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首页> 外文期刊>Toxicological sciences: An official journal of the Society of Toxicology >Atropselective Oxidation of 2,2 ',3,3 ',4,6 '-Hexachlorobiphenyl (PCB 132) to Hydroxylated Metabolites by Human Liver Microsomes and Its Implications for PCB 132 Neurotoxicity
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Atropselective Oxidation of 2,2 ',3,3 ',4,6 '-Hexachlorobiphenyl (PCB 132) to Hydroxylated Metabolites by Human Liver Microsomes and Its Implications for PCB 132 Neurotoxicity

机译:通过人肝微粒体对2,2',3,3',4,6'-甲磺基(PCB 132)的羟基化代谢物氧化及其对PCB 132神经毒性的影响

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Polychlorinated biphenyls (PCBs) have been associated with neurodevelopmental disorders. Several neurotoxic congeners display axial chirality and atropselectively affect cellular targets implicated in PCB neurotoxicity. Only limited information is available regarding the atropselective metabolism of these congeners in humans and their atropselective effects on neurotoxic outcomes. Here we investigate the hypothesis that the oxidation of 2,2',3,3',4,6'-hexachlorobiphenyl (PCB 132) by human liver microsomes (HLMs) and their effects on dopaminergic cells in culture are atropselective. Racemic PCB 132 was incubated with pooled or single donor HLMs, and levels and enantiomeric fractions of PCB 132 and its metabolites were determined gas chromatographically. The major metabolite was either 2,2',3,4,4',6'-hexachlorobiphenyl-3'-ol (3'-140), a 1,2-shift product, or 2,2',3,3',4,6'-hexachlorobiphenyl-5'-ol (5'-132). The PCB 132 metabolite profiles displayed interindividual differences and depended on the PCB 132 atropisomer. Computational studies suggested that 3'-140 is formed via a 3,4-arene oxide intermediate. The second eluting atropisomer of PCB 132, first eluting atropisomer of 3'-140, and second eluting atropisomer of 5'-132 were enriched in all HLM incubations. Enantiomeric fractions of the PCB 132 metabolites differed only slightly between the single donor HLM preparations investigated. Reactive oxygen species and levels of dopamine and its metabolites were not significantly altered after a 24 h exposure of dopaminergic cells to pure PCB 132 atropisomers. These findings suggest that there are interindividual differences in the atropselective biotransformation of PCB 132 to its metabolites in humans; however, the resulting atropisomeric enrichment of PCB 132 is unlikely to affect neurotoxic outcomes associated with the endpoints investigated in the study.
机译:多氯联苯(PCB)与神经发育障碍有关。几种神经毒性同质仪展示轴向手性和术语,影响含有PCB神经毒性的细胞靶标。在人类中这些同源者的常熟性代谢及其对神经毒性结果的心脏心脏切除作用仅提供有限的信息。在这里,我们研究了通过人肝微粒体(HLMS)的2,2',3,3',4,6'-六氯二苯基(PCB 132)的氧化和它们对培养中的多巴胺能细胞的影响是无论选择性的。将外消旋PCB 132与合并或单个供体HLM一起孵育,并且PCB 132的水平和对映体级分及其代谢物在色谱上测定气体。主要的代谢物是2,2',3,4,4',6'-六氯二苯基-3'-OL(3'-140),1,2转液或2,2',3,3 ',4,6'-六氯双苯基-5'-OL(5'-132)。 PCB 132代谢物简档显示了与PCB 132 Atropisomer依赖于PCB 132的差异。计算研究表明,通过3,4-芳烯中间体形成3'-140。 PCB 132的第二种洗脱的阿托聚异构体,首先洗脱3'-140的过度异构体,以及5'-132的第二洗脱的阿托异构体在所有HLM孵育中富集。 PCB 132代谢物的对映体级分仅在研究的单一供体HLM制剂之间略微不同。在将多巴胺能细胞24小时暴露于纯PCB 132取代体后,在24小时暴露于纯PCB 132取差体后,在多巴胺和其代谢物的反应性氧物质和水平并未显着改变。这些发现表明,PCB 132对人类代谢物的心脏反应性生物转化存在的间接差异;然而,由此产生的PCB 132的富集富集不太可能影响与研究中研究的终点相关的神经毒性结果。

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