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首页> 外文期刊>Toxicological sciences: An official journal of the Society of Toxicology >Formation of 1,2:3,4-Diepoxybutane-Specific Hemoglobin Adducts in 1,3-Butadiene Exposed Workers
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Formation of 1,2:3,4-Diepoxybutane-Specific Hemoglobin Adducts in 1,3-Butadiene Exposed Workers

机译:在1,3-丁二烯暴露工人中形成1,2:3,4-二环氧丁烷特定的血红蛋白加合物

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1,3-Butadiene (BD) Is an important industrial chemical that is classified as a human carcinogen. BD carcinogenicity has been attributed to its metabolism to several reactive epoxide metabolites and formation of the highly mutagenic 1,2:3,4-diepoxybutane (DEB) has been hypothesized to drive mutagenesis and carcieo-genesis at exposures experienced in humans. We report herein the formation of DEB-specific N,N-(2,3-dihydroxy-1,4-butadiyl)valine (pyr-Val) in BD-exposed workers as a biomarker of DEB formation. pyr-Val was determined in BD monomer and polymer plant workers that had been previously analyzed for several other biomarkers of exposure and effect. pyr-Val was detected in 68 of 81 (84%) samples ranging from 0.08 to 0.86 pmol/g globin. Surprisingly, pyr-Val was observed in 19 of 23 administrative control subjects not known to be exposed to BD, suggesting exposure from environmental sources of BD. The mean +- SD amounts of pyr-Val were 0.11 +- 0.07, 0.16 +- 0.12, and 0.29 +- 0.20 pmol/g globie in the controls, monomer, and polymer workers, respectively, clearly demonstrating formation of DEB in humans. The amounts of pyr-Val found in this study suggest that humans are much less efficient in the formation of DEB than mice or rats at similar exposures. Formation of pyr-Val was more than 50-fold lower than has been associated with increased mutagenesis in rodents. The results further suggest that formation of DEB relative to other epoxides is significantly different in the highest exposed polymer workers compared with controls and BD monomer workers. Whether this is due to saturation of metabolic formation or increased GST-mediated detoxification could not be determined.
机译:1,3-丁二烯(BD)是一种重要的工业化学品,被归类为人类致癌物。 BD致癌性归因于它的代谢是由于几种反应性环氧化物代谢产物,据推测,高致突变性的1,2:3,4-二环氧丁烷(DEB)的形成可在人类经历暴露后驱动诱变和致癌作用。我们在这里报道了BD暴露工人中DEB特异的N,N-(2,3-二羟基-1,4-丁二基)缬氨酸(pyr-Val)的形成,作为DEB形成的生物标记。已在BD单体和聚合物工厂的工人中测定了pyr-Val,之前已对它们进行了暴露和影响的其他几种生物标记分析。在81个样品中,有68个(84%)检测到pyr-Val,其球蛋白含量为0.08至0.86 pmol / g。出人意料的是,在23名未知的BD感染中,有19例中有19例观察到吡咯-缬氨酸,表明其暴露于BD的环境来源。对照,单体和聚合物中的pyr-Val平均±SD量分别为0.11±0.07、0.16±0.12和0.29±0.20 pmol / g球蛋白,清楚地证明了人体内DEB的形成。在这项研究中发现的pyr-Val数量表明,与相似暴露量的小鼠相比,人类形成DEB的效率低得多。 pyr-Val的形成比与啮齿类动物诱变增加相关的低50倍以上。结果进一步表明,与对照和BD单体加工剂相比,暴露量最高的聚合物加工剂中,相对于其他环氧化物而言,DEB的形成显着不同。无法确定这是由于代谢形成的饱和还是由GST介导的排毒增加所致。

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