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神经肽Y和[亮氨酸31,脯氨酸34]神经肽Y对大鼠实验性胃损伤形成及胃分泌的影响。

Effects of neuropeptide Y and [Leu31,Pro34] neuropeptide Y on experimental gastric lesion formation and gastric secretion in the rat.

作者信息

Penner S B, Smyth D D, Glavin G B

机构信息

Department of Pharmacology and Therapeutics, Faculty of Medicine, University of Manitoba, Winnipeg, Canada.

出版信息

J Pharmacol Exp Ther. 1993 Jul;266(1):339-43.

PMID:8101219
Abstract

The present study examined the effects of neuropeptide Y (NPY) and a selective NPY1 receptor agonist, leucine31 proline34 neuropeptide Y ([leu31,pro34]NPY) on gastric lesion formation and gastric secretion in three preparations: Basal gastric acid secretion in conscious rats, restraint-induced gastric lesion formation and acid and pepsin output and gastric mucosal damage in pylorus-ligated rats. The hypothesis that benextramine, a non-selective NPY receptor antagonist, could attenuate responses to NPY or [leu31,pro34]NPY was also tested. Both NPY and [leu31,pro34]NPY (i.p. and i.c.v.) decreased basal gastric acid output, restraint-induced gastric lesion formation, and acid and pepsin secretion and gastric mucosal damage in pylorus-ligated rats. The magnitude of inhibition of secretion and of ulcer reduction was significantly greater for [leu31,pro34]NPY than for NPY at comparable doses. Benextramine blocked the protective effect of NPY and [leu31,pro34]NPY against restraint-induced gastric mucosal injury. Both central and peripheral treatment with benextramine blocked the antisecretory effects of centrally administered NPY and [leu31,pro34]NPY. These data were consistent with both a central and a peripheral action of NPY on the gut, possibly through Y1 receptors.

摘要

本研究在三种实验制剂中检测了神经肽Y(NPY)和一种选择性NPY1受体激动剂,亮氨酸31脯氨酸34神经肽Y([亮氨酸31,脯氨酸34]NPY)对胃损伤形成和胃分泌的影响:清醒大鼠的基础胃酸分泌、束缚诱导的胃损伤形成以及幽门结扎大鼠的胃酸和胃蛋白酶分泌及胃黏膜损伤。还检验了一种非选择性NPY受体拮抗剂苄非他明能否减弱对NPY或[亮氨酸31,脯氨酸34]NPY的反应这一假设。NPY和[亮氨酸31,脯氨酸34]NPY(腹腔注射和脑室内注射)均可降低清醒大鼠的基础胃酸分泌、束缚诱导的胃损伤形成,以及幽门结扎大鼠的胃酸和胃蛋白酶分泌及胃黏膜损伤。在同等剂量下,[亮氨酸31,脯氨酸34]NPY对分泌的抑制程度和溃疡减少程度均显著大于NPY。苄非他明可阻断NPY和[亮氨酸31,脯氨酸34]NPY对束缚诱导的胃黏膜损伤的保护作用。苄非他明的中枢和外周给药均可阻断脑室内注射NPY和[亮氨酸31,脯氨酸34]NPY的抗分泌作用。这些数据与NPY可能通过Y1受体对肠道产生中枢和外周作用的观点一致。

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