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大鼠内嗅皮质损伤导致齿状回迅速出现小胶质细胞反应。一项光镜和电镜研究。

Lesion of the rat entorhinal cortex leads to a rapid microglial reaction in the dentate gyrus. A light and electron microscopical study.

作者信息

Gehrmann J, Schoen S W, Kreutzberg G W

机构信息

Max-Planck-Institut für Psychiatrie, Abteilung für Neuromorphologie, Martinsried, Federal Republic of Germany.

出版信息

Acta Neuropathol. 1991;82(6):442-55. doi: 10.1007/BF00293378.

Abstract

Stereotaxic lesioning of the entorhinal cortex leads to an anterograde axonal degeneration in the molecular layer of the dentate gyrus. As revealed by immunocytochemical and histochemical methods, lesion of the entorhinal cortex induced a proliferation of microglia and an increased expression of established microglial activation markers within the deafferented zone. Reactive microglial cells were detected as early as 24 h after the lesion. The microglial reaction showed a maximum around day 3 post-lesion and disappeared by day 8 post-lesion. Reactive microglia were strongly positive for the B4-isolectin from Griffonia simplicifolia (GSI-B4), expressed high levels of CR3 complement receptor and 5'-nucleotidase, but lacked CD4 and MHC class I and II antigens. In addition, microglial cells were identified using MUC 102, a new monoclonal antibody against rat microglia. At the ultrastructural level, reactive microglial cells were consistently seen to phagocytose degenerating terminals. Our data suggest that (1) axonal degeneration represents a sufficient stimulus for inducing microglial activation and proliferation in the deafferented dentate gyrus; (2) these activated microglial cells are characterized by immunophenotypes different from those observed in other types of CNS injury; (3) the early microglial reaction precedes the well-documented astrocyte reaction in the dentate gyrus; and (4) the timed interaction of microglia and astrocytes could be important for regulating regenerative sprouting processes in the mature CNS.

摘要

内嗅皮质的立体定向损伤导致齿状回分子层出现顺行性轴突退变。免疫细胞化学和组织化学方法显示,内嗅皮质损伤诱导了小胶质细胞增殖,并使去传入区域内已确定的小胶质细胞活化标志物表达增加。损伤后24小时即可检测到反应性小胶质细胞。小胶质细胞反应在损伤后第3天左右达到峰值,并在损伤后第8天消失。反应性小胶质细胞对来自西非单叶豆的B4异凝集素(GSI-B4)呈强阳性,表达高水平的CR3补体受体和5'-核苷酸酶,但缺乏CD4以及MHC I类和II类抗原。此外,使用针对大鼠小胶质细胞的新型单克隆抗体MUC 102鉴定小胶质细胞。在超微结构水平上,始终可见反应性小胶质细胞吞噬退变的终末。我们的数据表明:(1)轴突退变是诱导去传入齿状回中小胶质细胞活化和增殖的充分刺激;(2)这些活化的小胶质细胞具有与其他类型中枢神经系统损伤中观察到的免疫表型不同的特征;(3)小胶质细胞早期反应先于齿状回中已充分记录的星形胶质细胞反应;(4)小胶质细胞和星形胶质细胞的定时相互作用可能对调节成熟中枢神经系统中的再生芽生过程很重要。

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