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增强塑料工人中苯乙烯氧化物 N 末端缬氨酸血红蛋白加合物:药物代谢酶基因多态性的可能影响

Styrene-oxide N-terminal valine haemoglobin adducts in reinforced plastic workers: possible influence of genetic polymorphism of drug-metabolising enzymes.

作者信息

Teixeira J P, Gaspar J, Roma-Torres J, Silva S, Costa C, Roach J, Mayan O, Rueff J, Farmer P B

机构信息

National Institute of Health, Centre of Occupational and Environmental Health, Praça Coronel Pacheco, 15, 4050-453 Porto, Portugal.

Faculty of Medical Sciences UNL, Department of Genetics, Lisbon, Portugal.

出版信息

Toxicology. 2007 Jul 31;237(1-3):58-64. doi: 10.1016/j.tox.2007.04.019. Epub 2007 May 5.

Abstract

Styrene is one of the most important organic chemicals used worldwide. In humans, styrene metabolism involves oxidation by cytochrome P450 monooxygenases (CYPs) to styrene-7,8-oxide, an epoxide thought to be responsible for the genotoxic effects of styrene exposure, and detoxification by means of epoxide hydrolase (mEH) and glutathione S-transferases (GSTs). The objective of this study was to investigate if genetic polymorphisms of metabolic enzymes modulate the level of urinary styrene metabolites and styrene oxide adducts with N-terminal valine of human globin (SO-Hb) in 75 workers occupationally exposed to styrene and 77 unexposed controls. The mean air concentration of styrene in the breathing zone of workers (30.4ppm) was higher than the threshold limit value of 20ppm recommended by the American Conference of Governmental Industrial Hygienists (ACGIH), and the biological exposure index adopted by the ACGIH for exposure to styrene prior to the next shift (MA+PGA=400mg/g creatinine) was exceeded, indicating that styrene exposure for this group of workers was higher than recommended. A highly significant correlation was observed between styrene concentration in the breathing zone and the MA+PGA in urine of workers (r=0.85, P<0.001). The levels of SO-Hb adducts in exposed workers were significantly increased as compared with controls, although no difference was observed between subjects stratified as high and medium exposure categories based on MA+PGA excretion. Regarding the effect of the genetic polymorphisms we found that the level of SO-Hb adducts might be modulated by the predicted mEH enzymatic activity in the exposed workers. From our data we conclude that SO-Hb adduct measurement is a complementary method to MA+PG measurement for assessing exposure to styrene at occupational and environmental levels, which reflects a more extensive exposure period.

摘要

苯乙烯是全球使用的最重要的有机化学品之一。在人体中,苯乙烯代谢包括细胞色素P450单加氧酶(CYPs)将其氧化为苯乙烯-7,8-氧化物,这种环氧化物被认为是苯乙烯暴露产生遗传毒性作用的原因,以及通过环氧化物水解酶(mEH)和谷胱甘肽S-转移酶(GSTs)进行解毒。本研究的目的是调查代谢酶的基因多态性是否会调节75名职业性接触苯乙烯的工人和77名未接触者的尿中苯乙烯代谢物水平以及苯乙烯氧化物与人血红蛋白N端缬氨酸的加合物(SO-Hb)水平。工人呼吸带中苯乙烯的平均空气浓度(30.4ppm)高于美国政府工业卫生学家会议(ACGIH)推荐的20ppm阈限值,并且超过了ACGIH在下一班次之前接触苯乙烯的生物暴露指数(MA+PGA=400mg/g肌酐),这表明该组工人的苯乙烯暴露高于推荐水平。观察到工人呼吸带中的苯乙烯浓度与尿中MA+PGA之间存在高度显著的相关性(r=0.85,P<0.001)。与对照组相比,接触工人的SO-Hb加合物水平显著升高,尽管根据MA+PGA排泄量分为高暴露和中暴露类别的受试者之间未观察到差异。关于基因多态性的影响,我们发现接触工人中预测的mEH酶活性可能会调节SO-Hb加合物的水平。根据我们的数据,我们得出结论,SO-Hb加合物测量是一种补充方法,可用于在职业和环境水平上评估苯乙烯暴露,它反映了更广泛的暴露期。

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