a physiologic modulator of nutrient-stimulated insulin release.

Authors

D A D'Alessio, C Sieber, C Beglinger, J W Ensinck

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Year: 2025 2022 2021 2020 2019 2016 2015 2014 2012 2010 2008 2007 2006 2005 2004 2002 2000 1997 1996 1995 1994 1993 1992 1990 1987 Total
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Citations to this article (41)

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Molecular Metabolism 2025
GLP-1 Receptor Blockade Reduces Stimulated Insulin Secretion in Fasted Subjects With Low Circulating GLP-1
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The Journal of clinical endocrinology and metabolism 2022
Non-glucose modulators of insulin secretion in healthy humans: (dis)similarities between islet and in vivo studies
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Nature Reviews Endocrinology 2021
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MP Yavropoulou, K Kotsa, M Pikilidou, I Keisisoglou, JG Yovos
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Molecular and Cellular Endocrinology 2008
Somatostatin Receptor Subtype-2-Deficient Mice with Diet-Induced Obesity Have Hyperglycemia, Nonfasting Hyperglucagonemia, and Decreased Hepatic Glycogen Deposition
V Singh, C Grötzinger, KW Nowak, S Zacharias, E Göncz, G Pless, IM Sauer, I Eichhorn, B Pfeiffer-Guglielmi, B Hamprecht, B Wiedenmann, U Plöckinger, MZ Strowski
Endocrinology 2007
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1992
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