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降钙素基因相关肽:胃肠道生长抑素分泌的强效选择性刺激物。

Calcitonin gene-related peptide: a potent and selective stimulator of gastrointestinal somatostatin secretion.

作者信息

Dunning B E, Taborsky G J

出版信息

Endocrinology. 1987 May;120(5):1774-81. doi: 10.1210/endo-120-5-1774.

DOI:10.1210/endo-120-5-1774
PMID:2882997
Abstract

Calcitonin gene-related peptide (CGRP) exists in nerves throughout the gastrointestinal tract and pancreas, and exogenous CGRP has been reported to inhibit many endocrine and exocrine secretions of the gut and pancreas. Because somatostatin also has widespread inhibitory actions and because both gut and pancreatic somatostatin secretion may be under peptidergic control, we examined the influence of CGRP on circulating levels of somatostatin-like immunoreactivity (SLI) and on hormone output from the duodenal lobe of the dog pancreas in situ. Intravenous infusion of human CGRP in anesthetized dogs increased arterial SLI in a dose-dependent manner. During iv infusion of CGRP at 500 pmol/min, the increment of circulating SLI (change at 20 min, +175 +/- 24 fmol/ml) was composed of nearly equimolar amounts of SLI-14 and SLI-28, suggesting an effect of CGRP on both gastric and intestinal somatostatin secretion. The effect of iv CGRP (500 pmol/min) on arterial SLI exceeded those of iv CCK-8 (440 pmol/min), iv isoproterenol (10 nmol/min), and intragastric administration of acidified liver extract. In contrast, salmon calcitonin (500 pmol/min, iv) was without effect. CGRP did not stimulate pancreatic SLI output when infused iv (500 pmol/min) or when infused directly into a pancreatic artery (5 pmol/min). The pancreatic infusion of CGRP decreased insulin output slightly (change at 20 min, -21 +/- 8%), but did not affect glucagon output. We conclude that CGRP is a most effective yet selective stimulator of gastrointestinal somatostatin release, with little influence on islet function. We suggest that exogenous and possibly endogenous neuronal CGRP could exert inhibitory effects on gastrointestinal function via the release of somatostatin.

摘要

降钙素基因相关肽(CGRP)存在于整个胃肠道和胰腺的神经中,据报道外源性CGRP可抑制肠道和胰腺的许多内分泌和外分泌。由于生长抑素也具有广泛的抑制作用,且肠道和胰腺生长抑素的分泌可能受肽能控制,我们研究了CGRP对生长抑素样免疫反应性(SLI)循环水平以及对犬胰腺十二指肠叶原位激素分泌的影响。在麻醉犬中静脉输注人CGRP以剂量依赖方式增加动脉SLI。在以500 pmol/min静脉输注CGRP期间,循环SLI的增加(20分钟时的变化,+175±24 fmol/ml)由几乎等摩尔量的SLI-14和SLI-28组成,提示CGRP对胃和肠道生长抑素分泌均有作用。静脉注射CGRP(500 pmol/min)对动脉SLI的作用超过静脉注射CCK-8(440 pmol/min)、静脉注射异丙肾上腺素(10 nmol/min)和胃内给予酸化肝提取物。相比之下,鲑鱼降钙素(500 pmol/min,静脉注射)无作用。静脉输注CGRP(500 pmol/min)或直接注入胰腺动脉(5 pmol/min)时,CGRP均不刺激胰腺SLI分泌。胰腺内输注CGRP使胰岛素分泌略有减少(20分钟时的变化,-21±8%),但不影响胰高血糖素分泌。我们得出结论,CGRP是胃肠道生长抑素释放的最有效但具选择性的刺激物,对胰岛功能影响很小。我们认为外源性以及可能的内源性神经元CGRP可通过生长抑素的释放对胃肠功能发挥抑制作用。

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Endocrinology. 1987 May;120(5):1774-81. doi: 10.1210/endo-120-5-1774.
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