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首页> 外文期刊>Cell >Structural Basis of Semaphorin-Plexin Recognition and Viral Mimicry from Sema7A and A39R Complexes with PlexinC1
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Structural Basis of Semaphorin-Plexin Recognition and Viral Mimicry from Sema7A and A39R Complexes with PlexinC1

机译:Semaphorin-Plexin识别和Sema7A和A39R与PlexinC1配合物的病毒拟态的结构基础。

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摘要

Repulsive signaling by Semaphorins and Plexins is crucial for the development and homeostasis of the nervous, immune, and cardiovascular systems. Sema7A acts as both an immune and a neural Semaphorin through PlexinC1, and A39R is a Sema7A mimic secreted by smallpox virus. We report the structures of Sema7A and A39R complexed with the Semaphorin-binding module of PlexinC1. Both structures show two PlexinC1 molecules symmetrically bridged by Semaphorin dimers, in which the Semaphorin and PlexinC1 β propellers interact in an edge-on, orthogonal orientation. Both binding interfaces are dominated by the insertion of the Semaphorin's 4c-4d loop into a deep groove in blade 3 of the PlexinC1 propeller. A39R appears to achieve Sema7A mimicry by preserving key Plexin-binding determinants seen in the mammalian Sema7A complex that have evolved to achieve higher affinity binding to the host-derived PlexinC1. The complex structures support a conserved Semaphorin-Plexin recognition mode and suggest that Plexins are activated by dimerization.
机译:Semaphorins和Plexins的排斥信号对于神经,免疫和心血管系统的发育和体内平衡至关重要。 Sema7A通过PlexinC1同时充当免疫和神经Semaphorin,而A39R是天花病毒分泌的Sema7A模拟物。我们报告了Sema7A和A39R的结构与PlexinC1的Semaphorin结合模块复合。两种结构都显示了两个由Semaphorin二聚体对称桥接的PlexinC1分子,其中Semaphorin和PlexinC1β螺旋桨以边沿正交的方向相互作用。这两个绑定界面的主要作用是将Semaphorin的4c-4d环插入PlexinC1螺旋桨叶片3的深槽中。 A39R似乎通过保留在哺乳动物Sema7A复合物中观察到的关键Plexin结合决定簇来实现Sema7A模仿,这些决定簇已进化为实现与宿主衍生的PlexinC1的更高亲和力结合。复杂的结构支持保守的Semaphorin-Plexin识别模式,并表明Plexins被二聚化激活。

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