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Diversity of oligomerization in Drosophila semaphorins suggests a mechanism of functional fine-tuning

机译:果蝇semaphorins中寡聚的多样性表明功能微调的机制

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摘要

Semaphorin ligands and their plexin receptors are one of the major cell guidance factors that trigger localised changes in the cytoskeleton. Binding of semaphorin homodimer to plexin brings two plexins in close proximity which is a prerequisite for plexin signalling. This model appears to be too simplistic to explain the complexity and functional versatility of these molecules. Here, we determine crystal structures for all members of Drosophila class 1 and 2 semaphorins. Unlike previously reported semaphorin structures, Sema1a, Sema2a and Sema2b show stabilisation of sema domain dimer formation via a disulfide bond. Unexpectedly, our structural and biophysical data show Sema1b is a monomer suggesting that semaphorin function may not be restricted to dimers. We demonstrate that semaphorins can form heterodimers with members of the same semaphorin class. This heterodimerization provides a potential mechanism for cross-talk between different plexins and co-receptors to allow fine-tuning of cell signalling.
机译:信号量配体及其Plexin受体是触发细胞骨架局部变化的主要细胞指导因子之一。信号量同型二聚体与plexin的结合使两个plexins紧密接近,这是plexin信号转导的先决条件。该模型似乎过于简单,无法解释这些分子的复杂性和功能多样性。在这里,我们确定果蝇1类和2类信号灯的所有成员的晶体结构。与以前报道的信号量结构不同,Sema1a,Sema2a和Sema2b通过二硫键显示出稳定的信号域二聚体形成。出乎意料的是,我们的结构和生物物理数据显示Sema1b是单体,表明信号量蛋白功能可能不限于二聚体。我们证明信号量可以与同一个信号量类的成员形成异二聚体。这种异源二聚化提供了一种潜在的机制,可用于不同plexin和共受体之间的串扰,从而实现细胞信号传导的微调。

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