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Structural Basis for Plexin Activation and Regulation

机译:Plexin激活和调节的结构基础

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Class A plexins (PlxnAs) act as semaphorin receptors and control diverse aspects of nervous system development and plasticity, ranging from axon guidance and neuron migration to synaptic organization. PlxnA signaling requires cytoplasmic domain dimerization, but extracellular regulation and activation mechanisms remain unclear. Here we present crystal structures of PlxnA (PlxnA1, PlxnA2, and PlxnA4) full ectodomains. Domains 1-9 form a ring-like conformation from which the C-terminal domain 10 points away. All our PlxnA ectodomain structures show autoinhibitory, intermolecular "head-to-stalk" (domain 1 to domain 4-5) interactions, which are confirmed by biophysical assays, live cell fluorescence microscopy, and cell-based and neuronal growth cone collapse assays. This work reveals a 2-fold role of the PlxnA ectodomains: imposing a pre-signaling autoinhibitory separation for the cytoplasmic domains via intermolecular head-to-stalk interactions and supporting dimerization-based PlxnA activation upon ligand binding. More generally, our data identify a novel molecular mechanism for preventing premature activation of axon guidance receptors.
机译:A类丛蛋白(PlxnAs)充当信号量受体,并控制神经系统发育和可塑性的各个方面,从轴突指导和神经元迁移到突触组织。 PlxnA信号需要胞质域二聚化,但细胞外调节和激活机制仍不清楚。在这里,我们介绍PlxnA(PlxnA1,PlxnA2和PlxnA4)完整胞外域的晶体结构。结构域1-9形成环状构象,C末端结构域10从该环状构象指向。我们所有的PlxnA胞外域结构都表现出自抑制性分子间“头对茎”(域1到域4-5)相互作用,这已通过生物物理测定,活细胞荧光显微镜以及基于细胞和神经元的生长锥塌陷测定得到证实。这项工作揭示了PlxnA胞外域的2倍作用:通过分子间头与茎之间的相互作用对细胞质域施加信号传导前的自动抑制分离,并在配体结合后支持基于二聚化的PlxnA活化。更普遍地,我们的数据确定了一种防止轴突引导受体过早活化的新型分子机制。

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