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细胞色素P450多态性与外源性物质毒性

Polymorphism of cytochrome P450 and xenobiotic toxicity.

作者信息

Ingelman-Sundberg Magnus

机构信息

Division of Molecular Toxicology, Institute of Environmental Medicine, IMM, Karolinska Institute, Box 210, SE-171 77 Stockholm, Sweden.

出版信息

Toxicology. 2002 Dec 27;181-182:447-52. doi: 10.1016/s0300-483x(02)00492-4.

Abstract

The majority of human P450-dependent xenobiotic metabolism is carried out by polymorphic enzymes which can cause abolished, quantitatively or qualitatively altered or enhanced metabolism. The latter situation is due to stable duplication, multiduplication or amplification of active genes, most likely in response to dietary components that have resulted in a selection of alleles with multiple non-inducible genes. An updated list of variant CYP alleles is present at the Home Page of the Human Cytochrome P450 (CYP) Allele Nomenclature Committee (http://www.imm.ki.se/CYPalleles/). Several examples exist where subjects carrying certain alleles suffer from a lack of drug efficacy due to ultrarapid metabolism or, alternatively, adverse effects from the drug treatment due to the presence of defective alleles. Dosage requirements for several commonly used drugs that have a narrow therapeutic range can differ more than 20-fold dependent on the genotype or the enzyme expression status. By contrast, carcinogen metabolising cytochrome P450s are less polymorphic and no firm relationships have been established linking increased risk for cancer with any specific P450 polymorphism. In the present overview recent aspects of cytochrome P450 polymorphism and xenobiotic toxicity are discussed.

摘要

大多数人类依赖细胞色素P450的外源性物质代谢是由多态性酶进行的,这些酶可导致代谢被消除、在数量或质量上发生改变或增强。后一种情况是由于活性基因的稳定复制、多次复制或扩增,很可能是对饮食成分的反应,饮食成分导致了具有多个非诱导性基因的等位基因的选择。人类细胞色素P450(CYP)等位基因命名委员会的主页(http://www.imm.ki.se/CYPalleles/)上有一份最新的CYP变异等位基因列表。有几个例子表明,携带某些等位基因的个体由于代谢过快而缺乏药物疗效,或者由于存在缺陷等位基因而在药物治疗中出现不良反应。几种治疗范围较窄的常用药物的剂量要求因基因型或酶表达状态的不同而相差20倍以上。相比之下,致癌物代谢细胞色素P450的多态性较低,尚未确定癌症风险增加与任何特定的P450多态性之间的明确关系。在本综述中,讨论了细胞色素P450多态性和外源性物质毒性的最新研究进展。

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