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抗惊厥药在体外生物活化成细胞毒性代谢物的结构要求。

Structural requirements for bioactivation of anticonvulsants to cytotoxic metabolites in vitro.

作者信息

Riley R J, Kitteringham N R, Park B K

机构信息

Department of Pharmacology and Therapeutics, University of Liverpool.

出版信息

Br J Clin Pharmacol. 1989 Oct;28(4):482-7. doi: 10.1111/j.1365-2125.1989.tb03530.x.

Abstract

The formation of cytotoxic metabolites from the anticonvulsants phenytoin and carbamazepine was investigated in vitro using a hepatic microsomal enzyme system and human mononuclear leucocytes as target cells. Both drugs were metabolised to cytotoxic products. In order to assess the structural requirements for this bioactivation, a series of structurally related compounds was investigated. It was found that molecules which contain either an amide function or an aryl ring may undergo activation in vitro, but only the metabolism-dependent toxicity of the latter is potentiated by pre-treatment of the target cells with an epoxide hydrolase inhibitor. Taken collectively, these data are consistent with the concept that reactive epoxide metabolites of both phenytoin and carbamazepine may produce toxicity in individuals with an inherited deficiency in epoxide hydrolase.

摘要

利用肝微粒体酶系统和人单核白细胞作为靶细胞,在体外研究了抗惊厥药苯妥英和卡马西平细胞毒性代谢物的形成。两种药物均代谢为细胞毒性产物。为了评估这种生物活化的结构要求,研究了一系列结构相关的化合物。发现含有酰胺官能团或芳环的分子在体外可能会发生活化,但只有后者的代谢依赖性毒性可通过用环氧化物水解酶抑制剂预处理靶细胞而增强。总体而言,这些数据与以下概念一致,即苯妥英和卡马西平的活性环氧化物代谢物可能在环氧水解酶遗传性缺乏的个体中产生毒性。

相似文献

本文引用的文献

6
Phenytoin metabolism in mice.
Drug Metab Dispos. 1982 Mar-Apr;10(2):156-60.
7
Metabolism of carbamazepine.卡马西平的代谢
Drug Metab Dispos. 1982 Jan-Feb;10(1):1-10.
9
Arene oxides: a new aspect of drug metabolism.芳烃氧化物:药物代谢的一个新方面。
Science. 1974 Aug 16;185(4151):573-82. doi: 10.1126/science.185.4151.573.
10
Iminostilbene--a metabolite of carbamazepine isolated from rat urine.
J Pharm Pharmacol. 1973 Apr;25(4):340-1. doi: 10.1111/j.2042-7158.1973.tb10021.x.

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