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首页> 外文期刊>Chemico-biological interactions >Analysis of hydroquinone and catechol in peripheral blood of benzene-exposed workers.
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Analysis of hydroquinone and catechol in peripheral blood of benzene-exposed workers.

机译:苯接触工人外周血中对苯二酚和邻苯二酚的分析。

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摘要

We have developed a gas chromatography-mass spectrometry method for analysis of benzene (BZ) metabolites in human urine and blood. Here we describe peripheral blood concentrations of hydroquinone (HQ(1)) and catechol (CAT(2)) in total, protein-bound, and unbound (free) forms obtained from BZ-exposed factory workers and controls. Total and unbound metabolites were directly measured in independent experiments, while bound forms were calculated as [total]-[unbound]. In this subset of a larger study, breathing zone benzene, toluene, and xylene were measured for the duration of a workshift, and end-shift blood samples taken from 143 subjects and controls. Potential lifestyle and environmental influences were assessed by questionnaire and bioassay, and single nucleotide polymorphisms in xenobiotic metabolizing enzymes NQO1, MPO, CYP2E1, and GSTT1 were also analyzed for potential contribution to differences in blood metabolite concentration. Total CAT, bound CAT, total HQ, and bound HQ correlated well with benzene exposure, while unbound CAT and HQ displayed no correlation. Nearly all of the metabolites found in blood were bound to protein (CAT 96-99+%, HQ 78-92+%), and when the ratio of bound to unbound metabolites were compared in subsets of exposed workers, the increase in blood metabolite concentration was nearly all due to an increase in the protein-bound molecule. These findings suggest that a threshold for conjugation does not exist within the exposure spectrum studied (0.01-78.8 mg/m(3)). This method demonstrates the feasibility of analyzing benzene metabolites in human blood, and should allow for further investigation of the health effects of benzene and its metabolites.
机译:我们已经开发了一种气相色谱-质谱法,用于分析人尿液和血液中的苯(BZ)代谢产物。在这里,我们描述了从暴露于BZ的工厂工人和控制人员那里获得的总,蛋白结合和未结合(游离)形式的对苯二酚(HQ(1))和邻苯二酚(CAT(2))的外周血浓度。在独立的实验中直接测量了总代谢物和未结合的代谢物,而结合形式被计算为[总]-[未结合]。在这项更大的研究的子集中,测量了呼吸区苯,甲苯和二甲苯的轮班时间,以及从143名受试者和对照组中抽取的轮班终末血液样本。通过问卷调查和生物测定法评估了潜在的生活方式和环境影响,并分析了异种生物代谢酶NQO1,MPO,CYP2E1和GSTT1中的单核苷酸多态性对血液代谢物浓度差异的潜在影响。总CAT,结合的CAT,总HQ和结合的HQ与苯暴露高度相关,而未结合的CAT和HQ没有显示相关性。血液中发现的几乎所有代谢物都与蛋白质结合(CAT 96-99 +%,HQ 78-92 +%),并且当比较暴露工人的子集中与未结合代谢物的结合比率时,血液代谢物的增加浓度几乎全部归因于蛋白质结合分子的增加。这些发现表明,在研究的曝光光谱范围内(0.01-78.8 mg / m(3))不存在共轭阈值。该方法证明了分析人血中苯代谢物的可行性,并应允许进一步研究苯及其代谢物对健康的影响。

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