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来自单个神经元的中枢和外周轴突分支受信号素3D和瞬时轴突糖蛋白-1的不同引导。

Central and peripheral axon branches from one neuron are guided differentially by Semaphorin3D and transient axonal glycoprotein-1.

作者信息

Liu Yan, Halloran Mary C

机构信息

Department of Zoology, University of Wisconsin, Madison, Wisconsin 53706, USA.

出版信息

J Neurosci. 2005 Nov 9;25(45):10556-63. doi: 10.1523/JNEUROSCI.2710-05.2005.

Abstract

For multiple axons from one neuron to extend in different directions to unique targets, the growth cones of each axon must have distinct responses to guidance cues. However, the mechanisms by which separate axon branches are guided along different pathways are mainly unknown. Zebrafish Rohon-Beard (R-B) sensory neurons extend central axon branches in the spinal cord and peripheral axons to the epidermis. To investigate the differential guidance mechanisms of the central versus peripheral R-B axon branches, we used live-growth cone imaging in vivo combined with manipulation of individual guidance molecules. We show that a semaphorin expressed at the dorsal spinal cord midline, Semaphorin3D (Sema3D), may act to repel the peripheral axons out of the spinal cord. Sema3D knock-down reduces the number of peripheral axons. Remarkably, Sema3D ectopic expression repels and induces branching of peripheral axons in vivo but has no effect on central axons from the same neurons. Conversely, central axons require a growth-promoting molecule, transient axonal glycoprotein-1 (TAG-1), to advance, whereas peripheral axons do not. After TAG-1 knock-down, central growth cones display extensive protrusive activity but make little forward advance. TAG-1 knock-down has no effect on the motility or advance of peripheral growth cones. These experiments show how Sema3D and TAG-1 regulate the motility and behavior of growth cones extending in their natural in vivo environment and demonstrate that two different axon branches from one neuron respond differently to guidance cues in vivo.

摘要

为了使来自一个神经元的多个轴突向不同方向延伸至独特的靶标,每个轴突的生长锥必须对导向线索有不同的反应。然而,单独的轴突分支沿不同路径被导向的机制主要尚不清楚。斑马鱼的罗霍恩-比尔(R-B)感觉神经元在脊髓中延伸中央轴突分支,并向表皮延伸外周轴突。为了研究中央与外周R-B轴突分支的差异导向机制,我们在体内使用实时生长锥成像并结合对单个导向分子的操控。我们发现,在脊髓背侧中线表达的一种信号素,信号素3D(Sema3D),可能起到将外周轴突排斥出脊髓的作用。敲低Sema3D会减少外周轴突的数量。值得注意的是,Sema3D的异位表达在体内排斥并诱导外周轴突分支,但对来自同一神经元的中央轴突没有影响。相反,中央轴突需要一种促进生长的分子,瞬时轴突糖蛋白-1(TAG-1)才能向前延伸,而外周轴突则不需要。敲低TAG-1后,中央生长锥表现出广泛的突出活动,但几乎没有向前推进。敲低TAG-1对外周生长锥的运动性或推进没有影响。这些实验展示了Sema3D和TAG-1如何在其自然体内环境中调节生长锥的运动性和行为,并证明来自一个神经元的两个不同轴突分支在体内对导向线索的反应不同。

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