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人及其他哺乳动物肝脏羧酸酯酶对拟除虫菊酯类荧光底物的立体选择性水解作用。

Stereoselective hydrolysis of pyrethroid-like fluorescent substrates by human and other mammalian liver carboxylesterases.

作者信息

Huang Huazhang, Fleming Christopher D, Nishi Kosuke, Redinbo Matthew R, Hammock Bruce D

机构信息

Department of Entomology and Cancer Research Center, University of California, Davis, California 95616, USA.

出版信息

Chem Res Toxicol. 2005 Sep;18(9):1371-7. doi: 10.1021/tx050072+.

DOI:10.1021/tx050072+
PMID:16167828
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC1444893/
Abstract

Mammalian hepatic carboxylesterases (CEs) play important roles in the detoxification of ester-containing pyrethroids, which are widely used for the control of agricultural pests and disease vectors such as mosquitoes. Pyrethroids and pyrethroid-like fluorescent substrates exhibit a consistent pattern of stereoselective hydrolysis by a recombinant murine hepatic CE. We sought to understand whether this pattern is maintained in other hepatic CEs and to unravel the origin of the stereoselectivity. We found that all hepatic CEs tested displayed a consistent pattern of stereoselective hydrolysis: the chiral center(s) in the acid moiety more strongly influenced stereoselective hydrolysis than the chiral center in the alcohol moiety. For cypermethrin analogues with a cyclopropane ring in the acid moiety, trans-isomers were generally hydrolyzed faster than the corresponding cis-isomers. For fenvalerate analogues without a cyclopropane ring in the acid moiety, 2R-isomers were better substrates than 2S-isomers. These general hydrolytic patterns were examined by modeling the pyrethroid-like analogues within the active site of the crystal structure of human carboxylesterase 1 (hCE1). Stereoselective steric clashes were found to occur between the acid moieties and either the catalytic Ser loop (residues 219-225) or the oxyanion hole (residues140-144). These clashes appeared to explain the stereopreference between trans- and cis-isomers of cypermethrin analogues, and the 2R- and 2S-isomers of fenvalerate analogues by hCE1. The implications these findings have on the design and use of effective pesticides are discussed.

摘要

哺乳动物肝脏羧酸酯酶(CEs)在含酯拟除虫菊酯的解毒过程中发挥着重要作用,这类拟除虫菊酯广泛用于控制农业害虫和诸如蚊子等病媒。拟除虫菊酯和类拟除虫菊酯荧光底物通过重组鼠肝脏CE表现出一致的立体选择性水解模式。我们试图了解这种模式在其他肝脏CE中是否保持,并揭示立体选择性的起源。我们发现,所有测试的肝脏CE都显示出一致的立体选择性水解模式:酸部分的手性中心比醇部分的手性中心对立体选择性水解的影响更强。对于酸部分带有环丙烷环的氯氰菊酯类似物,反式异构体通常比相应的顺式异构体水解得更快。对于酸部分没有环丙烷环的氰戊菊酯类似物,2R-异构体比2S-异构体是更好的底物。通过在人羧酸酯酶1(hCE1)晶体结构的活性位点内对类拟除虫菊酯类似物进行建模,研究了这些一般水解模式。发现酸部分与催化性丝氨酸环(残基219 - 225)或氧阴离子洞(残基140 - 144)之间发生立体选择性空间冲突。这些冲突似乎解释了hCE1对氯氰菊酯类似物的反式和顺式异构体以及氰戊菊酯类似物的2R-和2S-异构体的立体偏好。讨论了这些发现对有效农药设计和使用的影响。

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本文引用的文献

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Development of optically pure pyrethroid-like fluorescent substrates for carboxylesterases.用于羧酸酯酶的光学纯拟除虫菊酯类荧光底物的开发。
Chem Res Toxicol. 2005 Mar;18(3):516-27. doi: 10.1021/tx049773h.
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Identification, expression, and purification of a pyrethroid-hydrolyzing carboxylesterase from mouse liver microsomes.从小鼠肝脏微粒体中鉴定、表达和纯化一种拟除虫菊酯水解羧酸酯酶。
J Biol Chem. 2004 Jul 9;279(28):29863-9. doi: 10.1074/jbc.M403673200. Epub 2004 Apr 30.
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