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CYP1A1基因中紧密连锁的点突变性MspI和异亮氨酸-缬氨酸多态性:芬兰研究人群中与肺癌易感性无关联

Point-mutational MspI and Ile-Val polymorphisms closely linked in the CYP1A1 gene: lack of association with susceptibility to lung cancer in a Finnish study population.

作者信息

Hirvonen A, Husgafvel-Pursiainen K, Karjalainen A, Anttila S, Vainio H

机构信息

Department of Industrial Hygiene and Toxicology, Institute of Occupational Health, Helsinki, Finland.

出版信息

Cancer Epidemiol Biomarkers Prev. 1992 Sep-Oct;1(6):485-9.

PMID:1284589
Abstract

In this study of 87 lung cancer patients, 23 patients with lung disease other than cancer, and 121 healthy controls, no association was found between the MspI restriction fragment length polymorphism (RFLP) of the CYP1A1 gene and lung cancer risk. In the lung cancer population, histological type, smoking, and occupational histories were also examined with respect to increased lung cancer risk. No association was found between the MspI RFLP in the CYP1A1 gene and any of these variables. This is in contrast to the results of an earlier report describing an association between the rare genotype m2m2 and susceptibility to lung cancer in a Japanese population; but another study in Norway found no such association. It is evident that, in the Nordic population, MspI polymorphism in the CYP1A1 gene does not indicate individual susceptibility to lung cancer. We also studied a new point mutation which has recently been closely linked to the MspI restriction site polymorphism in a Japanese study population. This mutation results in an isoleucine-valine amino acid replacement in the heme binding region of human CYP1A1. We obtained a similar linkage in our study, so the discrepancy between the Japanese and the Nordic MspI RFLP findings cannot be based on a different degree of linkage between these two point mutations.

摘要

在这项针对87名肺癌患者、23名患有非癌症肺部疾病的患者以及121名健康对照者的研究中,未发现CYP1A1基因的MspI限制性片段长度多态性(RFLP)与肺癌风险之间存在关联。在肺癌人群中,还就增加的肺癌风险对组织学类型、吸烟情况和职业史进行了检查。未发现CYP1A1基因中的MspI RFLP与这些变量中的任何一个之间存在关联。这与一份早期报告的结果形成对比,该报告描述了罕见基因型m2m2与日本人群中肺癌易感性之间的关联;但挪威的另一项研究未发现此类关联。显然,在北欧人群中,CYP1A1基因中的MspI多态性并不表明个体对肺癌的易感性。我们还研究了一种新的点突变,在日本研究人群中,该突变最近与MspI限制性位点多态性紧密相关。这种突变导致人CYP1A1血红素结合区域中的异亮氨酸 - 缬氨酸氨基酸替换。我们在研究中获得了类似的连锁关系,因此日本和北欧MspI RFLP研究结果之间的差异不能基于这两个点突变之间不同程度的连锁关系。

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