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Cytochrome c Adducts with PCB Quinoid Metabolites

机译:具有PCB醌类代谢物的细胞色素c加合物

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摘要

PCBs are a group of 209 individual congeners widely used as industrial chemicals. PCBs are found as by-products in dye and paint manufacture and are legacy, ubiquitous and persistent as human and environmental contaminants. PCBs with fewer chlorine atoms may be metabolized to hydroxy- and dihydroxy- metabolites and further oxidized to quinoid metabolites both in vitro and in vivo. Specifically, quinoid metabolites may form adducts on nucleophilic sites within cells. We hypothesized that the PCB-quinones covalently bind to cytochrome c and thereby cause defects in the function of cytochrome c. In this study synthetic PCB quinones (2-(4’-chlorophenyl)-1,4-benzoquinone, 2-(3’, 5’-dichlorophenyl)-1,4-benzoquinone, 2-(3’,4’, 5’-trichlorophenyl)-1,4-benzoquinone, and 2-(4’-chlorophenyl)-3,6-dichloro-1,4-benzoquinone) were incubated with cytochrome c, and adducts were detected by LC-MS and MALDI TOF. SDS PAGE gel electrophoresis was employed to separate the adducted proteins, while trypsin digestion and LC-MS/MS were applied to identify the amino acid binding sites on cytochrome c. Conformation change of cytochrome c after binding with PCB3-para-quinone was investigated by SYBYL-X simulation and cytochrome c function was examined. We found that more than one molecule of PCB-quinone may bind to one molecule of cytochrome c. Lysine and glutamic acid were identified as the predominant binding sites. Software simulation showed conformation changes of adducted cytochrome c. Additionally, cross-linking of cytochrome c was observed on the SDS PAGE gel. Cytochrome c was found to be in the reduced form after incubation with PCB quinones. These data provide evidence that the covalent binding of PCB quinone metabolites to cytochrome c may be included among the toxic effects of PCBs.
机译:多氯联苯是由209个单独的同类物组成的一组,广泛用作工业化学品。多氯联苯被发现是染料和油漆生产中的副产品,并且是遗留的,无处不在且持久存在的人和环境污染物。氯原子较少的PCB在体内和体外均可代谢为羟基和二羟基代谢物,并进一步氧化为醌型代谢物。具体而言,醌类代谢物可在细胞内的亲核位点上形成加合物。我们假设PCB醌共价结合到细胞色素c,从而导致细胞色素c功能的缺陷。在这项研究中,合成PCB醌(2-(4'-氯苯基)-1,4-苯醌,2-(3',5'-二氯苯基)-1,4-苯醌,2-(3',4',5将'-(三氯苯基)-1,4-苯醌和2-(4'-氯苯基)-3,6-二氯-1,4-苯醌)与细胞色素c一起孵育,并通过LC-MS和MALDI TOF检测加合物。 SDS PAGE凝胶电泳用于分离加合的蛋白质,而胰蛋白酶消化和LC-MS / MS则用于鉴定细胞色素c上的氨基酸结合位点。通过SYBYL-X模拟研究了与PCB3-对醌结合后细胞色素c的构象变化,并检测了细胞色素c的功能。我们发现,多于一分子的PCB醌可能与一分子的细胞色素c结合。赖氨酸和谷氨酸被确定为主要的结合位点。软件仿真显示加合物细胞色素c的构象变化。另外,在SDS PAGE凝胶上观察到细胞色素c的交联。与PCB醌孵育后,发现细胞色素c呈还原形式。这些数据提供了证据表明,PCB醌代谢物与细胞色素c的共价结合可能包括在PCB的毒性作用中。

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