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犬全脑缺血后给予尼莫地平的脑血流量和神经学转归

Cerebral blood flow and neurologic outcome when nimodipine is given after complete cerebral ischemia in the dog.

作者信息

Steen P A, Newberg L A, Milde J H, Michenfelder J D

出版信息

J Cereb Blood Flow Metab. 1984 Mar;4(1):82-7. doi: 10.1038/jcbfm.1984.10.

Abstract

Ten minutes of complete cerebral ischemia was produced in 26 dogs by temporary ligation of the aorta and the venae cavae. Twenty dogs received nimodipine, a calcium entry blocker, 10 micrograms kg-1 i.v. 2 min after the ischemic period, followed by 1 microgram kg-1 min-1 for 2-3 h. Six dogs received only the solvent used for nimodipine. Fourteen dogs received nimodipine for 3 h and were subsequently evaluated neurologically up to 48 h postischemia. In the 12 other dogs, CBF and metabolism were followed for 2 h postischemia while either nimodipine or the solvent only was infused. The results were compared to previously published results for untreated dogs and dogs given nimodipine before the ischemic event. Nimodipine had the same effect on postischemic CBF whether started before or after the ischemic event, nearly doubling the flow when compared with untreated controls, whereas the solvent alone caused only a slight increase in CBF over control. By contrast, nimodipine initiated in the preischemic period significantly improved the neurologic outcome, but when initiated in the postischemic period the results were equivocal, such that the outcome was not significantly different from either the untreated group or the group in which nimodipine was initiated preischemia. Metabolic measurements did not give any indication of a specific effect of nimodipine, nor could the metabolic results be used as an indicator of neurologic outcome. The results are consistent with a beneficial effect of nimodipine following complete cerebral ischemia; however, evaluation of neurologic functional effects will require a more sensitive model.

摘要

通过暂时结扎主动脉和腔静脉,在26只犬中造成10分钟的完全性脑缺血。20只犬在缺血期后2分钟静脉注射10微克/千克的钙通道阻滞剂尼莫地平,随后以1微克/千克·分钟的速度持续注射2 - 3小时。6只犬仅接受用于溶解尼莫地平的溶剂。14只犬接受尼莫地平治疗3小时,随后在缺血后48小时内进行神经学评估。在另外12只犬中,缺血后2小时持续输注尼莫地平或仅输注溶剂,同时监测脑血流量(CBF)和代谢情况。将结果与先前发表的未治疗犬以及在缺血事件前给予尼莫地平的犬的结果进行比较。无论在缺血事件之前还是之后开始使用,尼莫地平对缺血后脑血流量的影响相同,与未治疗的对照组相比,血流量几乎增加了一倍,而单独使用溶剂时,脑血流量仅比对照组略有增加。相比之下,在缺血前期开始使用尼莫地平可显著改善神经学结果,但在缺血后期开始使用时,结果不明确,其结果与未治疗组或在缺血前开始使用尼莫地平的组相比无显著差异。代谢测量未显示尼莫地平有任何特异性作用,代谢结果也不能用作神经学结果的指标。这些结果与尼莫地平在完全性脑缺血后具有有益作用一致;然而,对神经功能影响的评估需要更敏感的模型。

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