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肽YY的肠抑胃素样作用在犬中是由迷走神经介导的。

Enterogastrone-like effect of peptide YY is vagally mediated in the dog.

作者信息

Pappas T N, Debas H T, Taylor I L

出版信息

J Clin Invest. 1986 Jan;77(1):49-53. doi: 10.1172/JCI112300.

Abstract

Intraluminal fat inhibits gastric secretion through as yet undetermined mechanisms which involve release of one or more hormonal enterogastrones. As intraluminal fat releases Peptide YY (PYY) in amounts sufficient to inhibit meal-stimulated acid secretion, this ileo-colonic peptide exhibits the characteristics required of an enterogastrone. The present study seeks to determine the mechanism by which PYY inhibits acid secretion by examining the effects of PYY on gastric acid stimulated by pentagastrin, histamine, and bethanechol. In addition, effects of PYY on the acid response to sham feeding and distention of a denervated gastric pouch were examined. A dose of PYY (400 pmol X kg-1 X h-1) was employed that reproduced blood levels observed after intestinal perfusion with oleic acid and inhibited the acid secretory response to an intragastric meal by 35 +/- 6%. This same dose of PYY maximally inhibited histamine- and pentagastrin-stimulated acid secretion by 28 +/- 7% (P less than 0.05), and 17 +/- 4% (P less than 0.05), respectively. Although PYY had no effect on bethanechol-stimulated secretion it markedly inhibited the secretory response to sham feeding, maximally reducing secretion by 90 +/- 4% (P less than 0.01). We speculate that PYY acts by inhibiting acetylcholine release from vagal nerve fibers rather than by inhibiting acetylcholine's action on the parietal cell. The demonstration that PYY virtually abolishes cephalic phase acid secretion while having little if any effect on the response to exogenous secretogogues gives PYY unique characteristics among the known hormonal inhibitors of gastric secretion.

摘要

腔内脂肪通过尚未明确的机制抑制胃酸分泌,这些机制涉及一种或多种肠抑胃素的释放。由于腔内脂肪释放的肽YY(PYY)量足以抑制进餐刺激的胃酸分泌,这种回肠 - 结肠肽具有肠抑胃素所需的特性。本研究旨在通过检查PYY对五肽胃泌素、组胺和氨甲酰甲胆碱刺激的胃酸的影响,来确定PYY抑制胃酸分泌的机制。此外,还研究了PYY对假饲和去神经胃囊扩张引起的酸反应的影响。采用的PYY剂量(400 pmol·kg⁻¹·h⁻¹)可重现肠道灌注油酸后观察到的血药浓度,并使对胃内进餐的酸分泌反应抑制35±6%。相同剂量的PYY分别最大程度地抑制组胺和五肽胃泌素刺激的胃酸分泌28±7%(P<0.05)和17±4%(P<0.05)。虽然PYY对氨甲酰甲胆碱刺激的分泌没有影响,但它显著抑制假饲的分泌反应,最大程度地减少分泌90±4%(P<0.01)。我们推测PYY通过抑制迷走神经纤维释放乙酰胆碱起作用,而不是通过抑制乙酰胆碱对壁细胞的作用。PYY几乎消除头期胃酸分泌,而对外源性促分泌剂的反应几乎没有影响,这一证明使PYY在已知的胃酸分泌激素抑制剂中具有独特的特性。

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