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萝巴新与烯丙哌三嗪联合治疗脑缺血的实验方法

Experimental approach of treatment of cerebral ischemia by a combination of raubasine and almitrine.

作者信息

Borzeix M G, Cahn J

出版信息

Arzneimittelforschung. 1987 May;37(5):491-4.

PMID:2887170
Abstract

Post-oligemic syndrome in rat results from transient reduction of cerebral blood flow obtained by bilateral carotid ligation for 60 min and mild systemic hypotension induced by s.c. injection of sodium nitroprusside. Over an acute phase of 3 days the syndrome consisted in a marked neurological deficit evidenced by a decrease in scores obtained by rats in "visual placing" test, a loss in learning ability substantiated by a decrease in the ability of rats to integrate and remember a passive avoidance reflex; biochemical disorders revealed by an increase in cerebral water, calcium and free fatty acids (FFA) contents associated with a decrease in cerebral potassium content. From 2 weeks until 4 weeks after ischemic insult a process of malacia of the cerebral tissue occurred. Treatment of rats with a combination of raubasine and almitrine (5023 SE, Duxil) by oral route (16.7 to 66.6 mg kg-1) twice daily from 1 h post-oligemia to sacrifice, in the acute phase, led to 1. an improvement of visual placing response, 2. an increase in learning ability, 3. a decrease in water and calcium cerebral contents associated with an increase in potassium cerebral contents. Enhancement of FFA contents was reduced when preventive treatment was associated with curative treatment. Incidence and extent of encephalomalacia was reduced by the drug in the chronic phase. It is concluded that in a rat model of post-oligemic syndrome and under these experimental conditions 5023 SE caused, 3 days after the ischemic insult, a significant reduction of cerebral disorders that may explain the therapeutic effect of the drug evidenced 4 weeks later.

摘要

大鼠的低灌注后综合征是由双侧颈动脉结扎60分钟导致的脑血流量短暂减少以及皮下注射硝普钠引起的轻度全身性低血压所致。在3天的急性期内,该综合征表现为明显的神经功能缺损,表现为大鼠在“视觉定位”测试中的得分降低;学习能力丧失,表现为大鼠整合和记忆被动回避反射的能力下降;生化紊乱表现为脑水、钙和游离脂肪酸(FFA)含量增加,同时脑钾含量降低。缺血性损伤后2周至4周,脑组织发生软化过程。在急性期,从低灌注后1小时至处死,每天两次经口给大鼠联合使用萝巴新和阿米三嗪(5023 SE,都可喜)(16.7至66.6毫克/千克),导致:1. 视觉定位反应改善;2. 学习能力增强;3. 脑水和钙含量降低,同时脑钾含量增加。预防性治疗与治疗性治疗联合使用时,FFA含量的增加减少。在慢性期,该药物降低了脑软化的发生率和程度。得出的结论是,在低灌注后综合征的大鼠模型中,在这些实验条件下,5023 SE在缺血性损伤3天后导致脑功能障碍显著减轻,这可能解释了4周后该药物所证实的治疗效果。

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