首页> 外文期刊>Mutation Research: International Journal on Mutagenesis, Chromosome Breakage and Related Subjects >Sister-chromatid exchanges, glutathione S-transferase theta deletion and cytogenetic sensitivity to diepoxybutane in lymphocytes from butadiene monomer production workers.
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Sister-chromatid exchanges, glutathione S-transferase theta deletion and cytogenetic sensitivity to diepoxybutane in lymphocytes from butadiene monomer production workers.

机译:姊妹染色单体交换,谷胱甘肽S-转移酶theta缺失以及对丁二烯单体生产工人的淋巴细胞中的环氧丁烷的细胞遗传敏感性。

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The magnitude of health risks to workers associated with current and past exposures to butadiene has been the subject of considerable recent debate. Butadiene is metabolized in-vivo and in-vitro to the genotoxic intermediates 3,4-epoxybutene and diepoxybutane. Studies in animals and in-vitro systems have clearly demonstrated that 1,3-butadiene is a genotoxin and a potent inducer of sister-chromatid exchanges (SCEs). Data on the genotoxicity of butadiene in humans is, however, limited. Epidemiologic data indicate that butadiene is a probable human carcinogen. Recent work has further demonstrated that cultured lymphocytes from the approximately 20% of the Caucasian population that lack the glutathione S-transferase class theta gene (GSTT1) are relatively sensitive to the induction of cytogenetic damage by butadiene metabolites. In order to test whether butadiene exposure was associated with increases in SCE frequencies in peripheral blood lymphocytes and whether any increase observed could be affected bythe DEB sensitivity-GSTT1 deletion, we studied 40 workers employed in the production of butadiene. In these workers baseline frequencies of SCEs, diepoxybutane-induced SCE frequencies and GSTT1 deletion status were assessed. Questionnaires were administered to each worker and exposure to 1,3-butadiene was determined using three separate approaches. Industrial hygiene personal sampling was used to measure breathing zone butadiene exposure and urine was collected to use in measurement of the urinary butadiene metabolite 1,2-dihydroxy-4-(N-acetylcysteinyl-S-)-butane (M1). Exposure to butadiene was generally below 2 ppm. The urinary metabolite M1 was found in all workers, but it did not correlate significantly with exposure. Six of 40 of the workers were GST theta-deleted DEB sensitive. No measure of acute or chronic exposure to butadiene was associated with an increase in SCE frequency. However, smoking and DEB sensitivity-GSTT1 null status were each significantly associated with elevations in baseline SCE frequency.
机译:与当前和过去接触丁二烯相关的对工人健康的威胁程度一直是近期辩论的主题。丁二烯在体内和体外代谢为遗传毒性中间体3,4-环氧丁烯和二环氧丁烷。在动物和体外系统中的研究清楚地表明,1,3-丁二烯是一种基因毒素,是姐妹染色单体交换(SCE)的有效诱导剂。然而,关于丁二烯对人的遗传毒性的数据是有限的。流行病学数据表明,丁二烯可能是人类致癌物。最近的工作进一步证明,缺少谷胱甘肽S-转移酶类θ基因(GSTT1)的白种人人口中约有20%的培养淋巴细胞对丁二烯代谢物诱导的细胞遗传学损伤相对敏感。为了测试丁二烯暴露是否与外周血淋巴细胞SCE频率增加有关,以及观察到的任何增加是否可能受到DEB敏感性-GSTT1缺失的影响,我们研究了40名丁二烯生产工人。在这些工人中,对SCE的基线频率,二环氧丁烷诱导的SCE频率和GSTT1缺失状态进行了评估。对每位工人进行问卷调查,并使用三种不同的方法确定1,3-丁二烯的暴露水平。工业卫生个人采样用于测量呼吸区丁二烯暴露,收集尿液用于测量尿中丁二烯代谢产物1,2-二羟基-4-(N-乙酰基半胱氨酸-S-)-丁烷(M1)。丁二烯的暴露量通常低于2 ppm。在所有工人中都发现了尿代谢物M1,但它与暴露量没有显着相关。 40名工人中有6名对GST theta删除的DEB敏感。没有测量丁二烯急性或慢性暴露与SCE频率增加有关。但是,吸烟和DEB敏感性-GSTT1无效状态均与基线SCE频率升高显着相关。

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