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Robo 受体免疫球蛋白结构域的功能多样性促进了不同的轴突导向决定。

Functional diversity of Robo receptor immunoglobulin domains promotes distinct axon guidance decisions.

机构信息

Department of Neuroscience, University of Pennsylvania School of Medicine, 421 Curie Boulevard, Philadelphia, PA 19104, USA.

出版信息

Curr Biol. 2010 Mar 23;20(6):567-72. doi: 10.1016/j.cub.2010.02.021. Epub 2010 Mar 4.

Abstract

Recognition molecules of the immunoglobulin (Ig) superfamily control axon guidance in the developing nervous system. Ig-like domains are among the most widely represented protein domains in the human genome, and the number of Ig superfamily proteins is strongly correlated with cellular complexity. In Drosophila, three Roundabout (Robo) Ig superfamily receptors respond to their common Slit ligand to regulate axon guidance at the midline: Robo and Robo2 mediate midline repulsion, Robo2 and Robo3 control longitudinal pathway selection, and Robo2 can promote midline crossing. How these closely related receptors mediate distinct guidance functions is not understood. We report that the differential functions of Robo2 and Robo3 are specified by their ectodomains and do not reflect differences in cytoplasmic signaling. Functional modularity of Robo2's ectodomain facilitates multiple guidance decisions: Ig1 and Ig3 of Robo2 confer lateral positioning activity, whereas Ig2 confers promidline crossing activity. Robo2's distinct functions are not dependent on greater Slit affinity but are instead due in part to differences in multimerization and receptor-ligand stoichiometry conferred by Robo2's Ig domains. Together, our findings suggest that diverse responses to the Slit guidance cue are imparted by intrinsic structural differences encoded in the extracellular Ig domains of the Robo receptors.

摘要

免疫球蛋白 (Ig) 超家族的识别分子控制着发育中神经系统中的轴突导向。Ig 样结构域是人类基因组中最广泛存在的蛋白质结构域之一,Ig 超家族蛋白的数量与细胞复杂性密切相关。在果蝇中,三个 Roundabout (Robo) Ig 超家族受体对其共同的 Slit 配体做出反应,从而调节中线的轴突导向:Robo 和 Robo2 介导中线排斥,Robo2 和 Robo3 控制纵向通路选择,而 Robo2 可以促进中线穿越。这些密切相关的受体如何介导不同的导向功能尚不清楚。我们报告说,Robo2 和 Robo3 的功能差异是由它们的胞外结构域决定的,而不是细胞质信号传递的差异。Robo2 胞外结构域的功能模块化促进了多种导向决策:Robo2 的 Ig1 和 Ig3 赋予侧定位活性,而 Ig2 赋予中线穿越活性。Robo2 的不同功能并不依赖于更高的 Slit 亲和力,而是部分归因于 Robo2 的 Ig 结构域赋予的多聚化和受体-配体计量比的差异。总之,我们的发现表明,对 Slit 导向线索的不同反应是由 Robo 受体胞外 Ig 结构域中编码的内在结构差异赋予的。

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