脑curin和噻西坦对产前慢性酒精中毒条件下内源性神经保护机制的热休克蛋白70 (HSP70)依赖的药理学调节

I. Belenichev, E. Sokolik, Nina V. Bukhtiarova, S. V. Levich
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引用次数: 2

摘要

目的:基因组对应激反应的主要反应之一是热休克蛋白(HSP)的不同生成诱导。本研究旨在研究慢性产前酒精中毒大鼠脑内不同缺血时期热休克蛋白(HSP70)和缺氧诱导因子(HIF-1)的浓度变化,并探讨这些蛋白在脑curin和Tiocetam的神经保护作用中的作用。方法:以体重150 ~ 180 g的雌性大鼠为实验对象。所有动物均饲喂标准日粮,昼夜自然变化。大鼠来自“乌克兰医学科学院药理学和毒理学研究所”托儿所。所有实验程序和手术干预均按照WMA关于生物医学研究中动物使用的声明进行。妊娠第5 ~ 20天大鼠给予6 ~ 8 g/kg/d乙醇,对照组大鼠给予等热量蔗糖溶液。酒精中毒大鼠仔鼠出生后第25天腹腔注射噻西坦(125 mg/kg)、吡拉西坦(125 mg/kg)和脑curin (0.06 mg/kg),对照组大鼠腹腔注射生理盐水。每组20例。实验第26天进行脑生化研究,为此在硫喷妥钠麻醉下(30 mg/kg,腹腔注射)斩首动物。Western blot检测脑组织中HIF蛋白和HSP蛋白的浓度。结果:脑组织HIF蛋白和HSP蛋白的浓度研究表明,产前慢性酒精中毒后,HSP浓度明显下降,HIF蛋白也随之下降。脑curin和噻西坦治疗期间,与未治疗组相比,脑内HIF和HSP蛋白含量显著升高。脑curin和噻西坦的神经保护作用可以减少神经功能障碍,这可以从McGrow量表的平均得分显著降低中得到证明。脑curin和Tiocetam可直接或间接调节急性脑缺血神经元早期反应c-fos基因的表达,从而“运行”软件适应蛋白合成(包括HSP和HIF)。结论:脑curin和噻西坦的神经保护作用表现出明显的提高脑组织热休克蛋白浓度的作用。
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Pharmacological modulation of Heat Shock Protein 70 (HSP70) - dependent mechanisms of endogenous neuroprotection in conditions of prenatal chronic alcoholism by Cerebrocurin and Tiocetam -
Objective: One of the primary reactions of the genome in response to stress is different genesis induction of heat shock proteins – HSP. The purpose of this study was to investigate the concentration of heat shock protein (HSP70) and hypoxia-inducible factor (HIF-1) in the brain of rats undergoing chronic prenatal alcoholism in different periods of ischemia and define the role of these proteins in the implementation of neuroprotective effect of Cerebrocurin and Tiocetam. Methods: Experiments were carried out on female rats weighing 150-180 g. All animals were on standard food ration of vivarium, with natural alteration of day and night. Rats were recieved from nursery of «Institute of Pharmacology and Toxicology, Academy of Medical Sciences of Ukraine». All experimental procedures and operative interventions were done in accordance with WMA Statement on Animal Use in Biomedical Research. Rats from the 5th to the 20th day of gestation received ethanol in a dose of 6-8 g/kg/day, control rats – isocalorific sucrose solution. Offspring of alcoholized rats immediately after birth during 25 days were injected intraperitoneally Tiocetam (125 mg/kg), Piracetam (125 mg/kg) and Cerebrocurin (0.06 mg/kg), control rats received saline solution. There were 20 infants in each group. Biochemical studies carried out on brain on 26 days of the experiment, for this purpose the animals were decapitated under anesthesia using Thiopental (30 mg/kg, intraperitoneally). Concentration in the brain tissue and HIF proteins and HSP proteins were determined by Western blot analysis. Results: Study of concentration in brain tissue HIF proteins and HSP-proteins showed that after undergoing prenatal chronic alcoholism there was an observed decrease in concentration of HSP, so HIF-proteins. Course treatment by Cerebrocurin and Tiocetam resulted in statistically significant increased content of HIF and HSP proteins in the brain in comparison with a group of untreated animals. Neuroprotective activity of Cerebrocurin and Tiocetam was observed in reduction of neurological deficit, as evidenced by the statistically significant decrease in the average score on a scale of C.P. McGrow. Cerebrocurin and Tiocetam directly or indirectly can modulate the expression of early response c-fos genes and thus the “run” software adaptation protein synthesis (including HSP and HIF) in neurons with acute cerebral ischemia. Conclusion: Implementation of the neuroprotective effect of Cerebrocurin and Tiocetam revealed apparently their ability to increase the concentration in the brain tissues of HSP-protein.
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