Malagelada J R, Cortot A
Mayo Clin Proc. 1978 Mar;53(3):184-90.
Cimetidine, like its predecessors burinamide and metiamide, has been shown in vitro to be a specific competitive histamine H2-receptor antagonist. In vivo, it is a potent inhibitor of histamine-stimulated gastric acid secretion in animals and man after both intravenous and oral administration. Doses sufficient to inhibit gastric secretions are without measureable effects on other physiologic systems. The main indication for cimetidine is in the treatment of duodenal ulcer and of the Zollinger-Ellison syndrome. Useful indications are treatment of gastric ulcer and pnacreatic insufficiency. Possible indications are prevention of gastrointestinal bleeding and treatment of peptic esophagitis. The neutrophil toxicity seen with metiamide has so far not been demonstrated with cimetidine; side effects with cimetidine have generally been trivial. In the future, H2-receptor antagonists are likely to become key therapeutic agents in diseases in which gastric acid-pepsin secretion plays a pathogenetic role.
西咪替丁与其前辈药物布立马胺和甲硫米特一样,在体外已被证明是一种特异性竞争性组胺H2受体拮抗剂。在体内,静脉注射和口服后,它都是动物和人类组胺刺激胃酸分泌的强效抑制剂。足以抑制胃酸分泌的剂量对其他生理系统没有可测量的影响。西咪替丁的主要适应证是治疗十二指肠溃疡和卓-艾综合征。有效的适应证是治疗胃溃疡和胰腺功能不全。可能的适应证是预防胃肠道出血和治疗消化性食管炎。到目前为止,西咪替丁尚未出现甲硫米特所见的中性粒细胞毒性;西咪替丁的副作用一般较小。未来,H2受体拮抗剂可能会成为胃酸-胃蛋白酶分泌起致病作用的疾病的关键治疗药物。