首页> 美国卫生研究院文献>Toxicological Research >Effects of Styrene-metabolizing Enzyme Polymorphisms and Lifestyle Behaviors on Blood Styrene and Urinary Metabolite Levels in Workers Chronically Exposed to Styrene
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Effects of Styrene-metabolizing Enzyme Polymorphisms and Lifestyle Behaviors on Blood Styrene and Urinary Metabolite Levels in Workers Chronically Exposed to Styrene

机译:苯乙烯代谢酶多态性和生活方式行为对长期接触苯乙烯的工人血液中苯乙烯和尿中代谢物水平的影响

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摘要

The aim of this study was to investigate whether genetic polymorphisms of CYP2E1, GSTM1, and GSTT1 and lifestyle habits (smoking, drinking, and exercise) modulate the levels of urinary styrene metabolites such as mandelic acid (MA) and phenylglyoxylic acid (PGA) after occupational exposure to styrene. We recruited 79 male workers who had received chronic exposure in styrene fiberglass-reinforced plastic manufacturing factories. We found that serum albumin was significantly correlated with blood styrene/ambient styrene (BS/AS), urinary styrene (US)/AS, and US/BS ratios as well as urinary metabolites, that total protein correlated with US/MA and US/PGA ratios, and that low density lipoprotein (LDL)-cholesterol significantly correlated with US/BS, US/MA, and US/PGA ratios. Multiple logistic regression analyses using styrene-metabolizing enzyme genotypes and lifestyle habits as dependent variables and blood and urine styrene concentrations and urine styrene metabolite levels as independent variables revealed that CYP2E1*5 was associated with the MA/US ratio and GSTM1 with US/BS, that a smoking habit was associated with US/AS and MA/US ratios and MA and PGA levels, and that regular exercise was correlated with PGA/US. In conclusion, the results suggested that genetic polymorphisms of styrene-metabolizing enzymes, lifestyle behaviors, and albumin and LDL-cholesterol serving as homeostasis factors together are involved in styrene metabolism.
机译:这项研究的目的是调查CYP2E1,GSTM1和GSTT1的遗传多态性以及生活方式(吸烟,饮酒和运动)是否能调节尿苯乙烯代谢产物的水平,例如扁桃酸(MA)和苯乙醛酸(PGA)。职业接触苯乙烯。我们招募了79名在苯乙烯玻璃纤维增​​强塑料制造工厂中长期暴露的男性工人。我们发现血清白蛋白与血液中的苯乙烯/环境苯乙烯(BS / AS),尿苯乙烯(US)/ AS和US / BS比率以及尿液代谢物显着相关,总蛋白与US / MA和US / PGA比率以及低密度脂蛋白(LDL)-胆固醇与US / BS,US / MA和US / PGA比率显着相关。使用苯乙烯代谢酶基因型和生活方式习惯作为因变量,血液和尿液苯乙烯浓度以及尿液苯乙烯代谢产物水平作为自变量的多重逻辑回归分析显示,CYP2E1 * 5与MA / US比相关,而GSTM1与US / BS相关,吸烟习惯与US / AS和MA / US比率以及MA和PGA水平相关,而经常运动与PGA / US相关。总之,结果表明,苯乙烯代谢酶的遗传多态性,生活方式,以及白蛋白和LDL-胆固醇作为体内稳态因子共同参与了苯乙烯的代谢。

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