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在大鼠心肺骤停模型中,尼莫地平对神经功能结局无有益影响。

Nimodipine has no beneficial effect on neurological outcome in a cardiopulmonary arrest model in the rat.

作者信息

Calle P A, Bogaert M G, De Ridder L, Buylaert W A

机构信息

Heymans Institute of Pharmacology, Gent, Belgium.

出版信息

Naunyn Schmiedebergs Arch Pharmacol. 1990 Jun;341(6):586-91. doi: 10.1007/BF00171740.

Abstract

Brain damage after resuscitation from cardiac arrest is believed to be related to calcium influx in ischaemic neurons and to postischaemic calcium-dependent vasospasm. We therefore evaluated the potentially protective effects of the calcium-entry blocker nimodipine in a cardiopulmonary arrest model in the rat. Male Wistar rats were anaesthetized with ketamine (group I) or hexobarbital (group II) and subjected to a KCl-induced cardiac arrest during 7 min (group I) or 12 min (group II). Five minutes after resuscitation, the rats were treated intravenously in a randomized and blind fashion. Group I received either saline or 1 microgram.kg-1.min-1 or 5 micrograms.kg-1.min-1 of nimodipine and group II either saline or 1 microgram.kg-1.min-1 of nimodipine. Survival, occurrence of seizures and neurological status were assessed daily during 7 days after resuscitation. On day 7, the brains of the surviving rats were perfusion-fixed and a histopathological evaluation of the hippocampus was performed. Nimodipine, in the doses tested, had no beneficial influence on the 7 day survival rate, nor on the occurrence of seizures and the neurological and histopathological scores in the rats surviving after 7 days. With the highest dose of nimodipine, there was even a trend towards a decrease of the survival rate, probably related to the drug's hypotensive effect. Therefore, our data do not show a protective effect of nimodipine after cardiac arrest.

摘要

心脏骤停复苏后的脑损伤被认为与缺血神经元中的钙内流以及缺血后钙依赖性血管痉挛有关。因此,我们在大鼠心肺骤停模型中评估了钙通道阻滞剂尼莫地平的潜在保护作用。雄性Wistar大鼠用氯胺酮(I组)或己巴比妥(II组)麻醉,并在7分钟(I组)或12分钟(II组)内经历氯化钾诱导的心脏骤停。复苏后5分钟,大鼠以随机和盲法进行静脉治疗。I组接受生理盐水或1微克·千克-1·分钟-1或5微克·千克-1·分钟-1的尼莫地平,II组接受生理盐水或1微克·千克-1·分钟-1的尼莫地平。在复苏后的7天内每天评估存活率(生存情况)、癫痫发作的发生情况和神经状态。在第7天,对存活大鼠的大脑进行灌注固定,并对海马体进行组织病理学评估。在所测试的剂量下,尼莫地平对7天存活率、癫痫发作的发生情况以及7天后存活大鼠的神经和组织病理学评分均无有益影响。使用最高剂量的尼莫地平时,甚至有存活率下降的趋势,这可能与该药物的降压作用有关。因此,我们的数据未显示尼莫地平在心脏骤停后具有保护作用。

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