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45分钟后用药物终止大鼠体内梭曼诱发的惊厥:神经病理学与认知表现

Soman-induced convulsions in rats terminated with pharmacological agents after 45 min: neuropathology and cognitive performance.

作者信息

Myhrer Trond, Andersen Jannike M, Nguyen Nga H T, Aas Pål

机构信息

Norwegian Defence Research Establishment, Protection Division, NO-2027 Kjeller, Norway.

出版信息

Neurotoxicology. 2005 Jan;26(1):39-48. doi: 10.1016/j.neuro.2004.07.011.

Abstract

It has been demonstrated that a triple regimen consisting of procyclidine (6 mg/kg), diazepam (10 mg/kg) and pentobarbital (30 mg/kg) can effectively terminate soman-induced (1 x LD50) seizures/convulsions in rats when administered 30-40 min following onset. However, convulsive activity lasting for only 45 min can result in marked neuronal pathology. The purpose of the present study was to examine potential cognitive impairments of such brain lesions. The results showed that the neuronal pathology (assessed with Fluoro-Jade B) varied from none at all to 30% damage in the index areas (hippocampus, amygdala, piriform cortex). Cognitive deficits were seen in a novelty test (11 days post-exposure) and retention of a brightness discrimination task (28 days post-exposure) among the rats with neuropathology. Furthermore, significant correlations between neuropathology scores and behavioral measures were found for the animals that convulsed. Among these rats, the mortality rate was relatively high (60%) compared with rats in a previous study that had undergone implantation of hippocampal electrodes (17%). Neither the soman poisoning in the absence of convulsions nor the triple regimen alone affected behavior. It is concluded that early management of soman-induced convulsions is of major importance in preventing neuropathology and accompanying cognitive impairments.

摘要

已经证明,由丙环定(6毫克/千克)、地西泮(10毫克/千克)和戊巴比妥(30毫克/千克)组成的三联疗法在中毒发作后30 - 40分钟给药时,可有效终止大鼠体内梭曼诱导(1倍半数致死剂量)的癫痫发作/惊厥。然而,仅持续45分钟的惊厥活动可导致明显的神经元病变。本研究的目的是检查此类脑损伤潜在的认知障碍。结果表明,神经元病变(用荧光玉B评估)在指标区域(海马体、杏仁核、梨状皮质)从无到30%的损伤不等。在具有神经病理学改变的大鼠中,在新奇性测试(暴露后11天)和亮度辨别任务的记忆保持(暴露后28天)中观察到认知缺陷。此外,在发生惊厥的动物中,发现神经病理学评分与行为指标之间存在显著相关性。在这些大鼠中,死亡率相对较高(60%),而在先前一项进行海马电极植入的研究中的大鼠死亡率为17%。未发生惊厥的梭曼中毒以及单独的三联疗法均未影响行为。结论是,早期处理梭曼诱导的惊厥对于预防神经病理学改变及伴随的认知障碍至关重要。

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