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首页> 外文期刊>Archives of Toxicology >Reactivation kinetics of a homologous series of bispyridinium bis-oximes with nerve agent-inhibited human acetylcholinesterase
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Reactivation kinetics of a homologous series of bispyridinium bis-oximes with nerve agent-inhibited human acetylcholinesterase

机译:具有神经毒剂抑制的人乙酰胆碱酯酶的双系列联吡啶双肟的复活动力学

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The reactivation of organophosphorus compound (OP)-inhibited acetylcholinesterase (AChE) by oximes is inadequate in case of different OP nerve agents. This fact led to the synthesis of numerous novel oximes by different research groups in order to identify more effective reactivators. In the present study, we investigated the reactivation kinetics of a homologous series of bispyridinium bis-oximes bearing a (E)-but-2-ene linker with tabun-, sarin-, and cyclosarin-inhibited human AChE. In part, marked differences in affinity and reactivity of the investigated oximes toward OP-inhibited human AChE were recorded. These properties depended on the position of the oxime groups and the inhibitor. None of the tested oximes was equally effective against all used OPs. In addition, the data indicate that a (E)-but-2-ene linker decreased in most cases the reactivating potency in comparison to oximes bearing an oxybismethylene linker, e.g., obidoxime and HI-6. The results of this study give further insight into structural requirements for oxime reactivators, underline the necessity to investigate the kinetic interactions of oximes and AChE with structurally different OP inhibitors, and point to the difficulty to develop an oxime reactivator which is efficient against a broad spectrum of OPs.
机译:在不同的OP神经毒剂的情况下,肟对有机磷化合物(OP)抑制的乙酰胆碱酯酶(AChE)的再激活作用不足。这一事实导致不同研究小组合成了许多新颖的肟,以便鉴定出更有效的活化剂。在本研究中,我们研究了带有(E)-丁-2-烯连接基与烟碱,沙林和环沙林抑制的人AChE的同系列双吡啶双肟的复活动力学。部分地,记录了所研究的肟对OP-抑制的人AChE的亲和力和反应性的显着差异。这些性质取决于肟基和抑制剂的位置。没有一种测试过的肟对所有使用过的OP具有同样的效果。另外,数据表明,与带有氧双亚甲基连接基的肟,例如,obidoxime和HI-6相比,(E)-丁-2-烯连接基在大多数情况下降低了活化能力。这项研究的结果使人们进一步了解了肟活化剂的结构要求,强调了研究肟和AChE与结构上不同的OP抑制剂的动力学相互作用的必要性,并指出了开发对广谱有效的肟活化剂的难度。的OP。

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