DSCAM差异调节突触前和突触后结构和功能中枢连接在视觉系统布线。

IF 4 3区 生物学 Q1 DEVELOPMENTAL BIOLOGY Neural Development Pub Date : 2018-09-15 DOI:10.1186/s13064-018-0118-5
Rommel A Santos, Ariel J C Fuertes, Ginger Short, Kevin C Donohue, Hanjuan Shao, Julian Quintanilla, Parinaz Malakzadeh, Susana Cohen-Cory
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引用次数: 20

摘要

背景:树突和轴突的正确模式是形成功能性神经元回路的关键步骤。发育中的神经回路依赖于一系列分子线索来塑造树杈形态,但实时指导突触前和突触后树杈结构形成和相互连接的潜在机制尚不清楚。在这里,我们探讨唐氏综合征细胞粘附分子(DSCAM)如何在发育中的脊椎动物视觉系统中不同地塑造中枢神经元及其突触前视网膜神经节细胞(RGC)轴突的树突形态。方法:采用靶向单细胞敲除和过表达的方法,在发育中的非洲爪蟾蝌蚪中检测DSCAM在顶盖神经元和RGCs中的细胞自主作用。RGCs的轴突突和顶叶神经元的树突突在3天的实时体内共聚焦显微镜成像中可见。结果:在爪蟾视觉系统中,DSCAM免疫反应性存在于视顶叶的RGCs、视顶叶的细胞和顶叶神经细胞中。在顶状神经元中下调DSCAM可显著增加树突生长和分支速率,并诱导树突弯曲路径。相反,DSCAM的过表达减少了树突分支和生长速度。通过视觉引导的行为实验,研究了蝌蚪游泳过程中DSCAM基因敲除介导的功能缺陷,揭示了蝌蚪对视觉刺激的不规则行为反应。视觉行为的功能缺陷也与顶盖兴奋性和抑制性传递标志物VGLUT/VGAT表达的变化相对应。相反,单细胞DSCAM在视网膜中的敲除表明,RGC轴突在靶点的树突受DSCAM的影响,轴突生长速度较慢,保持相对简单。在视网膜中,RGCs的树突乔木不受DSCAM表达减少的影响。综上所述,我们的观察结果表明DSCAM在发育中的视网膜顶回路中控制突触前和突触后的结构和功能连接,在那里它主要作为神经元制动器限制和引导顶神经元的突触后树突生长,同时它也促进突触前RGC轴突细胞自主树突化。
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DSCAM differentially modulates pre- and postsynaptic structural and functional central connectivity during visual system wiring.

Background: Proper patterning of dendritic and axonal arbors is a critical step in the formation of functional neuronal circuits. Developing circuits rely on an array of molecular cues to shape arbor morphology, but the underlying mechanisms guiding the structural formation and interconnectivity of pre- and postsynaptic arbors in real time remain unclear. Here we explore how Down syndrome cell adhesion molecule (DSCAM) differentially shapes the dendritic morphology of central neurons and their presynaptic retinal ganglion cell (RGC) axons in the developing vertebrate visual system.

Methods: The cell-autonomous role of DSCAM, in tectal neurons and in RGCs, was examined using targeted single-cell knockdown and overexpression approaches in developing Xenopus laevis tadpoles. Axonal arbors of RGCs and dendritic arbors of tectal neurons were visualized using real-time in vivo confocal microscopy imaging over the course of 3 days.

Results: In the Xenopus visual system, DSCAM immunoreactivity is present in RGCs, cells in the optic tectum and the tectal neuropil at the time retinotectal synaptic connections are made. Downregulating DSCAM in tectal neurons significantly increased dendritic growth and branching rates while inducing dendrites to take on tortuous paths. Overexpression of DSCAM, in contrast, reduced dendritic branching and growth rate. Functional deficits mediated by tectal DSCAM knockdown were examined using visually guided behavioral assays in swimming tadpoles, revealing irregular behavioral responses to visual stimulus. Functional deficits in visual behavior also corresponded with changes in VGLUT/VGAT expression, markers of excitatory and inhibitory transmission, in the tectum. Conversely, single-cell DSCAM knockdown in the retina revealed that RGC axon arborization at the target is influenced by DSCAM, where axons grew at a slower rate and remained relatively simple. In the retina, dendritic arbors of RGCs were not affected by the reduction of DSCAM expression.

Conclusions: Together, our observations implicate DSCAM in the control of both pre- and postsynaptic structural and functional connectivity in the developing retinotectal circuit, where it primarily acts as a neuronal brake to limit and guide postsynaptic dendrite growth of tectal neurons while it also facilitates arborization of presynaptic RGC axons cell autonomously.

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来源期刊
Neural Development
Neural Development 生物-发育生物学
CiteScore
6.60
自引率
0.00%
发文量
11
审稿时长
>12 weeks
期刊介绍: Neural Development is a peer-reviewed open access, online journal, which features studies that use molecular, cellular, physiological or behavioral methods to provide novel insights into the mechanisms that underlie the formation of the nervous system. Neural Development aims to discover how the nervous system arises and acquires the abilities to sense the world and control adaptive motor output. The field includes analysis of how progenitor cells form a nervous system during embryogenesis, and how the initially formed neural circuits are shaped by experience during early postnatal life. Some studies use well-established, genetically accessible model systems, but valuable insights are also obtained from less traditional models that provide behavioral or evolutionary insights.
期刊最新文献
Correction: Embryonic development of a centralised brain in coleoid cephalopods. Terminal differentiation precedes functional circuit integration in the peduncle neurons in regenerating Hydra vulgaris. Mapping the cellular expression patterns of vascular endothelial growth factor aa and bb genes and their receptors in the adult zebrafish brain during constitutive and regenerative neurogenesis LRRK2 kinase activity is necessary for development and regeneration in Nematostella vectensis. Correction: scMultiome analysis identifies a single caudal hindbrain compartment in the developing zebrafish nervous system
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