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哌仑西平对大鼠胃的细胞保护作用:抗分泌剂细胞保护活性的评估方法

Gastric cytoprotection by pirenzepine in rats: evaluating method for cytoprotective activity by antisecretory agents.

作者信息

Takeda F, Kitagawa H, Kohei H

出版信息

Jpn J Pharmacol. 1985 Aug;38(4):337-46. doi: 10.1254/jjp.38.337.

Abstract

The effects of antisecretory agents, pirenzepine, atropine and cimetidine, on gastric mucosal lesions induced in rats by ethanol, HCI (0.6 N), HCI-acidified 50% ethanol and HCI-acidified 50 mM sodium taurocholate (TCA) were comparatively studied with PGE2. The involvement of gastric acid in the formation of ethanol-induced necrosis was also studied. PGE2 and pirenzepine inhibited necrosis induced by all necrotizing agents at the non-antisecretory doses, and the cytoprotective effect of pirenzepine was not abolished by indomethacin. Atropine and cimetidine did not inhibit HCI-induced necrosis even at the antisecretory dose. Atropine and cimetidine at the antisecretory dose inhibited necrosis induced by ethanol, but did not inhibit the red streaks. The ethanol-induced necrosis was also inhibited by neutralizing intragastric H+ with Tris buffer. In gastric fistula rats, alkalinization of the lumen was observed by exposure to ethanol, but necrosis was not produced. There is a close relationship between the necrosis and intragastric acid. Thus it is assumed that gastric acid is involved in the formation of ethanol-induced necrosis. It was suggested that pirenzepine possesses cytoprotective action which is not related to endogenous PGs. On the other hand, the antiulcer actions of atropine and cimetidine may be due, in a part, to antisecretory effects.

摘要

比较研究了抗分泌剂哌仑西平、阿托品和西咪替丁与前列腺素E2(PGE2)对乙醇、盐酸(0.6N)、盐酸酸化的50%乙醇以及盐酸酸化的50mM牛磺胆酸钠(TCA)诱导的大鼠胃黏膜损伤的影响。还研究了胃酸在乙醇诱导的坏死形成中的作用。PGE2和哌仑西平在非抗分泌剂量下可抑制所有坏死剂诱导的坏死,且哌仑西平的细胞保护作用不会被吲哚美辛消除。即使在抗分泌剂量下,阿托品和西咪替丁也不能抑制盐酸诱导的坏死。抗分泌剂量的阿托品和西咪替丁可抑制乙醇诱导的坏死,但不能抑制红色条纹。用Tris缓冲液中和胃内H+也可抑制乙醇诱导的坏死。在胃瘘大鼠中,暴露于乙醇会导致管腔碱化,但不会产生坏死。坏死与胃内酸之间存在密切关系。因此推测胃酸参与了乙醇诱导的坏死形成。提示哌仑西平具有与内源性前列腺素无关的细胞保护作用。另一方面,阿托品和西咪替丁的抗溃疡作用可能部分归因于抗分泌作用。

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