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N-乙酰转移酶2基因多态性:致癌物和单倍型对膀胱癌风险的影响。

N-acetyltransferase 2 genetic polymorphism: effects of carcinogen and haplotype on urinary bladder cancer risk.

作者信息

Hein D W

机构信息

Department of Pharmacology and Toxicology, University of Louisville School of Medicine, Louisville, KY 40292, USA.

出版信息

Oncogene. 2006 Mar 13;25(11):1649-58. doi: 10.1038/sj.onc.1209374.

Abstract

A role for the N-acetyltransferase 2 (NAT2) genetic polymorphism in cancer risk has been the subject of numerous studies. Although comprehensive reviews of the NAT2 acetylation polymorphism have been published elsewhere, the objective of this paper is to briefly highlight some important features of the NAT2 acetylation polymorphism that are not universally accepted to better understand the role of NAT2 polymorphism in carcinogenic risk assessment. NAT2 slow acetylator phenotype(s) infer a consistent and robust increase in urinary bladder cancer risk following exposures to aromatic amine carcinogens. However, identification of specific carcinogens is important as the effect of NAT2 polymorphism on urinary bladder cancer differs dramatically between monoarylamines and diarylamines. Misclassifications of carcinogen exposure and NAT2 genotype/phenotype confound evidence for a real biological effect. Functional understanding of the effects of NAT2 genetic polymorphisms on metabolism and genotoxicity, tissue-specific expression and the elucidation of the molecular mechanisms responsible are critical for the interpretation of previous and future human molecular epidemiology investigations into the role of NAT2 polymorphism on cancer risk. Although associations have been reported for various cancers, this paper focuses on urinary bladder cancer, a cancer in which a role for NAT2 polymorphism was first proposed and for which evidence is accumulating that the effect is biologically significant with important public health implications.

摘要

N - 乙酰基转移酶2(NAT2)基因多态性在癌症风险中的作用一直是众多研究的主题。尽管关于NAT2乙酰化多态性的全面综述已在其他地方发表,但本文的目的是简要强调NAT2乙酰化多态性的一些重要特征,这些特征并未被普遍接受,以便更好地理解NAT2多态性在致癌风险评估中的作用。NAT2慢乙酰化酶表型意味着接触芳香胺致癌物后膀胱癌风险持续且显著增加。然而,确定特定致癌物很重要,因为NAT2多态性对膀胱癌的影响在单芳基胺和二芳基胺之间存在显著差异。致癌物暴露以及NAT2基因型/表型的错误分类会混淆真实生物学效应的证据。对NAT2基因多态性对代谢和遗传毒性、组织特异性表达的影响以及对负责分子机制的阐明的功能理解,对于解释过去和未来关于NAT2多态性在癌症风险中作用的人类分子流行病学调查至关重要。尽管已报道了各种癌症之间的关联,但本文重点关注膀胱癌,这是一种首先提出NAT2多态性作用的癌症,并且有越来越多的证据表明其影响具有生物学意义,对公共卫生具有重要影响。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/150a/1434721/36e27d5859e8/nihms9197f1.jpg

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