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环型和非环型葫芦脲对化学战剂 VX 降解途径的影响。

Influence of cyclic and acyclic cucurbiturils on the degradation pathways of the chemical warfare agent VX.

机构信息

Technische Universität Kaiserslautern, Fachbereich Chemie - Organische Chemie, Erwin-Schrödinger-Straße, 67663 Kaiserslautern, Germany.

Institut für Pharmakologie und Toxikologie der Bundeswehr, Neuherbergstraße 11, 80937 München, Germany.

出版信息

Org Biomol Chem. 2020 Jul 15;18(27):5218-5227. doi: 10.1039/d0ob01167c.

DOI:10.1039/d0ob01167c
PMID:32602497
Abstract

The highly toxic nerve agent VX is a methylphosphonothioate that degrades via three pathways in aqueous solution, namely through the hydrolysis of the P-O or P-S bonds, or the cleavage of the C-S bond at the 2-aminoethyl residue. In the latter case, an aziridinium ion and a phosphonothioate is formed. Here it is shown that acyclic or cyclic cucurbiturils inhibit these reactions in phosphate buffer at physiological pH and thus stabilise the nerve agent. When using unbuffered basic solutions as the reaction medium, however, in which the P-S or P-O bonds are normally hydrolysed preferentially, cucurbiturils turned out to strongly shift VX degradation towards the cleavage of the C-S bond. Cucurbit[7]uril, in particular, has a so pronounced effect under suitable conditions that it almost completely suppresses the formation of products resulting from the other degradation pathways. Investigations involving VX analogues in combination with computational methods suggest that one reason for the reaction control exerted by the cucurbiturils is the preorganisation of VX for aziridinium ion formation. In addition, cucurbit[7]uril also lowers the transition state of the reaction by stabilising the positive charge developing on the way to the product. Cucurbiturils thus have a marked effect on the reactivity of a highly toxic nerve agent, which potentially allows using them for decontamination purposes.

摘要

高度有毒的神经毒剂 VX 是一种甲基膦酸硫酯,在水溶液中通过三种途径降解,即通过 P-O 或 P-S 键的水解,或在 2-氨基乙基残基处的 C-S 键断裂。在后一种情况下,形成氮丙啶离子和硫代膦酸酯。这里表明,无环或环状的葫芦脲在生理 pH 的磷酸盐缓冲液中抑制这些反应,从而稳定神经毒剂。然而,当使用未缓冲的碱性溶液作为反应介质时,其中 P-S 或 P-O 键通常优先水解,葫芦脲会强烈促使 VX 降解朝向 C-S 键的断裂。特别是葫芦[7]脲在适当的条件下具有如此显著的效果,以至于它几乎完全抑制了来自其他降解途径的产物的形成。涉及 VX 类似物的与计算方法相结合的研究表明,葫芦脲对反应进行控制的原因之一是 VX 为氮丙啶离子形成进行预组织。此外,葫芦[7]脲还通过稳定在产物形成过程中产生的正电荷来降低反应的过渡态。因此,葫芦脲对高度有毒的神经毒剂的反应性有显著影响,这可能使其可用于净化目的。

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