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视网膜神经节细胞在出生后发育过程中突触足蛋白和轴突起始段的动态调节

Dynamic Regulation of Synaptopodin and the Axon Initial Segment in Retinal Ganglion Cells During Postnatal Development.

作者信息

Schlüter Annabelle, Rossberger Sabrina, Dannehl Dominik, Janssen Jan Maximilian, Vorwald Silke, Hanne Janina, Schultz Christian, Mauceri Daniela, Engelhardt Maren

机构信息

Institute of Neuroanatomy, Center for Biomedical Research and Medical Technology, Medical Faculty Mannheim, Heidelberg University, Mannheim, Germany.

Department of Neurobiology, Interdisciplinary Center for Neurosciences, Heidelberg University, Heidelberg, Germany.

出版信息

Front Cell Neurosci. 2019 Jul 30;13:318. doi: 10.3389/fncel.2019.00318. eCollection 2019.

Abstract

A key component allowing a neuron to function properly within its dynamic environment is the axon initial segment (AIS), the site of action potential generation. In visual cortex, AIS of pyramidal neurons undergo periods of activity-dependent structural plasticity during development. However, it remains unknown how AIS morphology is organized during development for downstream cells in the visual pathway (retinal ganglion cells; RGCs) and whether AIS retain the ability to dynamically adjust to changes in network state. Here, we investigated the maturation of AIS in RGCs during mouse retinal development, and tested putative activity-dependent mechanisms by applying visual deprivation with a focus on the AIS-specific cisternal organelle (CO), a presumed Ca-store. Whole-mount retinae from wildtype and Thy1-GFP transgenic mice were processed for multi-channel immunofluorescence using antibodies against AIS scaffolding proteins ankyrin-G, βIV-spectrin and the CO marker synaptopodin (synpo). Confocal microscopy in combination with morphometrical analysis of AIS length and position as well as synpo cluster size was performed. Data indicated that a subset of RGC AIS contains synpo clusters and that these show significant dynamic regulation in size during development as well as after visual deprivation. Using super resolution microscopy, we addressed the subcellular localization of synpo in RGC axons. Similar to cortical neurons, RGCs show a periodic distribution of AIS scaffolding proteins. A previously reported scaffold-deficient nanodomain correlating with synpo localization is not evident in all RGC AIS. In summary, our work demonstrates a dynamic regulation of both the AIS and synpo in RGCs during retinal development and after visual deprivation, providing first evidence that the AIS and CO in RGCs can undergo structural plasticity in response to changes in network activity.

摘要

轴突起始段(AIS)是动作电位产生的部位,是使神经元在其动态环境中正常发挥功能的关键组成部分。在视觉皮层中,锥体神经元的AIS在发育过程中经历活动依赖性结构可塑性的时期。然而,对于视觉通路中的下游细胞(视网膜神经节细胞;RGCs),AIS形态在发育过程中是如何组织的,以及AIS是否保留动态适应网络状态变化的能力,仍然未知。在这里,我们研究了小鼠视网膜发育过程中RGCs中AIS的成熟情况,并通过应用视觉剥夺来测试假定的活动依赖性机制,重点关注AIS特异性池状细胞器(CO),一种假定的钙储存器。使用针对AIS支架蛋白锚蛋白-G、βIV-血影蛋白和CO标记物突触素(synpo)的抗体,对来自野生型和Thy1-GFP转基因小鼠的全视网膜进行多通道免疫荧光处理。结合AIS长度和位置以及synpo簇大小的形态计量分析进行共聚焦显微镜检查。数据表明,一部分RGC AIS含有synpo簇,并且这些簇在发育过程中以及视觉剥夺后显示出大小上的显著动态调节。使用超分辨率显微镜,我们确定了synpo在RGC轴突中的亚细胞定位。与皮层神经元相似,RGCs显示出AIS支架蛋白的周期性分布。先前报道的与synpo定位相关的支架缺陷纳米结构域在所有RGC AIS中并不明显。总之,我们的工作证明了在视网膜发育过程中以及视觉剥夺后,RGCs中AIS和synpo的动态调节,提供了首个证据表明RGCs中的AIS和CO可以响应网络活动的变化而发生结构可塑性。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/a738/6682679/89757683e94e/fncel-13-00318-g001.jpg

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