首页> 美国卫生研究院文献>Proceedings of the National Academy of Sciences of the United States of America >Rapid purification of cytosolic epoxide hydrolase from normal and clofibrate-treated animals by affinity chromatography.
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Rapid purification of cytosolic epoxide hydrolase from normal and clofibrate-treated animals by affinity chromatography.

机译:通过亲和色谱法从正常和经氯贝特治疗的动物中快速纯化胞质环氧酶水解酶。

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摘要

Epoxide hydrolase from liver cytosol (cEH) of both normal and clofibrate-treated mice can be bioselectively adsorbed onto an affinity column prepared from epoxy-activated Sepharose and 7-methoxycitronellyl thiol. The free ligand is a modest inhibitor of cEH (I50, approximately equal to 3 X 10(-4) M) and lacks the epoxide function necessary for it to be turned over as a substrate. This study demonstrates that a methoxy group can be used to mimic an oxirane in a vertebrate system. Bioselective elution of cEH can be accomplished with several chalcone oxides, which are selective potent inhibitors (I50, 1-50 X 10(-7) M), and activity can be recovered by dialysis. This procedure thus enhances the purification by offering independent opportunities for selective binding and selective elution. Conservatively, a 40%-80% recovery of partially inhibited enzyme activity can be achieved in 4-48 hr with a 30- to 90-fold purification. The purified cEH from clofibrate-induced animals was essentially homogeneous by NaDodSO4/PAGE and had an apparent subunit molecular weight of 58,000. The cEHs from normal and clofibrate-induced animals appeared identical by NaDodSO4/PAGE. Since the cEH activity in normal and clofibrate-treated animals is due to the same enzyme, the increase in cEH activity caused by selected hypolipidemic agents appears to be true induction.
机译:正常和经氯贝特治疗的小鼠的肝细胞溶质(cEH)的环氧水解酶都可以被生物选择性地吸附到由环氧活化的琼脂糖和7-甲氧基香茅醇硫醇制备的亲和柱上。游离配体是cEH的适度抑制剂(I50,大约等于3 X 10(-4)M),并且缺乏将其翻转为底物所需的环氧功能。这项研究表明,甲氧基可用于模拟脊椎动物系统中的环氧乙烷。 cEH的生物选择性洗脱可通过几种查尔酮氧化物完成,这些查尔酮氧化物是选择性强效抑制剂(I50、1-50 X 10(-7)M),并且可以通过透析恢复活性。因此,该程序通过提供选择性结合和选择性洗脱的独立机会来增强纯化。保守地,在30至90倍的纯化过程中,可以在4-48小时内实现部分抑制的酶活性40%-80%的回收率。通过NaDodSO4 / PAGE从氯贝特诱导的动物中纯化的cEH基本上是均质的,表观亚基分子量为58,000。通过NaDodSO4 / PAGE,来自正常动物和氯贝贝特诱导的动物的cEHs看起来相同。由于正常动物和经氯贝特治疗的动物体内的cEH活性是由于相同的酶引起的,因此由选定的降血脂药引起的cEH活性增加似乎是真正的诱导作用。

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