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开发一种用于 EPHX2 磷酸酶活性的高通量筛选 assay 并对非靶向文库进行筛选。

Development of an HTS assay for EPHX2 phosphatase activity and screening of nontargeted libraries.

机构信息

Department of Entomology and UCD Comprehensive Cancer Center, CA 95616, USA.

出版信息

Anal Biochem. 2013 Mar 1;434(1):105-11. doi: 10.1016/j.ab.2012.11.017. Epub 2012 Dec 3.

Abstract

The EPXH2 gene encodes soluble epoxide hydrolase (sEH), which has two distinct enzyme activities: epoxide hydrolase (Cterm-EH) and phosphatase (Nterm-phos). The Cterm-EH is involved in the metabolism of arachidonic acid epoxides that play important roles in blood pressure, cell growth, inflammation, and pain. While recent findings suggested complementary biological roles for Nterm-phos, research is limited by the lack of potent bioavailable inhibitors of this phosphatase activity. Also, a potent bioavailable inhibitor of this activity could be important in the development of therapy for cardiovascular diseases. We report herein the development of an HTS enzyme-based assay for Nterm-phos (Z'>0.9) using AttoPhos as the substrate. This assay was used to screen a wide variety of chemical entities, including a library of known drugs that have reached through clinical evaluation (Pharmakon 1600), as well as a library of pesticides and environmental toxins. We discovered that ebselen inhibits sEH phosphatase activity. Ebselen binds to the N-terminal domain of sEH (K(I)=550 nM) and chemically reacts with the enzyme to quickly and irreversibly inhibit Nterm-phos, and subsequently Cterm-EH, and thus represents a new class of sEH inhibitor.

摘要

EPXH2 基因编码可溶性环氧化物水解酶(sEH),它具有两种不同的酶活性:环氧化物水解酶(C 端-EH)和磷酸酶(N 端-phos)。C 端-EH 参与花生四烯酸环氧化物的代谢,这些物质在血压、细胞生长、炎症和疼痛中发挥重要作用。尽管最近的研究结果表明 N 端-phos 具有互补的生物学作用,但由于缺乏这种磷酸酶活性的有效生物可用抑制剂,研究受到限制。此外,这种活性的有效生物可用抑制剂在开发心血管疾病治疗方法方面可能很重要。我们在此报告了一种基于 HTS 的用于 N 端-phos(Z' > 0.9)的酶基测定法的开发,该测定法使用 AttoPhos 作为底物。该测定法用于筛选各种化学实体,包括已通过临床评估的已知药物文库(Pharmakon 1600)以及农药和环境毒素文库。我们发现埃斯硒啉抑制 sEH 磷酸酶活性。埃斯硒啉与 sEH 的 N 端结构域结合(K(I)=550 nM),并与酶发生化学反应,快速不可逆地抑制 N 端-phos,随后抑制 C 端-EH,因此代表了一类新的 sEH 抑制剂。

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