替扎尼定是预防大鼠局灶性脑缺血的有效药物：一项实验研究。

Tizanidine is an effective agent in the prevention of focal cerebral ischemia in rats: an experimental study.

作者信息

Berkman M Z, Zirh T A, Berkman K, Pamir M N

机构信息

Department of Neurosurgery, SSK Okmeydani Hospital, Istanbul, Turkey.

出版信息

Surg Neurol. 1998 Sep;50(3):264-70; discussion 270-1. doi: 10.1016/s0090-3019(97)00500-4.

DOI:10.1016/s0090-3019(97)00500-4

PMID:9736090

Abstract

BACKGROUND

Focal cerebral ischemia secondary to cerebral vessel occlusion is still an important cause of mortality and morbidity. Excitatory neurotransmitters are gathered in the extracellular space during ischemia and initiate or stimulate a series of pathophysiological biochemical processes and consequently lead to neuronal death. Tizanidine (Sandoz compound DS 103-282, 5-chloro4,2 (2-imidazolin-2-yl-amino)-2,1,3-benzothiazol hydrochloride) is a selective alpha 2 adrenoreceptor agonist which shows its effect by stimulating presynaptic alpha 2 adrenoreceptors in central ASPergic and GLUergic system by inhibiting aspartic acid and glutamic acid release. In this study, the effect of Tizanidine on reversible focal cerebral ischemia was evaluated.

METHODS

Cerebral blood flow to the left hemisphere of adult Sprague-Dawley rats (n=48) was temporarily interrupted by middle cerebral artery and bilateral common carotid artery occlusion for 3 hours in eight rats of each group. Tizanidine was given to each group of rats intraperitoneally before the ischemic insult, 2 hours after ischemia, right after the reperfusion, 2 h after reperfusion, and 4 hours after reperfusion; the animals survived for 24 hours after the reperfusion. After killing and triphenyltetrasoliumchloride staining of brain slices, infarction volumes and ratios of the brains were calculated and the results were compared with those of the control group.

RESULTS

Infarction volumes and infarction ratios of the Tizanidine group 1/2 hours before ischemia (143.7+/-6.34 mm3 and 10.1+/-0.43%) and the Tizanidine group 2 hours after ischemia (145.6+/-6.32 mm3 and 10.3+/-0.43%) were found to be significantly lower in favor of the Tizanidine groups when compared with those of the control group (173.9+/-6.38 mm3 and 12,4+/-0.41%). Tizanidine is not effective if used just after reperfusion or later.

CONCLUSION

This study shows that Tizanidine pretreatment before the ischemic insult and the administration of the drug within the 2 hours after ischemia reduces ischemic damage significantly. Therefore, this drug can be used as a protective and therapeutic agent in ischemic diseases.

摘要

背景

脑动脉闭塞继发的局灶性脑缺血仍是导致死亡和发病的重要原因。在缺血期间，兴奋性神经递质聚集在细胞外间隙，引发或刺激一系列病理生理生化过程，进而导致神经元死亡。替扎尼定（山德士化合物DS 103 - 282，5 - 氯 - 4,2 -（2 - 咪唑啉 - 2 - 基 - 氨基）- 2,1,3 - 苯并噻唑盐酸盐）是一种选择性α2肾上腺素能受体激动剂，它通过抑制天冬氨酸和谷氨酸的释放，刺激中枢天冬氨酸能和谷氨酸能系统中的突触前α2肾上腺素能受体来发挥作用。在本研究中，评估了替扎尼定对可逆性局灶性脑缺血的影响。

方法

将成年Sprague - Dawley大鼠（n = 48）的左半球脑血流通过大脑中动脉和双侧颈总动脉闭塞暂时阻断3小时，每组8只大鼠。在缺血损伤前、缺血后2小时、再灌注后即刻、再灌注后2小时和再灌注后4小时，对每组大鼠腹腔注射替扎尼定；动物在再灌注后存活24小时。处死动物并对脑切片进行氯化三苯基四氮唑染色后，计算脑梗死体积和梗死率，并将结果与对照组进行比较。

结果

发现缺血前1/2小时替扎尼定组（143.7±6.34 mm³和10.1±0.43%）和缺血后2小时替扎尼定组（145.6±6.32 mm³和10.3±0.43%）的梗死体积和梗死率与对照组（173.9±6.38 mm³和12.4±0.41%）相比，显著降低，替扎尼定组更具优势。如果在再灌注后即刻或之后使用替扎尼定则无效。