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谷胱甘肽S-转移酶M1基因型影响白人、黑人和亚洲吸烟者及非吸烟者的氨基联苯-血红蛋白加合物水平。

Glutathione S-transferase M1 genotype affects aminobiphenyl-hemoglobin adduct levels in white, black and Asian smokers and nonsmokers.

作者信息

Yu M C, Ross R K, Chan K K, Henderson B E, Skipper P L, Tannenbaum S R, Coetzee G A

机构信息

Department of Preventive Medicine, University of Southern California/Norris Comprehensive Cancer Center, Los Angeles 90033, USA.

出版信息

Cancer Epidemiol Biomarkers Prev. 1995 Dec;4(8):861-4.

PMID:8634658
Abstract

Cigarette smoking is the major cause of bladder cancer in men in the United States, and the arylamines contained in cigarettes smoke, including 4-amino-biphenyl (4-ABP), are believed to play an important role in the induction of bladder cancer among smokers. N-acetylation, which is catalyzed by the genetically controlled hepatic N-acetyltransferase enzyme displaying two phenotypes (slow versus rapid), is a detoxification pathway for arylamines with regard to bladder carcinogenesis. In Los Angeles, CA, non-Hispanic white (white), black, and Asian males have comparable smoking habits and yet dramatically different risks of bladder cancer (31 of 100,000 in whites, 16 of 100,000 in blacks, and 13 of 100,000 in Chinese and Japanese). Previously, we have demonstrated that the prevalence of slow acetylators (the high-risk phenotype) was highest in whites (54%), intermediate in blacks (34%), and lowest in Asians (14%). We also showed that mean 3- and 4-ABP hemoglobin adduct levels were significantly higher in cigarette smokers relative to nonsmokers, and that the level increased with increasing number of cigarettes smoke/day. Most importantly, slow acetylators consistently exhibited higher mean levels of ABP hemoglobin adducts relative to rapid acetylators, regardless of race and level of cigarette smoking. We assessed 151 residents of Los Angeles County (CA) who were either white, black, or Asian (Chinese or Japanese) and over the age of 30 years for their glutathione S-transferase M1 (GSTM1) genotype (null versus non-null), acetylator phenotype (slow versus rapid), levels of 3- and 4-ABP hemoglobin adducts, and current use of tobacco products. Whites (27%) had the highest prevalence of the highest risk profile (slow acetylator, GSTM1 null), followed by blacks (15%) and Asians (2.7%), and the difference was statistically significant (P = 0.006). Whites also had less than one-half the prevalence of the "protective" profile (rapid acetylator, GSTM1 non-null) relative to blacks and Asians (23 versus 57%; P = 0.0001). Regardless of race and level of cigarette smoking, mean levels of 3- and 4-ABP hemoglobin adducts were higher in subjects possessing the higher risk (GSTM1/acetylator profile. Mean level of 4-ABP hemoglobin adduct (adjusting for race, cigarette smoking, and acetylator phenotype) was significantly higher in subjects possessing the GSTM1-null versus GSTM1-non-null genotype (46.5 versus 36.0 pg/g Hb; P = 0.037). The comparable difference in mean levels of 3-ABP hemoglobin adduct was borderline significant (1.6 versus 1.1 pg/g Hb; P = 0.07). Thus, our results suggest that GSTM1 is involved in the detoxification of 3- and 4-ABP and may contribute to the racial variation in bladder cancer incidence among white, black, and Asian males in Los Angeles, CA.

摘要

在美国,吸烟是男性膀胱癌的主要病因,香烟烟雾中含有的芳基胺,包括4-氨基联苯(4-ABP),被认为在吸烟者膀胱癌的诱发中起重要作用。N-乙酰化作用由遗传控制的肝脏N-乙酰转移酶催化,该酶表现出两种表型(慢型与快型),就膀胱癌发生而言,是芳基胺的一种解毒途径。在加利福尼亚州洛杉矶,非西班牙裔白人、黑人和亚洲男性有相似的吸烟习惯,但患膀胱癌的风险却有显著差异(白人中每10万人有31例,黑人中每10万人有16例,华人和日本人中每10万人有13例)。此前,我们已证明慢乙酰化者(高危表型)的比例在白人中最高(54%),在黑人中居中(34%),在亚洲人中最低(14%)。我们还表明,吸烟者中3-和4-ABP血红蛋白加合物的平均水平相对于不吸烟者显著更高,且该水平随每日吸烟量的增加而升高。最重要的是,无论种族和吸烟水平如何,慢乙酰化者始终表现出相对于快乙酰化者更高的ABP血红蛋白加合物平均水平。我们评估了加利福尼亚州洛杉矶县151名年龄在30岁以上的居民,他们分别为白人、黑人或亚洲人(华人或日本人),检测了他们的谷胱甘肽S-转移酶M1(GSTM1)基因型(缺失型与非缺失型)、乙酰化表型(慢型与快型)、3-和4-ABP血红蛋白加合物水平以及当前烟草制品使用情况。白人(27%)具有最高风险特征(慢乙酰化者,GSTM1缺失)的比例最高,其次是黑人(15%)和亚洲人(2.7%),差异具有统计学意义(P = 0.006)。相对于黑人和亚洲人(23%对57%;P = 0.0001),白人具有“保护性”特征(快乙酰化者,GSTM1非缺失)的比例不到一半。无论种族和吸烟水平如何,具有较高风险(GSTM1/乙酰化特征)的受试者中3-和4-ABP血红蛋白加合物的平均水平更高。具有GSTM1缺失基因型的受试者中4-ABP血红蛋白加合物的平均水平(校正种族、吸烟和乙酰化表型后)显著高于具有GSTM1非缺失基因型的受试者(46.5对36.0 pg/g Hb;P = 0.037)。3-ABP血红蛋白加合物平均水平的类似差异接近显著(1.6对1.1 pg/g Hb;P = 0.07)。因此,我们的结果表明GSTM1参与3-和4-ABP的解毒作用,并可能导致加利福尼亚州洛杉矶白人、黑人和亚洲男性膀胱癌发病率的种族差异。

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