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沙鼠脑缺血的免疫组织化学研究

Immunohistochemical investigation of cerebral ischemia in gerbils.

作者信息

Yanagihara T, Yoshimine T, Morimoto K, Yamamoto K, Homburger H A

出版信息

J Neuropathol Exp Neurol. 1985 Mar;44(2):204-15. doi: 10.1097/00005072-198503000-00009.

Abstract

Experimental cerebral ischemia was produced in gerbils by occlusion of the right common carotid artery in the neck. The evolution of the ischemic lesions was followed from five minutes to six hours by using the immunohistochemical techniques for tubulin and creatine kinase BB-isoenzyme. The earliest lesion was found in the subiculum-CA1 and CA2 regions of the hippocampus in five minutes. There was loss of staining in the apical dendrites and perikarya of the pyramidal cells. The earliest lesion in the cerebral cortex, visible in ten minutes, was a laminar loss of staining for tubulin. Evolution of the ischemic lesions in the thalamus and caudoputamen was delayed. However, in two hours widespread ischemic lesions were seen there. Evolution of the ischemic lesions was slightly slower with the reaction for creatine kinase BB-isoenzyme as compared to the reaction for tubulin, but was far more sensitive than hematoxylin-eosin staining. The distribution of ischemic lesions detected by the immunohistochemical method compared to ischemic areas detected by an India ink perfusion study suggested that both the extent of regional ischemia and regional difference in tissue vulnerability were contributing factors for the emergence of early ischemic lesions. The mechanism for prompt disappearance of the immunohistochemical reaction for tubulin is not clear, but the present investigation demonstrates the usefulness of the immunohistochemical technique for detecting early ischemic lesions and provides a possible biochemical mechanism for cellular damage after ischemic insults.

摘要

通过结扎颈部右侧颈总动脉在沙鼠身上制造实验性脑缺血。利用微管蛋白和肌酸激酶BB同工酶的免疫组织化学技术,观察缺血性病变从5分钟到6小时的演变过程。最早的病变在5分钟时出现在海马的下托 - CA1和CA2区域。锥体细胞的顶端树突和胞体出现染色缺失。大脑皮层最早的病变在10分钟时可见,表现为微管蛋白的层状染色缺失。丘脑和尾状核缺血性病变的演变延迟。然而,在2小时时在那里可见广泛的缺血性病变。与微管蛋白反应相比,肌酸激酶BB同工酶反应的缺血性病变演变稍慢,但比苏木精 - 伊红染色敏感得多。免疫组织化学方法检测到的缺血性病变分布与印度墨汁灌注研究检测到的缺血区域相比,表明局部缺血程度和组织易损性的区域差异都是早期缺血性病变出现的促成因素。微管蛋白免疫组织化学反应迅速消失的机制尚不清楚,但本研究证明了免疫组织化学技术在检测早期缺血性病变方面的有用性,并为缺血性损伤后细胞损伤提供了一种可能的生化机制。

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