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小鼠视网膜光诱导感光细胞变性的小胶质细胞反应。

Microglial response to light-induced photoreceptor degeneration in the mouse retina.

机构信息

Departamento de Biología Celular, Facultad de Ciencias, Universidad de Granada, E-18071 Granada, Spain.

出版信息

J Comp Neurol. 2010 Feb 15;518(4):477-92. doi: 10.1002/cne.22227.

DOI:10.1002/cne.22227
PMID:20020538
Abstract

The microglial response elicited by degeneration of retinal photoreceptor cells was characterized in BALB/c mice exposed to bright light for 7 hours and then kept in complete darkness for survival times ranging from 0 hours to 10 days. Photodegeneration resulted in extensive cell death in the retina, mainly in the outer nuclear layer (ONL), where the photoreceptor nuclei are located. Specific immunolabeling of microglial cells with anti-CD11b, anti-CD45, anti-F4/80, anti-SRA, and anti-CD68 antibodies revealed that microglial cells were activated in light-exposed retinas. They migrated to the ONL, changed their morphology, becoming rounded cells with short and thick processes, and, finally, showed immunophenotypic changes. Specifically, retinal microglia began to strongly express antigens recognized by anti-CD11b, anti-CD45, and anti-F4/80, coincident with cell degeneration. In contrast, upregulation of the antigen recognized by anti-SRA was not detected by immunocytochemistry until 6 hours after light exposure. Differences were also observed at 10 days after light exposure: CD11b, CD45, and F4/80 continued to be strongly expressed in retinal microglia, whereas the expression of CD68 and SRA had decreased to near-normal values. Therefore, microglia did not return to their original state after photodegeneration and continued to show a degree of activation. The accumulation of activated microglial cells in affected regions simultaneously with photoreceptor degeneration suggests that they play some role in photodegeneration.

摘要

在暴露于强光 7 小时然后在完全黑暗中存活 0 至 10 天的 BALB/c 小鼠中,研究了由视网膜光感受器细胞变性引起的小胶质细胞反应。光变性导致视网膜中广泛的细胞死亡,主要在外核层 (ONL) 中,光感受器核位于该处。用抗 CD11b、抗 CD45、抗 F4/80、抗 SRA 和抗 CD68 抗体对小胶质细胞进行特异性免疫标记,显示光暴露的视网膜中小胶质细胞被激活。它们迁移到 ONL,改变其形态,变成具有短而粗突起的圆形细胞,最终表现出免疫表型变化。具体而言,视网膜小胶质细胞开始强烈表达被抗 CD11b、抗 CD45 和抗 F4/80 识别的抗原,与细胞变性一致。相比之下,用光照射后 6 小时才通过免疫细胞化学检测到抗 SRA 识别的抗原的上调。在光暴露 10 天后也观察到差异:CD11b、CD45 和 F4/80 在视网膜小胶质细胞中继续强烈表达,而 CD68 和 SRA 的表达已降低到接近正常水平。因此,光变性后小胶质细胞没有恢复到原来的状态,并且继续表现出一定程度的激活。受影响区域中活化的小胶质细胞与光感受器变性同时积累,表明它们在光变性中发挥某些作用。

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