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NGL-2 调节视网膜中特定途径的神经突生长和分层、突触形成和信号传递。

NGL-2 regulates pathway-specific neurite growth and lamination, synapse formation, and signal transmission in the retina.

机构信息

Department of Ophthalmology and Visual Sciences, Washington University School of Medicine, St. Louis, MO 63110, USA.

出版信息

J Neurosci. 2013 Jul 17;33(29):11949-59. doi: 10.1523/JNEUROSCI.1521-13.2013.

Abstract

Parallel processing is an organizing principle of many neural circuits. In the retina, parallel neuronal pathways process signals from rod and cone photoreceptors and support vision over a wide range of light levels. Toward this end, rods and cones form triad synapses with dendrites of distinct bipolar cell types, and the axons or dendrites, respectively, of horizontal cells (HCs). The molecular cues that promote the formation of specific neuronal pathways remain largely unknown. Here, we discover that developing and mature HCs express the leucine-rich repeat (LRR)-containing protein netrin-G ligand 2 (NGL-2). NGL-2 localizes selectively to the tips of HC axons, which form reciprocal connections with rods. In mice with null mutations in Ngl-2 (Ngl-2⁻/⁻), many branches of HC axons fail to stratify in the outer plexiform layer (OPL) and invade the outer nuclear layer. In addition, HC axons expand lateral territories and increase coverage of the OPL, but establish fewer synapses with rods. NGL-2 can form transsynaptic adhesion complexes with netrin-G2, which we show to be expressed by photoreceptors. In Ngl-2⁻/⁻ mice, we find specific defects in the assembly of presynaptic ribbons in rods, indicating that reverse signaling of complexes involving NGL-2 regulates presynaptic maturation. The development of HC dendrites and triad synapses of cone photoreceptors proceeds normally in the absence of NGL-2 and in vivo electrophysiology reveals selective defects in rod-mediated signal transmission in Ngl-2⁻/⁻ mice. Thus, our results identify NGL-2 as a central component of pathway-specific development in the outer retina.

摘要

平行处理是许多神经回路的组织原则。在视网膜中,平行的神经元通路处理来自视杆和视锥光感受器的信号,并在广泛的光水平下支持视觉。为此,视杆和视锥与不同双极细胞类型的树突形成三联突触,而轴突或树突分别与水平细胞(HCs)形成三联突触。促进特定神经元通路形成的分子线索在很大程度上仍然未知。在这里,我们发现发育中和成熟的 HC 表达富含亮氨酸重复序列(LRR)的蛋白 netrin-G 配体 2(NGL-2)。NGL-2 选择性定位到 HC 轴突的尖端,HC 轴突与视杆形成相互连接。在 Ngl-2(Ngl-2⁻/⁻)缺失突变的小鼠中,许多 HC 轴突分支未能在外丛状层(OPL)分层,并侵入外核层。此外,HC 轴突扩展了侧部区域并增加了对 OPL 的覆盖,但与视杆建立的突触较少。NGL-2 可以与 netrin-G2 形成突触后粘附复合物,我们发现 netrin-G2 由光感受器表达。在 Ngl-2⁻/⁻小鼠中,我们发现视杆中突触前带的组装存在特定缺陷,表明涉及 NGL-2 的复合物的反向信号转导调节了突触前成熟。在没有 NGL-2 的情况下,HC 树突和视锥光感受器的三联突触发育正常,体内电生理学显示 Ngl-2⁻/⁻小鼠中杆介导的信号传递存在选择性缺陷。因此,我们的结果表明 NGL-2 是外视网膜中特定通路发育的核心组成部分。

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