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首页> 外文期刊>Basic & clinical pharmacology & toxicology. >Reactivation of human brain homogenate cholinesterases inhibited by Tabun using newly developed oximes K117 and K127.
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Reactivation of human brain homogenate cholinesterases inhibited by Tabun using newly developed oximes K117 and K127.

机译:使用新开发的肟K117和K127重新激活由Tabun抑制的人脑匀浆胆碱酯酶。

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摘要

Newly developed acetylcholinesterase reactivators K117 [1,5-bis(4-hydroxyiminomethylpyridinium)-3-oxapentane dichloride] and K127 [(1-(4-hydroxyiminomethylpyridinium)-5-(4-carbamoylpyridinium)-3-oxapentane dibromide)] were tested for their potency to reactivate tabun-inhibited human brain cholinesterases. Pralidoxime and trimedoxime were chosen as standard reference reactivators. Human tissue was used, as that was closer on the real treatment of human beings. As a result, oxime K127 was found as the best tested reactivator according to the constant k(r), characterizing the overall reactivation process. On the contrary, the maximal reactivation ability expressed as percentage of reactivation was the best for trimedoxime. This differences were caused as a result of using the enzyme from different species. Due to this, experiments on human tissue should be conducted after in vitro and in vivo tests on animals to eliminate such important failures of promising oximes.
机译:测试了新开发的乙酰胆碱酯酶活化剂K117 [1,5-双(4-羟基亚氨基甲基吡啶)-3-氧杂戊烷二氯化物]和K127 [(1-(4-羟基亚氨基甲基吡啶)-5-(4-氨基甲酰基吡啶)-3-氧杂戊烷二溴化物)]。因为它们有潜力重新激活禁忌抑制的人脑胆碱酯酶。选择普利肟和三甲肟作为标准参考活化剂。使用了人体组织,因为它更接近于人类的实际治疗。结果,根据常数k(r),发现肟K127是测试最好的再活化剂,表征了整个再活化过程。相反,表示为再活化百分比的最大再活化能力对于三甲肟是最好的。这种差异是由于使用不同物种的酶引起的。因此,应在对动物进行体外和体内试验后对人体组织进行实验,以消除有希望的肟的此类重要失效。

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