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大鼠和人细胞色素 P4501A1(CYP1A1)对 3,3',4,4'-四氯联苯(CB77)的羟化和脱氯作用及其底物结合腔中组成氨基酸的关键作用。

Hydroxylation and dechlorination of 3,3',4,4'-tetrachlorobiphenyl (CB77) by rat and human CYP1A1s and critical roles of amino acids composing their substrate-binding cavity.

机构信息

Graduate School of Agricultural Science, Kobe University, 1-1 Rokkodaicho, Nada-ku, Kobe, Hyogo 657-8501, Japan.

Hyogo Prefectural Institute of Environmental Sciences, 3-1-18 Yukihiracho, Suma-ku, Kobe, Hyogo 654-0037, Japan.

出版信息

Sci Total Environ. 2022 Sep 1;837:155848. doi: 10.1016/j.scitotenv.2022.155848. Epub 2022 May 11.

DOI:10.1016/j.scitotenv.2022.155848
PMID:35568185
Abstract

Cytochrome P450 (CYP) monooxygenases play critical roles in determining the toxicity of polychlorinated biphenyls (PCBs) in mammals. Hydroxylation of PCBs by these enzymes leads to increased water solubility, promoting the elimination of PCBs from the body. The CYP1 family is mainly responsible for metabolizing PCBs that exhibit a dioxin-like toxicity. Although the dioxin-like PCB 3,3',4,4'-tetrachlorobiphenyl (CB77) is abundant in the environment and accumulates in organisms, information on CB77 metabolism by CYP1A1s is limited. In this study, recombinant rat CYP1A1 metabolized CB77 to 4'-hydroxy (OH)-3,3',4,5'-tetrachlorobiphenyl (CB79) and 4'-OH-3,3',4-trichlorobiphenyl (CB35), whereas human CYP1A1 produced only 4'-OH-CB79. Rat CYP1A1 exhibited much higher metabolizing activity than human CYP1A1 because CB77 was stably accommodated in the substrate-binding cavity of rat CYP1A1 and was close to its heme. In a rat CYP1A1 mutant with two human-type amino acids, the production of 4'-OH-CB79 decreased, whereas that of the dechlorinated metabolite 4'-OH-CB35 increased. These results are explained by a shift in the CB77 positions toward the heme. This study provides insight into the development of enzymes with high metabolizing activity and clarifies the structural basis of PCB metabolism, as dechlorination contributes to a drastic decrease in dioxin-like toxicity.

摘要

细胞色素 P450(CYP)单加氧酶在确定多氯联苯(PCBs)在哺乳动物中的毒性方面起着关键作用。这些酶将 PCBs 羟化导致其水溶性增加,促进 PCBs 从体内排出。CYP1 家族主要负责代谢具有类二恶英毒性的 PCBs。尽管环境中存在大量且具有类二恶英毒性的 PCB3,3',4,4'-四氯联苯(CB77),并在生物体中积累,但关于 CYP1A1 代谢 CB77 的信息有限。在这项研究中,重组大鼠 CYP1A1 将 CB77 代谢为 4'-羟基(OH)-3,3',4,5'-四氯联苯(CB79)和 4'-OH-3,3',4-三氯联苯(CB35),而人 CYP1A1 仅产生 4'-OH-CB79。大鼠 CYP1A1 的代谢活性远高于人 CYP1A1,因为 CB77 稳定地容纳在大鼠 CYP1A1 的底物结合腔中并且靠近其血红素。在具有两种人源型氨基酸的大鼠 CYP1A1 突变体中,4'-OH-CB79 的产生减少,而脱氯代谢物 4'-OH-CB35 的产生增加。这些结果可以通过 CB77 位置向血红素的转移来解释。这项研究提供了对具有高代谢活性的酶的发展的深入了解,并阐明了 PCB 代谢的结构基础,因为脱氯作用导致类二恶英毒性急剧降低。

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