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斑马鱼视网膜变性和再生过程中小胶质细胞和巨噬细胞特征的动态变化。

Dynamic changes in microglial and macrophage characteristics during degeneration and regeneration of the zebrafish retina.

机构信息

Department of Biological Sciences, University of Idaho, 875 Perimeter Drive, MS 3051, Moscow, ID, 83844-3051, USA.

出版信息

J Neuroinflammation. 2018 May 28;15(1):163. doi: 10.1186/s12974-018-1185-6.

Abstract

BACKGROUND

In contrast to mammals, zebrafish have the capacity to regenerate retinal neurons following a variety of injuries. Two types of glial cells, Müller glia (MG) and microglia, are known to exist in the zebrafish retina. Recent work has shown that MG give rise to regenerated retinal neurons, but the role of resident microglia, and the innate immune system more generally, during retinal regeneration is not well defined. Specifically, characteristics of the immune system and microglia following substantial neuron death and a successful regenerative response have not been documented.

METHODS

The neurotoxin ouabain was used to induce a substantial retinal lesion of the inner retina in zebrafish. This lesion results in a regenerative response that largely restores retinal architecture, neuronal morphologies, and connectivities, as well as recovery of visual function. We analyzed cryosections from damaged eyes following immunofluorescence and H&E staining to characterize the initial immune response to the lesion. Whole retinas were analyzed by confocal microscopy to characterize microglia morphology and distribution. Statistical analysis was performed using a two-tailed Student's t test comparing damaged to control samples.

RESULTS

We find evidence of early leukocyte infiltration to the retina in response to ouabain injection followed by a period of immune cell proliferation that likely includes both resident microglia and substantial numbers of proliferating, extra-retinally derived macrophages, leading to rapid accumulation upon retinal damage. Following immune cell proliferation, Müller glia re-enter the cell cycle. In retinas that have regenerated the layers lost to the initial injury (histologically regenerated), microglia retain morphological features of activation, suggesting ongoing functions that are likely essential to restoration of retinal function.

CONCLUSIONS

Collectively, these results indicate that microglia and the immune system are dynamic during a successful regenerative response in the retina. This study provides an important framework to probe inflammation in the initiation of, and functional roles of microglia during retinal regeneration.

摘要

背景

与哺乳动物不同,斑马鱼在受到各种损伤后能够再生视网膜神经元。已知在斑马鱼的视网膜中有两种神经胶质细胞,即 Muller 胶质细胞(MG)和小胶质细胞。最近的研究表明,MG 产生再生的视网膜神经元,但在视网膜再生过程中,常驻小胶质细胞和固有免疫系统的作用尚不清楚。具体来说,大量神经元死亡和成功的再生反应后,免疫系统和小胶质细胞的特征尚未被记录。

方法

使用神经毒素哇巴因在斑马鱼中诱导大量的内视网膜损伤。这种损伤会引发再生反应,在很大程度上恢复视网膜结构、神经元形态和连接性,以及视觉功能的恢复。我们通过免疫荧光和 H&E 染色分析受损眼睛的冷冻切片,以表征对损伤的初始免疫反应。通过共聚焦显微镜分析整个视网膜,以表征小胶质细胞形态和分布。使用双尾学生 t 检验比较损伤和对照样本进行统计分析。

结果

我们发现哇巴因注射后有证据表明白细胞早期浸润到视网膜,随后是免疫细胞增殖期,其中可能包括常驻小胶质细胞和大量增殖的、来自视网膜外的巨噬细胞,导致在视网膜损伤后迅速积累。在免疫细胞增殖之后,Muller 胶质细胞重新进入细胞周期。在初始损伤导致的层丢失(组织学上再生)已再生的视网膜中,小胶质细胞保留激活的形态特征,这表明持续的功能可能对视网膜功能的恢复至关重要。

结论

总之,这些结果表明,小胶质细胞和免疫系统在视网膜成功再生反应中是动态的。这项研究为探究炎症在视网膜再生起始中的作用以及小胶质细胞在视网膜再生中的功能作用提供了重要框架。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/bc99/5971432/3ad66fac8b93/12974_2018_1185_Fig1_HTML.jpg

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