首页> 外文期刊>Brain research >Neuroprotection with felbamate: a 7- and 28-day study in transient forebrain ischemia in gerbils.
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Neuroprotection with felbamate: a 7- and 28-day study in transient forebrain ischemia in gerbils.

机译:氟苯甲酸酯的神经保护作用:一项为期7天和28天的沙土鼠短暂性前脑缺血研究。

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摘要

The use of glutamate antagonists and GABA agonists may protect neurons from the effects of transient ischemia. Felbamate is a new antiepileptic drug with glutamate antagonist and GABA agonist properties. We tested the efficacy of felbamate in a gerbil model of transient forebrain ischemia. Damage assessment was done with silver staining at 7 and 28 days after 5 min of bilateral carotid occlusion. Cerebral cortex, hippocampus (CA1 and CA4), thalamus and striatum were evaluated on a 4-point scoring system. The animals sacrificed at 28 days were also tested in a water-maze task to assess recovery of function. The initial dose of felbamate (300 mg/kg) was given 30 min before the ischemic insult in one set of animals and 30 min after the insult in another set of animals. There were 8 animals tested per group (total: 48 animals). There was significant neuronal protection with the use of felbamate, both before and after ischemia in all regions of the brain. Protection was seen in animals sacrificed at 7 and 28 days. Protection was moderate when felbamate was used before ischemia. It was highly significant when felbamate was given 30 min after the insult. Behavioral studies however did not show any difference in the felbamate treated animals versus the saline treated controls. The structural protection with felbamate was very significant when used in the post-ischemic period. This window for protection merits further evaluation in relation to the clinical setting of stroke.
机译:谷氨酸拮抗剂和GABA激动剂的使用可以保护神经元免受短暂性脑缺血的影响。 Felbamate是一种具有谷氨酸拮抗剂和GABA激动剂特性的新型抗癫痫药。我们在短暂的前脑缺血的沙鼠模型中测试了非尔贝特的疗效。在双侧颈动脉闭塞5分钟后的第7和28天用银染进行损伤评估。在4分制评分系统中评估大脑皮层,海马(CA1和CA4),丘脑和纹状体。还在水迷宫任务中测试了在第28天处死的动物,以评估其功能恢复。一组动物在缺血性伤害发生前30分钟给予氟苯甲酸酯的初始剂量(300 mg / kg),另一组动物则在伤害发生后30分钟给予氟苯甲酸酯的初始剂量。每组测试8只动物(总共48只动物)。在大脑的所有区域缺血之前和之后,使用非氨酯对神经元都有明显的保护作用。在第7和28天处死的动物中看到保护。当在缺血前使用非贝氨酸盐时,保护作用中等。侮辱30分钟后给予非贝氨酯非常重要。然而,行为研究未显示在用非贝马特治疗的动物与用盐水治疗的对照中有任何差异。在局部缺血后阶段使用非贝氨酸盐的结构保护作用非常重要。该保护窗值得进一步评估中风的临床背景。

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