首页> 美国卫生研究院文献>other >Mass spectrometry identifies covalent binding of soman sarin chlorpyrifos oxon diisopropyl fluorophosphate and FP-biotin to tyrosines on tubulin: a potential mechanism of long term toxicity by organophosphorus agents
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Mass spectrometry identifies covalent binding of soman sarin chlorpyrifos oxon diisopropyl fluorophosphate and FP-biotin to tyrosines on tubulin: a potential mechanism of long term toxicity by organophosphorus agents

机译:质谱鉴定了梭曼沙林毒死氟代磷酸二异丙酯和FP-生物素与微管蛋白上的酪氨酸的共价结合:有机磷试剂长期毒性的潜在机制

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摘要

Chronic low dose exposure to organophosphorus poisons (OP) results in cognitive impairment. Studies in rats have shown that OP interfere with microtubule polymerization. Since microtubules are required for transport of nutrients from the nerve cell body to the nerve synapse, it has been suggested that disruption of microtubule function could explain the learning and memory deficits associated with OP exposure. Tubulin is a major constituent of microtubules. We tested the hypothesis that OP bind to tubulin by treating purified bovine tubulin with sarin, soman, chlorpyrifos oxon, diisopropylfluorophosphate, and 10-fluoroethoxyphosphinyl-N-biotinamidopentyldecanamide (FP-biotin). Tryptic peptides were isolated and analyzed by mass spectrometry. It was found that OP bound to tyrosine 83 of alpha tubulin in peptide TGTYR, tyrosine 59 in beta tubulin peptide YVPR, tyrosine 281 in beta tubulin peptide GSQQYR, and tyrosine 159 in beta tubulin peptide EEYPDR. The OP reactive tyrosines are located either near the GTP binding site or within loops that interact laterally with protofilaments. It is concluded that OP bind covalently to tubulin, and that this binding could explain cognitive impairment associated with OP exposure.
机译:长期低剂量接触有机磷中毒(OP)会导致认知障碍。在大鼠中的研究表明,OP干扰微管聚合。由于需要微管将营养物从神经细胞体转运到神经突触,因此建议微管功能的破坏可以解释与OP暴露相关的学习和记忆缺陷。微管蛋白是微管的主要成分。我们通过用沙林蛋白,梭曼蛋白,毒死oxon,二异丙基氟磷酸盐和10-氟乙氧基次膦酰基-N-biotinamidopentyldecanamide(FP-生物素)处理纯化的牛微管蛋白来检验OP与微管蛋白结合的假设。分离胰蛋白酶肽并通过质谱分析。发现OP与肽TGTYR中的α微管蛋白的酪氨酸83,β微管蛋白肽YVPR中的酪氨酸59,β微管蛋白肽GSQQYR中的酪氨酸281和β微管蛋白肽EEYPDR中的酪氨酸159结合。 OP反应性酪氨酸位于GTP结合位点附近或与原丝横向相互作用的环内。结论是OP与微管蛋白共价结合,并且这种结合可以解释与OP暴露相关的认知障碍。

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