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餐后胃、胰腺及胆汁对组胺H2受体拮抗剂治疗活动性十二指肠溃疡的反应。

Postprandial gastric, pancreatic, and biliary response to histamine H2-receptor antagonists active duodenal ulcer.

作者信息

Longstreth G F, Go V L, Malagelada J R

出版信息

Gastroenterology. 1977 Jan;72(1):9-13.

PMID:11148
Abstract

Histamine H2-receptor antagonists are potentially useful agents in duodenal ulcer and knowledge of their effect on postprandial digestive events will contribute to their clinical application. We studied the effect of 200- and 300-mg doses of cimetidine, an H2-receptor antagonist, taken with an ordinary meal, on gastric, pancreatic, and biliary function. Both doses significantly reduced acid output and its delivery into the duodenum. Gastric secretory volume and pepsin output were less affected. Acid inhibition was related to blood drug levels and was less than that previously found at night in nocturnal fasting studies. As the stomach emptied the food, the gastric pH rose. The fractional gastric emptying rate, pancreatic enzyme, and bile acid outputs were unaltered. Cimetidine taken orally with meals at these doses is a potent gastric antisecretory agent without affecting other postprandial gastric, pancreatic, or biliary functions.

摘要

组胺H2受体拮抗剂在十二指肠溃疡治疗中可能是有用的药物,了解它们对餐后消化过程的影响将有助于其临床应用。我们研究了与普通餐同服200毫克和300毫克剂量的H2受体拮抗剂西咪替丁对胃、胰腺和胆汁功能的影响。两种剂量均显著降低了胃酸分泌量及其进入十二指肠的量。胃分泌量和胃蛋白酶分泌量受影响较小。胃酸抑制与血药浓度有关,且低于此前夜间禁食研究中的发现。随着胃排空食物,胃内pH值升高。胃排空分数、胰酶和胆汁酸分泌量未改变。这些剂量的西咪替丁与餐同服时是一种有效的胃分泌抑制剂,不影响其他餐后胃、胰腺或胆汁功能。

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