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人类可溶性环氧化物水解酶的多态性:对酶活性、酶稳定性和四级结构的影响。

Polymorphisms in human soluble epoxide hydrolase: effects on enzyme activity, enzyme stability, and quaternary structure.

作者信息

Srivastava Punit K, Sharma Vikas K, Kalonia Davendra S, Grant David F

机构信息

Department of Pharmaceutical Sciences, University of Connecticut, Storrs, CT 06269, USA.

出版信息

Arch Biochem Biophys. 2004 Jul 15;427(2):164-9. doi: 10.1016/j.abb.2004.05.003.

Abstract

Human soluble epoxide hydrolase (hsEH) has been shown to play a role in regulating blood pressure and inflammation. HsEH consists of an N-terminal phosphatase and a C-terminal epoxide hydrolase domain. In the present study, we examined the effects of polymorphisms in the hsEH gene on phosphatase activity, enzyme stability, and protein quaternary structure. The results showed that mutants Lys55Arg, Arg103Cys, Cys154Tyr, Arg287Gln, and the Arg103Cys/Arg287Gln (double mutant) have significantly lower phosphatase activity compared to the most frequent allele (MFA) of hsEH. In addition, the Lys55Arg, Arg103Cys, Cys154Tyr, Arg287Gln, and the double mutant have significantly lower kcat/Km values. The stabilities at 37 degrees C of purified Arg287Gln and Arg103Cys/Arg287Gln mutants were also significantly reduced compared to the MFA. HPLC size-exclusion studies showed that the MFA exists predominantly as a dimer. However, the Arg287Gln and Arg103Cys/Arg287Gln mutants show increased concentration of the monomer. We conclude that the Arg287Gln polymorphism disrupts putative intra- and inter-monomeric salt-bridges responsible for dimerization.

摘要

人可溶性环氧化物水解酶(hsEH)已被证明在调节血压和炎症中发挥作用。HsEH由一个N端磷酸酶和一个C端环氧化物水解酶结构域组成。在本研究中,我们研究了hsEH基因多态性对磷酸酶活性、酶稳定性和蛋白质四级结构的影响。结果表明,与hsEH最常见等位基因(MFA)相比,突变体Lys55Arg、Arg103Cys、Cys154Tyr、Arg287Gln以及Arg103Cys/Arg287Gln(双突变体)的磷酸酶活性显著降低。此外,Lys55Arg、Arg103Cys、Cys154Tyr、Arg287Gln以及双突变体的kcat/Km值显著降低。与MFA相比,纯化的Arg287Gln和Arg103Cys/Arg287Gln突变体在37摄氏度时的稳定性也显著降低。高效液相色谱尺寸排阻研究表明,MFA主要以二聚体形式存在。然而,Arg287Gln和Arg103Cys/Arg287Gln突变体的单体浓度增加。我们得出结论,Arg287Gln多态性破坏了负责二聚化的假定的单体内部和单体间盐桥。

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