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乙酰胆碱酯酶复活剂和非复活剂解毒剂对梭曼所致骨骼肌损伤的减轻作用。

Attenuation of soman-induced lesions of skeletal muscle by acetylcholinesterase reactivating and non-reactivating antidotes.

作者信息

Dekleva A, Sket D, Sketelj J, Brzin M

机构信息

Institute of Anatomy, School of Medicine, Ljubljana, Yugoslavia.

出版信息

Acta Neuropathol. 1989;79(2):183-9. doi: 10.1007/BF00294377.

Abstract

It has been reported recently that some oximes reactivating acetylcholinesterase (AChE) exhibit concomitant ganglion-blocking effects which presumably could contribute independently to their powerful antidotal action in organophosphate inhibitor (OPI) poisoning, thus mimicking some unrelated substances which are effective antidotes without reactivating AChE. This raises the question whether OPI-induced muscle lesions, like some other symptoms could also be attenuated by oximes and other antidotes in the absence of AChE reactivation. To test this possibility, the oxime HI-6 was applied at increasing time intervals after the injection of soman until and beyond the point when soman-AChE complex becomes completely "aged" and not capable of reactivation. As the examples of OPI antidotes which do not reactivate AChE, the muscarinic antagonist atropine and the ganglion-blocking agent hexamethonium were also tested on possible attenuation of muscle lesions. The proportions of fibers with lesions, AChE inhibition and muscle fasciculations in experimental groups relative to the controls treated with soman only were evaluated. The results show that HI-6 can attenuate lesions only if AChE is partially reactivated and muscle fasciculations are permanently eliminated. However, atropine does not affect either AChE inhibition or muscle fasciculations and is also ineffective in counteracting the lesions in spite of its potency as an effective general antidote. Hexamethonium also does not affect AChE inhibition, but abolishes fasciculations and effectively attenuates muscle lesions. The latter findings reveal the existence of lesion-protecting mechanisms unrelated to AChE reactivation, which if further elucidated might become potentially relevant for additional treatment in OPI poisoning.

摘要

最近有报道称,一些能使乙酰胆碱酯酶(AChE)重新活化的肟类药物具有伴随的神经节阻断作用,据推测,这可能独立地促成了它们在有机磷酸酯抑制剂(OPI)中毒时强大的解毒作用,从而类似于一些不相关的物质,这些物质是有效的解毒剂,但不会使AChE重新活化。这就提出了一个问题,即OPI引起的肌肉损伤,是否像其他一些症状一样,在没有AChE重新活化的情况下也能被肟类药物和其他解毒剂减轻。为了检验这种可能性,在注射梭曼后,以越来越长的时间间隔应用肟类药物HI-6,直到梭曼-AChE复合物完全“老化”且无法重新活化之后。作为不使AChE重新活化的OPI解毒剂的例子,还测试了毒蕈碱拮抗剂阿托品和神经节阻断剂六甲铵对肌肉损伤可能的减轻作用。评估了实验组中出现损伤的纤维比例、AChE抑制情况和肌肉束颤相对于仅用梭曼处理的对照组的情况。结果表明,只有当AChE部分重新活化且肌肉束颤被永久消除时,HI-6才能减轻损伤。然而,阿托品既不影响AChE抑制,也不影响肌肉束颤,尽管它作为一种有效的通用解毒剂有一定效力,但在对抗损伤方面也无效。六甲铵也不影响AChE抑制,但能消除束颤并有效减轻肌肉损伤。后一发现揭示了存在与AChE重新活化无关的损伤保护机制,如果进一步阐明,这可能对OPI中毒的额外治疗具有潜在意义。

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