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小胶质细胞 Cx3cr1 通路在视网膜光感受器出生后成熟中的作用。

The Role of the Microglial Cx3cr1 Pathway in the Postnatal Maturation of Retinal Photoreceptors.

机构信息

Department of Anatomy and Neuroscience, The University of Melbourne, Parkville 3010 Victoria, Australia.

Department of Anatomy and Neuroscience, The University of Melbourne, Parkville 3010 Victoria, Australia

出版信息

J Neurosci. 2018 May 16;38(20):4708-4723. doi: 10.1523/JNEUROSCI.2368-17.2018. Epub 2018 Apr 18.

Abstract

Microglia are the resident immune cells of the CNS, and their response to infection, injury and disease is well documented. More recently, microglia have been shown to play a role in normal CNS development, with the fractalkine-Cx3cr1 signaling pathway of particular importance. This work describes the interaction between the light-sensitive photoreceptors and microglia during eye opening, a time of postnatal photoreceptor maturation. Genetic removal of Cx3cr1 ( ) led to an early retinal dysfunction soon after eye opening [postnatal day 17 (P17)] and cone photoreceptor loss (P30 onward) in mice of either sex. This dysfunction occurred at a time when fractalkine expression was predominantly outer retinal, when there was an increased microglial presence near the photoreceptor layer and increased microglial-cone photoreceptor contacts. Photoreceptor maturation and outer segment elongation was coincident with increased opsin photopigment expression in wild-type retina, while this was aberrant in the retina and outer segment length was reduced. A beadchip array highlighted Cx3cr1 regulation of genes involved in the photoreceptor cilium, a key structure that is important for outer segment elongation. This was confirmed with quantitative PCR with specific cilium-related genes, and , downregulated at eye opening (P14). While the overall cilium structure was unaffected, expression of Rpgr, Rpgrip1, and centrin were restricted to more proximal regions of the transitional zone. This study highlighted a novel role for microglia in postnatal neuronal development within the retina, with loss of fractalkine-Cx3cr1 signaling leading to an altered distribution of cilium proteins, failure of outer segment elongation and ultimately cone photoreceptor loss. Microglia are involved in CNS development and disease. This work highlights the role of microglia in postnatal development of the light-detecting photoreceptor neurons within the mouse retina. Loss of the microglial Cx3cr1 signaling pathway resulted in specific alterations in the cilium, a key structure in photoreceptor outer segment elongation. The distribution of key components of the cilium transitional zone, Rpgr, Rpgrip1, and centrin, were altered in retinae lacking Cx3cr1 with reduced outer segment length and cone photoreceptor death observed at later postnatal ages. This work identifies a novel role for microglia in the postnatal maturation of retinal photoreceptors.

摘要

小胶质细胞是中枢神经系统的常驻免疫细胞,其对感染、损伤和疾病的反应已有充分的记录。最近,小胶质细胞在中枢神经系统的正常发育中发挥了作用,其中 fractalkine-Cx3cr1 信号通路尤为重要。这项工作描述了光敏感感光器与小胶质细胞在眼睛张开过程中的相互作用,眼睛张开是一个后生感光器成熟的时期。在眼睛张开后不久(出生后 17 天(P17)),Cx3cr1(-/-)基因缺失的小鼠出现了早期视网膜功能障碍,并且在两性小鼠中出现了视锥细胞丧失(P30 及以后)。这种功能障碍发生在 fractalkine 表达主要在外视网膜时,此时在感光器层附近有更多的小胶质细胞存在,并且小胶质细胞-视锥细胞接触增加。感光器成熟和外节伸长与野生型视网膜中视蛋白光色素表达的增加同时发生,而在 视网膜中则出现异常,外节长度缩短。beadchip 阵列突出显示了 Cx3cr1 对参与光感受器纤毛的基因的调节作用,纤毛是一个重要的结构,对于外节伸长很重要。这通过定量 PCR 与特定的纤毛相关基因 、 和 得到了证实,这些基因在眼睛张开时(P14)下调。虽然整体纤毛结构不受影响,但 Rpgr、Rpgrip1 和 centrin 的表达仅限于过渡区的更近端区域。这项研究强调了小胶质细胞在视网膜后生神经元发育中的新作用,在 fractalkine-Cx3cr1 信号转导缺失后,纤毛蛋白的分布发生改变,外节伸长失败,最终导致视锥细胞丧失。小胶质细胞参与中枢神经系统的发育和疾病。这项工作强调了小胶质细胞在小鼠视网膜内光探测感光器神经元后生发育中的作用。小胶质细胞 Cx3cr1 信号通路的缺失导致纤毛的特定改变,纤毛是感光器外节伸长的关键结构。在缺乏 Cx3cr1 的视网膜中,纤毛过渡区的关键成分 Rpgr、Rpgrip1 和 centrin 的分布发生改变,外节长度缩短,并且在后期的后生年龄观察到视锥细胞死亡。这项工作确定了小胶质细胞在后生视网膜感光器成熟中的新作用。

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