Effect of Soluble Epoxide Hydrolase Polymorphism on Substrate and Inhibitor Selectivity and Dimer Formation

Overview

Journal J Lipid Res

Publisher Elsevier

Specialty Biochemistry

Date 2014 Apr 29

PMID 24771868

Citations 32

Authors

Christophe Morisseau

Aaron T Wecksler

Catherine Deng

Hua Dong

Jun Yang

Kin Sing S Lee

Sean D Kodani

Bruce D Hammock

Affiliations

Soon will be listed here.

Abstract

Epoxy FAs (EpFAs) are important lipid mediators that are mainly metabolized by soluble epoxide hydrolase (sEH). Thus, sEH inhibition is a promising therapeutic target to treat numerous ailments. Several sEH polymorphisms result in amino acid substitutions and alter enzyme activity. K55R and R287Q are associated with inflammatory, cardiovascular, and metabolic diseases. R287Q seems to affect sEH activity through reducing formation of a catalytically active dimer. Thus, understanding how these SNPs affect the selectivity of sEH for substrates and inhibitors is of potential clinical importance. We investigated the selectivity of four sEH SNPs toward a series of EpFAs and inhibitors. We found that the SNPs alter the catalytic activity of the enzyme but do not alter the relative substrate and inhibitor selectivity. We also determined their dimer/monomer constants (KD/M). The WT sEH formed a very tight dimer, with a KD/M in the low picomolar range. Only R287Q resulted in a large change of the KD/M However, human tissue concentrations of sEH suggest that it is always in its dimer form independently of the SNP. These results suggest that the different biologies associated with K55R and R287Q are not explained by alteration in dimer formation or substrate selectivity.

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