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首页> 外文期刊>Japanese Journal of Pharmacology >Effect of Minaprine and Other Reference Drugs on Passive Avoidance Impairment Induced by Cerebral Ischemia in Mongolian Gerbils
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Effect of Minaprine and Other Reference Drugs on Passive Avoidance Impairment Induced by Cerebral Ischemia in Mongolian Gerbils

机译:Minaprine和其他参考药物对蒙古沙鼠脑缺血所致被动回避障碍的影响

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摘要

References(12) Cited-By(8) We examined the characteristics of cerebral ischemia-induced behavioral deficit in the passive avoidance task and the effect of minaprine and other cytoprotective drugs on passive avoidance deficit induced by cerebral ischemia in Mongolian gerbils. Severe impairment of passive avoidance was apparent when the duration of the ischemia exceeded 2 min. Histopathological ischemic neuronal damage in CA1 neurons at 7 days after occlusion was also induced when the ischemia was over 2 min. Otherwise, although cerebral ischemia was carried out at 5 min, 2 hr, 5 hr or 24 hr after the training session, the passive avoidance deficit was produced 24 hr after the training session. When the training session was carried out 24 hr before the occlusion, minaprine, which was administered 30 min before the occlusion, led to a recovery of the response latency. Pentobarbital, diazepam and ethylapovincamine improved the passive avoidance deficit induced by 5-min bilateral carotid artery occlusion. On the other hand, the passive avoidance deficit was not ameliorated by Ca++-hopantenate, nicardipine and idebenone. The hippocampal damage at 7 days after occlusion was prevented by the drugs that ameliorated the passive avoidance deficit. The relationship between passive avoidance deficit and CA1 neuronal death in the hippocampus induced by cerebral ischemia warrants further attention.
机译:参考文献(12)Cited-By(8)研究了蒙古沙鼠被动回避任务中脑缺血引起的行为缺陷的特征,以及米那芬和其他细胞保护药物对脑缺血引起的被动回避缺陷的影响。当缺血持续时间超过2分钟时,就会明显出现被动回避的严重损害。当缺血超过2分钟时,在闭塞后第7天,也会诱发CA1神经元的组织病理学缺血性神经元损伤。否则,尽管在训练后的5分钟,2小时,5小时或24小时进行了脑缺血,但在训练后24小时仍会产生被动回避缺陷。当训练在闭塞前24小时进行时,米那芬在闭塞前30分钟给药,导致反应潜伏期恢复。戊巴比妥,地西epa和乙基apovincamine改善了5分钟的双侧颈动脉闭塞引起的被动回避缺陷。另一方面,戊二酸钙++,尼卡地平和艾地苯醌不能改善被动回避缺陷。缓解被动回避缺陷的药物可预防闭塞后7天的海马损伤。被动回避缺陷与脑缺血引起的海马CA1神经元死亡之间的关系值得进一步关注。

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