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1,3 - 丁二烯及相关化合物的生物监测

Biomonitoring of 1,3-butadiene and related compounds.

作者信息

Osterman-Golkar S, Bond J A

机构信息

Department of Radiobiology, Stockholm University, Sweden.

出版信息

Environ Health Perspect. 1996 Oct;104 Suppl 5(Suppl 5):907-15. doi: 10.1289/ehp.96104s5907.

Abstract

The 1990 Clean Air Act Amendments list several volatile organic chemicals as hazardous air pollutants, including ethylene oxide, butadiene, styrene, and acrylonitrile. The toxicology of many of these compounds shares several common elements such as carcinogenicity in laboratory animals, genotoxicity of the epoxide intermediates, involvement of cytochrome P450 for metabolic activation (except ethylene oxide), and involvement of at least two enzymes for detoxication of the epoxides (e.g., hydrolysis or conjugation with glutathione). These similarities facilitate research strategies for identifying and developing biomarkers of exposure. This article reviews the current knowledge about biomarkers of butadiene. Butadiene is carcinogenic in mice and rats, which raises concern for potential carcinogenicity in humans. Butadiene is metabolized to DNA-reactive metabolites, including 1,2-epoxy-3-butene and diepoxybutane. These epoxides are thought to play a critical role in butadiene carcinogenicity. Butadiene and some of its metabolites (e.g., epoxybutene) are volatile. Exhalation of unchanged butadiene and excretion of butadiene metabolites in urine represent major routes of elimination. Therefore, biomonitoring of butadiene exposure could be based on chemical analysis of butadiene in exhaled breath, blood levels of butadiene epoxides, excretion of butadiene metabolites in urine, or adducts of butadiene epoxides with DNA or blood proteins. Mutation induction in specific genes (e.g., HPRT) following butadiene exposure can be potentially used as a biomarker. Excretion of 1,2-dihydroxy-4-(N-acetylcysteinyl-S)butane or the product of epoxybutene with N-7 in guanine in urine, epoxybutene-hemoglobin adducts, and HPRT mutation have been used as biomarkers in recent studies of occupational exposure to butadiene. Data in laboratory animals suggest that diepoxybutane may be a more important genotoxic metabolite than epoxybutene. Biomonitoring methods need to be developed for diepoxybutane and other putative reactive butadiene metabolites. With butadiene and related compounds, the ultimate challenge is to identify useful biomarkers of exposure in which quantitative linkages between exposure and internal dose of the important DNA-reactive metabolites are established.

摘要

1990年的《清洁空气法修正案》将几种挥发性有机化合物列为有害空气污染物,包括环氧乙烷、丁二烯、苯乙烯和丙烯腈。这些化合物中的许多化合物的毒理学具有几个共同要素,如在实验动物中的致癌性、环氧化物中间体的遗传毒性、细胞色素P450参与代谢活化(环氧乙烷除外)以及至少两种酶参与环氧化物的解毒(例如,水解或与谷胱甘肽结合)。这些相似性有助于制定识别和开发暴露生物标志物的研究策略。本文综述了关于丁二烯生物标志物的现有知识。丁二烯在小鼠和大鼠中具有致癌性,这引发了人们对其在人类中潜在致癌性的担忧。丁二烯被代谢为具有DNA反应性的代谢物,包括1,2-环氧-3-丁烯和1,2,3,4-二环氧丁烷。这些环氧化物被认为在丁二烯致癌性中起关键作用。丁二烯及其一些代谢物(例如环氧丁烯)具有挥发性。呼出未变化的丁二烯和尿液中丁二烯代谢物的排泄是主要的消除途径。因此,丁二烯暴露的生物监测可以基于对呼出气体中丁二烯的化学分析、丁二烯环氧化物的血液水平、尿液中丁二烯代谢物的排泄,或丁二烯环氧化物与DNA或血液蛋白质的加合物。丁二烯暴露后特定基因(例如次黄嘌呤-鸟嘌呤磷酸核糖转移酶)中的突变诱导可潜在地用作生物标志物。1,2-二羟基-4-(N-乙酰半胱氨酰-S)丁烷或环氧丁烯与鸟嘌呤中N-7的产物在尿液中的排泄、环氧丁烯-血红蛋白加合物以及次黄嘌呤-鸟嘌呤磷酸核糖转移酶突变已在近期丁二烯职业暴露研究中用作生物标志物。实验动物的数据表明,1,2,3,4-二环氧丁烷可能是比环氧丁烯更重要的遗传毒性代谢物。需要为1,2,3,4-二环氧丁烷和其他假定的反应性丁二烯代谢物开发生物监测方法。对于丁二烯及相关化合物,最终的挑战是识别有用的暴露生物标志物,其中要建立暴露与重要的具有DNA反应性的代谢物的内部剂量之间的定量联系。

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