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新型强效H2受体阻滞剂3-[[2-[(二氨基亚甲基)氨基]-4-噻唑基]甲基]-硫代]-N2-氨磺酰基丙脒(YM-11170)对清醒犬组胺和食物诱导的胃酸分泌的影响。

Effect of a new potent H2-blocker, 3-]]]2-[(diaminomethylene)amino]-4-thiazolyl]methyl]-thio]-N2-sulfamoylpropionamidine (YM-11170) on gastric secretion induced by histamine and food in conscious dogs.

作者信息

Takagi T, Takeda M, Maeno H

出版信息

Arch Int Pharmacodyn Ther. 1982 Mar;256(1):49-58.

PMID:6124219
Abstract

The inhibitory effect of a new H2-receptor antagonist YM-11170 on gastric acid response to histamine and food was compared with that of cimetidine in the conscious dog with a Heidenhain pouch. When given intravenously at a steady state of gastric secretion by continuous infusion of histamine. YM-11170 was 42 times more potent and 1.3 times longer-lasting (p less than 0.05) than cimetidine in reducing the total acid output. The higher potency of YM-11170 than that of cimetidine was also demonstrated in oral antisecretory tests with histamine. The oral ED50 relative to i.v. ED50 as an indirect indication of absorption rate of the drugs was 2.9 for YM-11170 and 2.7 for cimetidine. The secretory response to food stimulation was also antagonized by oral administration of YM-11170 with 40 times greater potency than that of cimetidine. The antisecretory effects of the drugs on the histamine-induced gastric secretion were characterized by a marked decrease in the secretory volume. No behavioral change was observed in association with the H2-blockers. These results indicate that YM-11170 is a very potent inhibitor of gastric acid secretion and also suggest that the absorption rate of YM-11170 from the gastro-intestinal tract is similar to that of cimetidine.

摘要

在具有海登海因小胃的清醒犬中,比较了新型H2受体拮抗剂YM - 11170和西咪替丁对组胺和食物引起的胃酸反应的抑制作用。当通过持续输注组胺使胃酸分泌处于稳定状态时静脉给药,在降低总酸分泌量方面,YM - 11170的效力比西咪替丁高42倍,作用持续时间长1.3倍(p < 0.05)。在组胺口服抑酸试验中也证明了YM - 11170比西咪替丁具有更高的效力。作为药物吸收速率的间接指标,相对于静脉注射ED50的口服ED50,YM - 11170为2.9,西咪替丁为2.7。口服YM - 11170也能拮抗食物刺激引起的分泌反应,其效力比西咪替丁高40倍。药物对组胺诱导的胃酸分泌的抑酸作用表现为分泌量显著减少。未观察到与H2阻滞剂相关的行为变化。这些结果表明YM - 11170是一种非常有效的胃酸分泌抑制剂,也提示YM - 11170从胃肠道的吸收速率与西咪替丁相似。

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