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细胞色素P450 2A6基因变异及其潜在影响。

CYP2A6 genetic variation and potential consequences.

作者信息

Xu Chun, Goodz Shari, Sellers Edward M, Tyndale Rachel F

机构信息

Centre for Addiction and Mental Health, University of Toronto, Toronto M5S 1A8, Canada.

出版信息

Adv Drug Deliv Rev. 2002 Nov 18;54(10):1245-56. doi: 10.1016/s0169-409x(02)00065-0.

DOI:10.1016/s0169-409x(02)00065-0
PMID:12406643
Abstract

Human cytochrome P450 2A6 (CYP2A6) has been shown to have large interindividual and interethnic variability in levels of expression and activity. This is thought to be largely due to genetic polymorphisms. In recent years, 13 genetic variants (CYP2A6*1-*11 and the gene duplication, *1 x 2) of CYP2A6 have been identified and a number of these have been shown to result in altered CYP2A6 enzyme activity. For example, there are alleles which result in variants that are in inactive (e.g. due to a gene deletion), have decreased activity (e.g. altered enzyme structure or transcriptional activity) or have increased activity (e.g. due to gene duplications). The resulting interindividual variation in metabolic activity may affect the metabolism of CYP2A6 substrates including nicotine, cotinine (the major metabolite of nicotine), several tobacco-specific procarcinogens, coumarin and many toxins. The frequencies of the CYP2A6 alleles vary considerably among different ethnic populations, which may partially explain the interethnic variability found in CYP2A6-related metabolic activity (e.g. nicotine metabolism), behaviors (i.e. smoking) and disease (i.e. lung cancer). Investigations of the genetic variation of CYP2A6 and its resulting effects on metabolism and health consequences are still fairly early; this review summarizes what is presently known about CYP2A6, its genetic variants and their clinical consequences.

摘要

人类细胞色素P450 2A6(CYP2A6)在表达水平和活性方面存在较大的个体间和种族间差异。这被认为主要是由于基因多态性。近年来,已鉴定出13种CYP2A6的基因变异(CYP2A6*1-*11以及基因重复,*1 x 2),其中一些已被证明会导致CYP2A6酶活性改变。例如,有些等位基因会导致产生无活性的变异体(如由于基因缺失)、活性降低的变异体(如酶结构或转录活性改变)或活性增加的变异体(如由于基因重复)。由此产生的个体间代谢活性差异可能会影响CYP2A6底物的代谢,这些底物包括尼古丁、可替宁(尼古丁的主要代谢物)、几种烟草特有的致癌物、香豆素和许多毒素。CYP2A6等位基因的频率在不同种族人群中差异很大,这可能部分解释了在CYP2A6相关代谢活性(如尼古丁代谢)、行为(即吸烟)和疾病(即肺癌)中发现的种族间差异。对CYP2A6基因变异及其对代谢和健康后果的影响的研究仍处于早期阶段;本综述总结了目前关于CYP2A6、其基因变异及其临床后果的已知信息。

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