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首页> 外文期刊>Japanese Journal of Pharmacology >Studies on the Mechanism for the Gastric Mucosal Protection by Famotidine in Rats
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Studies on the Mechanism for the Gastric Mucosal Protection by Famotidine in Rats

机译:法莫替丁对大鼠胃粘膜保护机制的研究

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References(48) Cited-By(10) The effect of famotidine on gastric lesions induced by the decrease in mucosal defensive resistance was investigated in rats and compared with those of cimetidine, pirenzepine and cetraxate. Famotidine (0.03, 0.1 and 0.3 mg/kg, p.o.) inhibited dose-dependently the development of gastric lesions produced by taurocholatehistamine in doses that suppressed histamine-induced acid secretion in pylorus-ligated rats. The H2-antagonist also prevented gastric mucosal lesions induced by taurocholate-serotonin, iodoacetamide, acidified aspirin and acidified ethanol. Cimetidine, pirenzepine and cetraxate showed the inhibitory effects on almost all types of the gastric lesions, but their inhibitory effects were much less potent than those of famotidine. On the other hand, famotidine inhibited the decreases of gastric mucosal blood flow induced by acidified ethanol and the mucosal contents of glycoprotein induced by water immersion restraint stress. In addition, famotidine increased the transgastric potential difference (PD) and promoted the recovery of decreased transgastric PD induced by acidified ethanol in rats. These results suggest that the preventive effect of famotidine on gastric lesions is attributable not only to suppression of acid secretion but to activation of the gastric mucosal defensive mechanisms.
机译:参考文献(48)Cited-By(10)研究了法莫替丁对大鼠黏膜防御抵抗力降低引起的胃部损伤的影响,并与西咪替丁,哌仑西平和头孢曲酯进行了比较。法莫替丁(0.03,0.1和0.3 mg / kg,p.o.)剂量依赖性地抑制牛磺胆酸组胺产生的胃损伤的发展,该剂量可抑制结扎幽门的大鼠中组胺诱导的酸分泌。 H2拮抗剂还可以预防牛磺酸胆碱-5-羟色胺,碘乙酰胺,酸化阿司匹林和酸化乙醇引起的胃粘膜损伤。西咪替丁,哌仑西平和cetraxate对几乎所有类型的胃部病变均显示抑制作用,但其抑制作用远不如法莫替丁。另一方面,法莫替丁抑制酸化乙醇诱导的胃粘膜血流减少和水浸抑制应激诱导的糖蛋白黏膜含量降低。此外,法莫替丁可增加大鼠经胃酸电位差(PD)并促进其恢复。这些结果表明法莫替丁对胃损伤的预防作用不仅归因于酸分泌的抑制,而且归因于胃粘膜防御机制的激活。

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