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高加索吸烟者中CYP2D6基因多态性:肺癌易感性及表型-基因型关系

CYP2D6 gene polymorphism in caucasian smokers: lung cancer susceptibility and phenotype-genotype relationships.

作者信息

Laforest L, Wikman H, Benhamou S, Saarikoski S T, Bouchardy C, Hirvonen A, Dayer P, Husgafvel-Pursiainen K

机构信息

Unit of Cancer Epidemiology, INSERM U521, Institut Gustave-Roussy, Villejuif, France.

出版信息

Eur J Cancer. 2000 Sep;36(14):1825-32. doi: 10.1016/s0959-8049(00)00185-4.

Abstract

Individual susceptibility to smoking-related cancers is proposed to partly depend on a genetically determined ability to metabolise tobacco carcinogens. We previously reported on the association between the activity of the xenobiotic-metabolising enzyme CYP2D6 and lung cancer risk in a hospital-based case-control study among French Caucasian smokers. Here we extended the study to address the effect of four gene-inactivating mutations (CYP2D6()3, ()4, ()5 and ()16) and the gene duplication of the CYP2D6 gene (CYP2D6()2x2 or CYP2D6()1x2) on lung cancer risk in the same population (150 patients with primary lung carcinoma of squamous cell or small cell histology and 172 controls). The risk of lung cancer associated with the CYP2D6 poor metaboliser genotype (odds ratio 1.5, 95% confidence interval 0.5-4.3) did not differ from that in the reference category of extensive metaboliser and ultra-rapid metaboliser genotypes combined. Lung cancer risks for the CYP2D6 PM genotype amongst light smokers (tobacco consumption </=20 g/day) or heavy smokers (>20 g/day) were not significantly different. The present findings agree with the discrepancy between the phenotype-based and genotype-based studies indicated by the recent meta-analyses.

摘要

个体对吸烟相关癌症的易感性部分取决于遗传决定的代谢烟草致癌物的能力。我们之前在一项针对法国白种吸烟者的医院病例对照研究中报告了异源物质代谢酶CYP2D6的活性与肺癌风险之间的关联。在此,我们扩展了该研究,以探讨四种基因失活突变(CYP2D6()3、()4、()5和()16)以及CYP2D6基因的基因重复(CYP2D6()2x2或CYP2D6()1x2)对同一人群(150例鳞状细胞或小细胞组织学的原发性肺癌患者和172例对照)肺癌风险的影响。与CYP2D6慢代谢基因型相关的肺癌风险(比值比1.5,95%置信区间0.5 - 4.3)与广泛代谢型和超快代谢型基因型组合的参考类别相比无差异。轻度吸烟者(烟草消费量≤20克/天)或重度吸烟者(>20克/天)中CYP2D6 PM基因型的肺癌风险无显著差异。目前的研究结果与近期荟萃分析所表明的基于表型和基于基因型的研究之间的差异一致。

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