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Irreversible inhibition of the thermophilic esterase EST2 from Alicyclobacillus acidocaldarius

机译:酸热脂环酸杆菌对嗜热酯酶EST2的不可逆抑制

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Kinetic studies of irreversible inhibition in recent years have received growing attention owing to their relevance to problems of basic scientific interest as well as to their practical importance. Our studies have been devoted to the characterization of the effects that well-known acetylcholinesterase irreversible inhibitors exert on a carboxylesterase (EST2) from the thermophilic eubacterium Alicyclobacillus acidocaldarius. In particular, sulfonyl inhibitors and the organophosphorous insecticide diethyl-p-nitrophenyl phosphate (paraoxon) have been studied. The incubation of EST2 with sulfonyl inhibitors resulted in a time-dependent inactivation according to a pseudo-first-order kinetics. On the other hand, the EST2 inactivation process elicited by paraoxon, being the inhibition reaction completed immediately after the inhibitor addition, cannot be described as a pseudo-first-order kinetics but is better considered as a high affinity inhibition. The values of apparent rate constants for paraoxon inactivation were determined by monitoring the enzyme/substrate reaction in the presence of the inhibitor, and were compared with those of the sulfonyl inhibitors. The protective effect afforded by a competitive inhibitor on the EST2 irreversible inhibition, and the reactivation of a complex enzyme/irreversible-inhibitor by hydroxylamine and 2-PAM, were also investigated. The data have been discussed in the light of the recently described dual substrate binding mode of EST2, considering that the irreversible inhibitors employed were able to discriminate between the two different binding sites.
机译:近年来,由于不可逆抑制的动力学研究与基础科学问题相关,并且具有实际意义,因此受到越来越多的关注。我们的研究致力于表征知名的乙酰胆碱酯酶不可逆抑制剂对嗜热真细菌嗜酸拟酸杆菌的一种酶(EST2)的作用。特别地,已经研究了磺酰基抑制剂和有机磷杀虫剂二乙基-对-硝基苯基磷酸酯(对氧磷)。 EST2与磺酰基抑制剂的孵育导致时间依赖性的失活根据伪一级动力学。另一方面,由对氧磷引发的EST2失活过程,即添加抑制剂后立即完成的抑制反应,不能被描述为拟一级动力学,而是更好地被认为是高亲和力抑制作用。通过监测在抑制剂存在下的酶/底物反应来确定对氧磷灭活的表观速率常数,并将其与磺酰基抑制剂进行比较。还研究了竞争性抑制剂对EST2不可逆抑制的保护作用,以及羟胺和2-PAM对复合酶/不可逆抑制剂的再激活。考虑到所使用的不可逆抑制剂能够区分两个不同的结合位点,已经根据最近描述的EST2的双重底物结合模式讨论了该数据。

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