Polymorphisms in Human Soluble Epoxide Hydrolase

环氧化物水解酶2 突变体 生物 生物化学 微粒体环氧化物水解酶 人口 氨基酸 互补DNA 基因 环氧化物水解酶 分子生物学 遗传学 微粒体 社会学 人口学
作者
Beata Przybyla‐Zawislak,Punit Srivastava,Johana Vázquez‐Matías,Harvey W. Mohrenweiser,Joseph E. Maxwell,Bruce D. Hammock,J. Alyce Bradbury,Ahmed Enayetallah,Darryl C. Zeldin,David F. Grant
出处
期刊:Molecular Pharmacology [American Society for Pharmacology and Experimental Therapeutics]
卷期号:64 (2): 482-490 被引量:159
标识
DOI:10.1124/mol.64.2.482
摘要

Human soluble epoxide hydrolase (hsEH) metabolizes a variety of epoxides to the corresponding vicinal diols. Arachidonic and linoleic acid epoxides are thought to be endogenous substrates for hsEH. Enzyme activity in humans shows high interindividual variation (e.g., 500-fold in liver) suggesting the existence of regulatory and/or structural gene polymorphisms. We resequenced each of the 19 exons of the hsEH gene (EPHX2) from 72 persons representing black, Asian, and white populations. A variety of polymorphisms was found, six of which result in amino acid substitutions. Amino acid variants were localized on the crystal structure of the mouse sEH, resulting in the prediction that at least two of these (Arg287Gln and Arg103Cys) might significantly affect enzyme function. The six variants of the hsEH cDNA corresponding to each single polymorphism and one corresponding to a double polymorphism were then constructed by site-directed mutagenesis and expressed in insect cells. As predicted, Arg287Gln and the double mutant Arg287Gln/Arg103Cys showed decreased enzyme activity using trans-stilbene oxide, trans-diphenylpropene oxide, and 14,15-epoxyeicosatrienoic acid as substrates. Lys55Arg and Cys154Tyr mutants had elevated activity for all three substrates. Detailed kinetic studies revealed that the double mutant Arg287Gln/Arg103Cys showed significant differences in Km and Vmax. In addition, stability studies showed that the double mutant was less stable than wild-type protein when incubated at 37°C. These results suggest that at least six hsEH variants exist in the human population and that at least four of these may influence hsEH-mediated metabolism of exogenous and endogenous epoxide substrates in vivo.
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