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Netrin 1 和 Dcc 信号对于中枢轴突在中枢神经系统内的限制是必需的。

Netrin 1 and Dcc signalling are required for confinement of central axons within the central nervous system.

机构信息

Umeå Centre for Molecular Medicine, Umeå University, 901-87 Umeå, Sweden.

出版信息

Development. 2014 Feb;141(3):594-603. doi: 10.1242/dev.099606.

DOI:10.1242/dev.099606
PMID:24449837
Abstract

The establishment of anatomically stereotyped axonal projections is fundamental to neuronal function. While most neurons project their axons within the central nervous system (CNS), only axons of centrally born motoneurons and peripherally born sensory neurons link the CNS and peripheral nervous system (PNS) together by navigating through specialized CNS/PNS transition zones. Such selective restriction is of importance because inappropriate CNS axonal exit could lead to loss of correct connectivity and also to gain of erroneous functions. However, to date, surprisingly little is known about the molecular-genetic mechanisms that regulate how central axons are confined within the CNS during development. Here, we show that netrin 1/Dcc/Unc5 chemotropism contributes to axonal confinement within the CNS. In both Ntn1 and Dcc mutant mouse embryos, some spinal interneuronal axons exit the CNS by traversing the CNS/PNS transition zones normally reserved for motor and sensory axons. We provide evidence that netrin 1 signalling preserves CNS/PNS axonal integrity in three ways: (1) netrin 1/Dcc ventral attraction diverts axons away from potential exit points; (2) a Dcc/Unc5c-dependent netrin 1 chemoinhibitory barrier in the dorsolateral spinal cord prevents interneurons from being close to the dorsal CNS/PNS transition zone; and (3) a netrin 1/Dcc-dependent, Unc5c-independent mechanism that actively prevents exit from the CNS. Together, these findings provide insights into the molecular mechanisms that maintain CNS/PNS integrity and, to the best of our knowledge, present the first evidence that chemotropic signalling regulates interneuronal CNS axonal confinement in vertebrates.

摘要

轴突在解剖学上的定向投射对于神经元的功能至关重要。虽然大多数神经元将其轴突投射到中枢神经系统(CNS)内,但只有中枢神经系统产生的运动神经元和外周神经系统产生的感觉神经元的轴突通过穿越专门的 CNS/PNS 过渡区将 CNS 和外周神经系统(PNS)连接在一起。这种选择性限制很重要,因为中枢轴突的不当退出可能导致正确连接的丧失,以及错误功能的获得。然而,迄今为止,人们对调节中枢轴突在发育过程中如何被局限在 CNS 内的分子遗传机制知之甚少。在这里,我们表明 netrin 1/Dcc/Unc5 趋化性有助于轴突在 CNS 内的限制。在 Ntn1 和 Dcc 突变体小鼠胚胎中,一些脊髓中间神经元轴突通过穿越通常保留给运动和感觉轴突的 CNS/PNS 过渡区而离开 CNS。我们提供的证据表明,netrin 1 信号通过三种方式来维持 CNS/PNS 轴突的完整性:(1)netrin 1/Dcc 腹侧吸引使轴突远离潜在的退出点;(2)在背外侧脊髓中的 Dcc/Unc5c 依赖性 netrin 1 化学抑制性屏障阻止中间神经元靠近背侧 CNS/PNS 过渡区;(3)netrin 1/Dcc 依赖性、Unc5c 非依赖性的机制,可积极阻止从 CNS 退出。这些发现共同为维持 CNS/PNS 完整性的分子机制提供了深入的见解,据我们所知,这是第一个表明化学趋化性信号调节脊椎动物中间神经元 CNS 轴突限制的证据。

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