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大鼠和人类海马体中微管相关蛋白(tau、MAP2和MAP1B)水平及定位的死后变化

Postmortem changes in the levels and localization of microtubule-associated proteins (tau, MAP2 and MAP1B) in the rat and human hippocampus.

作者信息

Schwab C, Bondada V, Sparks D L, Cahan L D, Geddes J W

机构信息

Sanders-Brown Center on Aging, University of Kentucky, Lexington.

出版信息

Hippocampus. 1994 Apr;4(2):210-25. doi: 10.1002/hipo.450040212.

Abstract

The neuronal cytoskeleton is disrupted in neurodegenerative disorders such as Alzheimer's disease. Due to the lack of suitable animal models, studies examining the events involved in the neurodegeneration have relied on postmortem human brain tissue obtained from individuals with the disease and from normal controls. However, it is uncertain if the neuronal cytoskeleton is stable during the postmortem interval. Immunohistochemistry and immunoblots were used to examine the microtubule-associated proteins tau, MAP2, and MAP1B in the rat hippocampus at various times after death. Shortly after death, tau immunoreactivity was lost from axons and accumulated in somatodendritic compartments. MAP2 and MAP1B also accumulated in neuronal cell bodies prior to a loss of immunostaining in some regions, notably subiculum. Immunoblots confirmed a loss of MAP2 and MAP1B within a few hours after death. Tau levels remained constant during the 8-hour postmortem interval examined, although the electrophoretic mobility of some tau bands was altered. Human brain tissue obtained at autopsy and at surgery demonstrated similar cytoskeletal alterations in postmortem tissue. These results demonstrate that microtubules and associated proteins are not stable postmortem.

摘要

在诸如阿尔茨海默病等神经退行性疾病中,神经元细胞骨架会遭到破坏。由于缺乏合适的动物模型,研究神经退行性变所涉及的事件一直依赖于从患有该疾病的个体以及正常对照者获取的死后人类脑组织。然而,尚不确定在死后间隔期间神经元细胞骨架是否稳定。运用免疫组织化学和免疫印迹法,在大鼠死后的不同时间点检测海马体中的微管相关蛋白tau、微管相关蛋白2(MAP2)和微管相关蛋白1B(MAP1B)。死后不久,tau免疫反应性从轴突消失,并在体树突区室中积累。在某些区域,尤其是下托,MAP2和MAP1B在免疫染色消失之前也在神经元细胞体中积累。免疫印迹证实死后数小时内MAP2和MAP1B丢失。在所检测的8小时死后间隔期间,tau水平保持恒定,尽管一些tau条带的电泳迁移率发生了改变。尸检和手术时获取的人类脑组织在死后组织中显示出相似的细胞骨架改变。这些结果表明微管及相关蛋白在死后并不稳定。

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