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Dscam1 Forms a Complex with Robo1 and the N-Terminal Fragment of Slit to Promote the Growth of Longitudinal Axons

机译:Dscam1与Robo1和狭缝的N末端片段形成复合体以促进纵向轴突的生长。

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摘要

The Slit protein is a major midline repellent for central nervous system (CNS) axons. In vivo, Slit is proteolytically cleaved into N- and C-terminal fragments, but the biological significance of this is unknown. Analysis in the Drosophila ventral nerve cord of a slit allele (slit-UC) that cannot be cleaved revealed that midline repulsion is still present but longitudinal axon guidance is disrupted, particularly across segment boundaries. Double mutants for the Slit receptors Dscam1 and robo1 strongly resemble the slit-UC phenotype, suggesting they cooperate in longitudinal axon guidance, and through biochemical approaches, we found that Dscam1 and Robo1 form a complex dependent on Slit-N. In contrast, Robo1 binding alone shows a preference for full-length Slit, whereas Dscam1 only binds Slit-N. Using a variety of transgenes, we demonstrated that Dscam1 appears to modify the output of Robo/Slit complexes so that signaling is no longer repulsive. Our data suggest that the complex is promoting longitudinal axon growth across the segment boundary. The ability of Dscam1 to modify the output of other receptors in a ligand-dependent fashion may be a general principle for Dscam proteins.
机译:Slit蛋白是中枢神经系统(CNS)轴突的主要中线驱避剂。在体内,Slit被蛋白水解切割成N和C末端片段,但是其生物学意义尚不清楚。在果蝇腹侧神经索中,无法切割的狭缝等位基因(slit-UC)的分析显示,中线排斥仍然存在,但纵向轴突导向受到干扰,尤其是跨节边界。 Slit受体Dscam1和robo1的双突变体非常类似于狭缝UC表型,表明它们在纵向轴突导向中协同作用,并且通过生化方法,我们发现Dscam1和Robo1形成了依赖于Slit-N的复合体。相反,单独的Robo1绑定显示对全长Slit的偏好,而Dscam1仅绑定Slit-N。使用各种转基因,我们证明了Dscam1似乎修饰了Robo / Slit复合物的输出,因此信号不再具有排斥性。我们的数据表明,该复合物正在促进跨节边界的纵向轴突生长。 Dscam1以配体依赖性方式修饰其他受体输出的能力可能是Dscam蛋白的一般原理。

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