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保护性药物对人体胃碱性分泌的影响。

Effects of protective drugs on gastric alkaline secretion in man.

作者信息

Konturek S J, Kwiecien N, Obtulowicz W, Hebzda Z, Oleksy J

机构信息

Institute of Physiology, Academy of Medicine, Cracow, Poland.

出版信息

Scand J Gastroenterol. 1987 Nov;22(9):1059-63. doi: 10.3109/00365528708991957.

Abstract

This study was designed to determine the effects of sucralfate, De-Nol, and Maalox 70 on gastric HCO3 secretion in 34 healthy humans. Alkaline secretion was measured after pretreatment with ranitidine to abolish H+ secretion, using a constant perfusion-aspiration system and back-titration of the perfusates to the original pH 6.0. Luminal release of PGE2 was also measured in the gastric perfusates. Addition of sucralfate or De-Nol resulted in increments of gastric HCO3 secretion, reaching about 45% and 59%, respectively, of the maximal HCO3 response to 16,16-dimethyl PGE2 (dmPGE2). The highest response to Maalox 70 reached about 21% of dmPGE2 maximum. These effects of sucralfate, De-Nol, and Maalox 70 were accompanied by a significant increase in luminal release of PGE2. Pretreatment with atropine reduced basal and, in part, sucralfate-, De-Nol-, and Maalox 70-induced alkaline secretion, whereas pirenzepine did not affect this secretion. Aspirin reduced the release of PGE2 by about 80% and suppressed almost completely the gastric HCO3 response to sucralfate, De-Nol, and Maalox 70. This study provides evidence that sucralfate, De-Nol, and Maalox 70 stimulate gastric alkaline secretion via a prostaglandin-dependent mechanism.

摘要

本研究旨在确定硫糖铝、德诺和氢氧化铝镁混悬液(Maalox 70)对34名健康人胃HCO₃分泌的影响。使用恒定灌注-抽吸系统并将灌流液回滴定至初始pH 6.0,在使用雷尼替丁预处理以消除H⁺分泌后测量碱性分泌。还测量了胃灌流液中PGE₂的腔内释放。添加硫糖铝或德诺会导致胃HCO₃分泌增加,分别达到对16,16-二甲基PGE₂(dmPGE₂)最大HCO₃反应的约45%和59%。对氢氧化铝镁混悬液(Maalox 70)的最高反应达到dmPGE₂最大值的约21%。硫糖铝、德诺和氢氧化铝镁混悬液(Maalox 70)的这些作用伴随着腔内PGE₂释放的显著增加。用阿托品预处理可降低基础分泌以及部分由硫糖铝、德诺和氢氧化铝镁混悬液(Maalox 70)诱导的碱性分泌,而哌仑西平不影响这种分泌。阿司匹林使PGE₂的释放减少约80%,并几乎完全抑制了胃对硫糖铝、德诺和氢氧化铝镁混悬液(Maalox 70)的HCO₃反应。本研究提供了证据表明硫糖铝、德诺和氢氧化铝镁混悬液(Maalox 70)通过前列腺素依赖性机制刺激胃碱性分泌。

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