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大脑中动脉永久性闭塞后大鼠脑片中小胶质细胞和血源性细胞的不同生理特性

Distinct physiologic properties of microglia and blood-borne cells in rat brain slices after permanent middle cerebral artery occlusion.

作者信息

Lyons S A, Pastor A, Ohlemeyer C, Kann O, Wiegand F, Prass K, Knapp F, Kettenmann H, Dirnagl U

机构信息

Cellular Neuroscience, Max Delbrück Center for Molecular Medicine, Berlin, Germany.

出版信息

J Cereb Blood Flow Metab. 2000 Nov;20(11):1537-49. doi: 10.1097/00004647-200011000-00003.

Abstract

The authors investigated the time course of leukocyte infiltration compared with microglial activation in adult rat brain slices after permanent middle cerebral artery occlusion (MCAO). To distinguish peripheral leukocytes from microglia, the blood cells were prelabeled in vivo with Rhodamine 6G (Rhod6G) i.v. before induction of ischemia. At specific times after infarct, invading leukocytes, microglia, and endothelial cells were labeled in situ with isolectin (IL)B4-FITC (ILB4). Six hours after MCAO only a few of the ILB4+ cells were colabeled by Rhod6G. These cells expressed the voltage-gated inwardly and outwardly rectifying K+ currents characteristic of macrophages. The majority of the ILB4+ cells were Rhod6G- and expressed a lack of voltage-gated channels, recently described for ramified microglial cells in brain slices, or exhibited only an inward rectifier current, a unique marker for cultured (but unstimulated) microglia. Forty-eight hours after MCAO, all blood-borne and the majority of Rhod6G- cells expressed outward and inward currents indicating that the intrinsic microglial population exhibited physiologic features of stimulated, cultured microglia. The ILB4+/Rhod6G- intrinsic microglial population was more abundant in the border zone of the infarct and their morphology changed from radial to ameboid. Within this zone, the authors observed rapidly migrating cells and recorded this movement by time-lapse microscopy. The current findings indicate that microglial cells acquire physiologic features of leukocytes at a later time point after MCAO.

摘要

作者研究了成年大鼠大脑切片在大脑中动脉永久性闭塞(MCAO)后白细胞浸润与小胶质细胞激活的时间进程。为了区分外周白细胞和小胶质细胞,在缺血诱导前,通过静脉注射罗丹明6G(Rhod6G)对血细胞进行体内预标记。在梗死发生后的特定时间,用异凝集素(IL)B4-异硫氰酸荧光素(ILB4)对侵入的白细胞、小胶质细胞和内皮细胞进行原位标记。MCAO后6小时,只有少数ILB4+细胞被Rhod6G共标记。这些细胞表达了巨噬细胞特有的电压门控内向和外向整流钾电流。大多数ILB4+细胞为Rhod6G阴性,表达缺乏电压门控通道,这是最近在脑切片中描述的分支状小胶质细胞的特征,或者仅表现出内向整流电流,这是培养的(但未刺激的)小胶质细胞的独特标记。MCAO后48小时,所有血源性细胞和大多数Rhod6G阴性细胞均表达外向和内向电流,表明内在的小胶质细胞群体表现出受刺激的培养小胶质细胞的生理特征。ILB4+/Rhod6G阴性的内在小胶质细胞群体在梗死边缘区更为丰富,其形态从放射状变为阿米巴样。在这个区域内,作者观察到快速迁移的细胞,并通过延时显微镜记录了这种运动。目前的研究结果表明,小胶质细胞在MCAO后的较晚时间点获得白细胞的生理特征。

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