谷胱甘肽S-转移酶M1及其A和B变体作为膀胱癌易感性的宿主因素：一项病例对照研究。

Glutathione S-transferase M1 and its variants A and B as host factors of bladder cancer susceptibility: a case-control study.

作者信息

Brockmöller J, Kerb R, Drakoulis N, Staffeldt B, Roots I

机构信息

Institute of Clinical Pharmacology, Universitätsklinikum Charité, Humboldt University of Berlin, Germany.

出版信息

Cancer Res. 1994 Aug 1;54(15):4103-11.

PMID:8033143

Abstract

Glutathione S-transferase M1 (GSTM1) is a foreign compound-metabolizing enzyme with a heritable complete lack of activity in about 50% of Caucasians. GSTM1 deficiency may predispose individuals to urinary bladder cancer. Thus, a hospital-based case-control study was performed with 296 patients with bladder cancer and 400 controls, investigating this GSTM1 deficiency in relation to environmental risk factors and types of bladder cancer. Frequencies of the GSTM1 gene deletion (genotype, GSTM10/0) and of the allele variants A (mu) and B (psi) of the GSTM1-active trait were determined using an internal standard-controlled polymerase chain reaction technique. Moreover, in all patients GSTM1 expression was quantified in blood by an immunoassay. Of the cases, 59.1% had the GSTM10/0 genotype, in contrast to 50.7% of the controls (odds ratio, 1.40; 95% confidence limits, 1.02-1.92; P = 0.017). The odds ratio after adjustment for age and gender by logistic regression analysis was 1.54 (95% confidence limits, 1.12-2.13). Occupational risk was defined as previous employment in occupations with known increased bladder cancer risk, but the impact of GSTM10/0 was not significantly different in individuals with risk jobs versus those without. The greater proportion of the GSTM1-deficient individuals in the group with cancer was due to a lower frequency of carriers of GSTM1A. The odds ratio for the subgroup of individuals with the GSTM1B phenotype versus carriers of the GSTM1A phenotype in cases versus controls was 1.65 (95% confidence limits, 0.976-2.78; two-tailed Fisher's exact P = 0.057). Analysis of functional GSTM1 activity in a subset of 370 blood samples with the model substrate trans-stilbene oxide confirmed the genetic results and showed that 9 of 10 individuals with mu/psi heterodimers (genotype, GSTM1A/B) had activities above the median of all genetically GSTM1-active individuals (24 pmol/min/1 x 10(6) lymphocytes; P < 0.01), indicating a gene dose relationship for GSTM1. GSTM1 expression in the urinary bladder endothelium detected by immunoassay and immunohistology corresponded to the genotype of the patients. It may be concluded from this study that the heritable GSTM1 deficiency is responsible for 17% (etiological fraction; 95% confidence limits, 2-30%) of bladder cancer cases.

摘要

谷胱甘肽S-转移酶M1（GSTM1）是一种外源性化合物代谢酶，约50%的白种人存在遗传性的完全活性缺失。GSTM1缺乏可能使个体易患膀胱癌。因此，开展了一项基于医院的病例对照研究，纳入296例膀胱癌患者和400例对照，研究这种GSTM1缺乏与环境危险因素及膀胱癌类型的关系。采用内标对照聚合酶链反应技术测定GSTM1基因缺失（基因型，GSTM10/0）的频率以及GSTM1活性性状等位基因变体A（μ）和B（ψ）的频率。此外，对所有患者采用免疫测定法对血液中的GSTM1表达进行定量。病例组中59.1%具有GSTM10/0基因型，而对照组为50.7%（比值比，1.40；95%置信区间，1.02 - 1.92；P = 0.017）。经逻辑回归分析对年龄和性别进行校正后的比值比为1.54（95%置信区间，1.12 - 2.13）。职业风险定义为既往从事已知膀胱癌风险增加职业的工作，但GSTM10/0在有风险工作的个体与无风险工作的个体中的影响无显著差异。癌症组中GSTM1缺乏个体比例较高是由于GSTM1A携带者频率较低。病例组与对照组中具有GSTM1B表型的个体亚组与GSTM1A表型携带者相比的比值比为1.65（95%置信区间，0.976 - 2.78；双侧Fisher精确检验P = 0.057）。用模型底物反式氧化 stilbene对370份血样子集进行功能性GSTM1活性分析，证实了基因检测结果，并显示10例μ/ψ异二聚体（基因型，GSTM1A/B）个体中有9例的活性高于所有基因上GSTM1有活性个体的中位数（24 pmol/min/1×10⁶淋巴细胞；P < 0.01），表明GSTM1存在基因剂量关系。通过免疫测定和免疫组织化学检测膀胱内皮中的GSTM1表达与患者的基因型相符。从这项研究可以得出结论，遗传性GSTM1缺乏导致17%（病因分数；95%置信区间，2 - 30%）的膀胱癌病例。