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在缺乏信号素III的情况下,许多主要的中枢神经系统轴突投射仍能正常发育。

Many major CNS axon projections develop normally in the absence of semaphorin III.

作者信息

Catalano S M, Messersmith E K, Goodman C S, Shatz C J, Chédotal A

机构信息

Howard Hughes Medical Institute and Department of Molecular and Cell Biology, University of California, Berkeley, Berkeley, California, 94720-3200, USA.

出版信息

Mol Cell Neurosci. 1998 Jul;11(4):173-82. doi: 10.1006/mcne.1998.0687.

Abstract

The semaphorins constitute a large gene family of transmembrane and secreted molecules, many of which are expressed in the nervous system. Genetic studies in Drosophila have revealed a role for semaphorins in axon guidance and synapse formation, and several in vitro studies in mice have demonstrated a dramatic chemorepellent effect of semaphorin III (Sema III) on the axons of several populations of neurons. To investigate the function of Sema III during in vivo axon guidance in the mammalian CNS, we studied the development of axonal projections in mutant mice lacking Sema III. Projections were studied for which either the in vitro evidence suggests a role for Sema III in axon guidance (e.g., cerebellar mossy fibers, thalamocortical axons, or cranial motor neurons) or the in vivo expression suggests a role for Sema III in axon guidance (e.g., cerebellar Purkinje cells, neocortex). We find that many major axonal projections, including climbing fiber, mossy fiber, thalamocortical, and basal forebrain projections and cranial nerves, develop normally in the absence of Sema III. Despite its in vitro function and in vivo expression, it appears as if Sema III is not absolutely required for the formation of many major CNS tracts. Such data are consistent with recent models suggesting that axon guidance is controlled by a balance of forces resulting from multiple guidance cues. Our data lead us to suggest that if Sema III functions in part to guide the formation of major axonal projections, then it does so in combination with both other semaphorins and other families of guidance molecules.

摘要

信号素构成了一个由跨膜和分泌分子组成的大基因家族,其中许多在神经系统中表达。果蝇的遗传学研究揭示了信号素在轴突导向和突触形成中的作用,并且在小鼠中进行的多项体外研究表明,信号素III(Sema III)对多个神经元群体的轴突具有显著的化学排斥作用。为了研究Sema III在哺乳动物中枢神经系统体内轴突导向过程中的功能,我们研究了缺乏Sema III的突变小鼠中轴突投射的发育情况。我们研究了那些体外证据表明Sema III在轴突导向中起作用的投射(例如,小脑苔藓纤维、丘脑皮质轴突或颅运动神经元),以及体内表达表明Sema III在轴突导向中起作用的投射(例如,小脑浦肯野细胞、新皮层)。我们发现,许多主要的轴突投射,包括攀缘纤维、苔藓纤维、丘脑皮质和基底前脑投射以及颅神经,在没有Sema III的情况下正常发育。尽管Sema III具有体外功能和体内表达,但似乎许多主要的中枢神经系统通路的形成并不绝对需要Sema III。这些数据与最近的模型一致,该模型表明轴突导向是由多种导向线索产生的力的平衡所控制的。我们的数据使我们提出,如果Sema III部分地起到引导主要轴突投射形成的作用,那么它是与其他信号素和其他导向分子家族共同发挥作用的。

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