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首页> 外文期刊>Pharmacology, Biochemistry and Behavior >Neuroprotective effects of currently used antidotes in soman-poisoned rats.
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Neuroprotective effects of currently used antidotes in soman-poisoned rats.

机译:当前使用的解毒剂对人中毒大鼠的神经保护作用。

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The neuroprotective effects of antidotes (atropine, obidoxime, obidoxime/atropine mixture) on rats poisoned with soman at a sublethal dose (54 microg/kg, im, 80% of LD(50) value) were studied. The soman-induced neurotoxicity was monitored using a functional observational battery (FOB) and an automatic measurement of motor activity. The neurotoxicity of soman was monitored at 24 h and 7 days following soman challenge. The results indicate that obidoxime alone is not able to protect the rats from the lethal effects of soman. Three soman-poisoned rats treated with obidoxime alone died within 24 h. On the other hand, atropine alone or combined with obidoxime allows all soman-poisoned rats to survive within 7 days following soman challenge. Atropine alone and combined with obidoxime seems to be relatively effective antidotal treatment for the elimination of soman-induced neurotoxicity in the case of sublethal poisonings, although the antidotal mixture is significantly less effective than atropine alone because obidoxime can counteract the beneficial effects of atropine. Obidoxime appears to be practically ineffective to diminish soman-induced neurotoxicity. The neuroprotective effects of antidotal mixture consisting of atropine and obidoxime depend on the antimuscarinic effects of atropine only. Thus, the replacement of obidoxime by more effective acetylcholinesterase (AChE) reactivators is necessary to increase the neuroprotective efficacy of antidotal treatment in the case of soman poisonings.
机译:研究了解毒剂(阿托品,奥比多辛,奥比多肟/阿托品混合物)对亚致死剂量(54微克/千克,im,LD(50)值的80%)中毒的梭曼中毒大鼠的神经保护作用。使用功能性观察电池(FOB)和运动活动的自动测量来监测梭曼诱发的神经毒性。在梭曼攻击后24小时和7天监测梭曼的神经毒性。结果表明,仅obidoxime不能保护大鼠免受梭曼的致死作用。单独用obidoxime治疗的三只梭曼中毒大鼠在24小时内死亡。另一方面,单独使用阿托品或与奥比多肟组合使用的阿托品可使所有梭曼中毒的大鼠在梭曼攻击后7天内存活。在亚致死性中毒的情况下,单独使用阿托品和与obidoxime联合使用似乎是相对有效的解毒剂,以消除梭曼诱导的神经毒性,尽管解毒剂混合物比单独使用阿托品的效果明显差,因为obidoxime可以抵消阿托品的有益作用。奥比多肟似乎对减少梭曼诱导的神经毒性实际上无效。由阿托品和奥比多肟组成的解毒混合物的神经保护作用仅取决于阿托品的抗毒蕈碱作用。因此,在梭曼中毒的情况下,用更有效的乙酰胆碱酯酶(AChE)活化剂替代obidoxime对于提高解毒剂治疗的神经保护功效是必要的。

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