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人CYP1家族和CYP2A亚家族细胞色素P450酶对1-氯芘的氧化作用:两种CYP1B1和五种CYP2A13等位基因变体的催化作用

Oxidation of 1-chloropyrene by human CYP1 family and CYP2A subfamily cytochrome P450 enzymes: catalytic roles of two CYP1B1 and five CYP2A13 allelic variants.

作者信息

Shimada Tsutomu, Murayama Norie, Kakimoto Kensaku, Takenaka Shigeo, Lim Young-Ran, Yeom Sora, Kim Donghak, Yamazaki Hiroshi, Guengerich F Peter, Komori Masayuki

机构信息

a Laboratory of Cellular and Molecular Biology, Osaka Prefecture University , Osaka , Japan.

b Laboratory of Drug Metabolism and Pharmacokinetics, Showa Pharmaceutical University , Machida , Tokyo.

出版信息

Xenobiotica. 2018 Jun;48(6):565-575. doi: 10.1080/00498254.2017.1347306. Epub 2017 Jul 21.

DOI:10.1080/00498254.2017.1347306
PMID:28648140
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC5780263/
Abstract

1. 1-Chloropyrene, one of the major chlorinated polycyclic aromatic hydrocarbon contaminants, was incubated with human cytochrome P450 (P450 or CYP) enzymes including CYP1A1, 1A2, 1B1, 2A6, 2A13, 2B6, 2C9, 2D6, 2E1, 3A4 and 3A5. Catalytic differences in 1-chloropyrene oxidation by polymorphic two CYP1B1 and five CYP2A13 allelic variants were also examined. 2. CYP1A1 oxidized 1-chloropyrene at the 6- and 8-positions more actively than at the 3-position, while both CYP1B1.1 and 1B1.3 preferentially catalyzed 6-hydroxylation. 3. Five CYP2A13 allelic variants oxidized 8-hydroxylation much more than 6- and 3-hydroxylation, and the variant CYP2A13.3 was found to slowly catalyze these reactions with a lower k value than other CYP2A13.1 variants. 4. CYP2A6 catalyzed 1-chloropyrene 6-hydroxylation at a higher rate than the CYP2A13 enzymes, but the rate was lower than the CYP1A1 and 1B1 variants. Other human P450 enzymes had low activities towards 1-chloropyrene. 5. Molecular docking analysis suggested differences in the interaction of 1-chloropyrene with active sites of CYP1 and 2 A enzymes. In addition, a naturally occurring Thr134 insertion in CYP2A13.3 was found to affect the orientation of Asn297 in the I-helix in interacting with 1-chloropyrene (and also 4-(methylnitrosamino)-1-(3-pyridyl)-1-butanone, NNK) and caused changes in the active site of CYP2A13.3 as compared with CYP2A13.1.

摘要
  1. 1-氯芘是主要的氯代多环芳烃污染物之一,它与包括CYP1A1、1A2、1B1、2A6、2A13、2B6、2C9、2D6、2E1、3A4和3A5在内的人细胞色素P450(P450或CYP)酶一起孵育。还研究了多态性的两种CYP1B1和五种CYP2A13等位基因变体对1-氯芘氧化的催化差异。2. CYP1A1在1-氯芘的6位和8位氧化比在3位更活跃,而CYP1B1.1和1B1.3都优先催化6-羟基化。3. 五种CYP2A13等位基因变体对8-羟基化的催化比对6-羟基化和3-羟基化的催化多得多,并且发现变体CYP2A13.3以比其他CYP2A13.1变体更低的k值缓慢催化这些反应。4. CYP2A6催化1-氯芘6-羟基化的速率高于CYP2A13酶,但低于CYP1A1和1B1变体。其他人类P450酶对1-氯芘的活性较低。5. 分子对接分析表明1-氯芘与CYP1和2A酶活性位点的相互作用存在差异。此外,发现CYP2A13.3中天然存在的苏氨酸134插入会影响I螺旋中Asn297与1-氯芘(以及4-(甲基亚硝基氨基)-1-(3-吡啶基)-1-丁酮,NNK)相互作用时的方向,并导致与CYP2A13.1相比CYP2A13.3活性位点发生变化。

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