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神经钙黏蛋白在电路连接中的功能的结构基础:突触处的毒素基序。

Structural Basis for Teneurin Function in Circuit-Wiring: A Toxin Motif at the Synapse.

机构信息

Department of Biochemistry and Molecular Biology, The University of Chicago, Chicago, IL 60637, USA; Grossman Institute for Neuroscience, Quantitative Biology and Human Behavior, The University of Chicago, Chicago, IL 60637, USA.

Department of Molecular and Cellular Physiology, Stanford University, Stanford, CA 94305, USA; Department of Structural Biology, Stanford University, Stanford, CA 94305, USA.

出版信息

Cell. 2018 Apr 19;173(3):735-748.e15. doi: 10.1016/j.cell.2018.03.036.

Abstract

Teneurins (TENs) are cell-surface adhesion proteins with critical roles in tissue development and axon guidance. Here, we report the 3.1-Å cryoelectron microscopy structure of the human TEN2 extracellular region (ECR), revealing a striking similarity to bacterial Tc-toxins. The ECR includes a large β barrel that partially encapsulates a C-terminal domain, which emerges to the solvent through an opening in the mid-barrel region. An immunoglobulin (Ig)-like domain seals the bottom of the barrel while a β propeller is attached in a perpendicular orientation. We further show that an alternatively spliced region within the β propeller acts as a switch to regulate trans-cellular adhesion of TEN2 to latrophilin (LPHN), a transmembrane receptor known to mediate critical functions in the central nervous system. One splice variant activates trans-cellular signaling in a LPHN-dependent manner, whereas the other induces inhibitory postsynaptic differentiation. These results highlight the unusual structural organization of TENs giving rise to their multifarious functions.

摘要

腱糖蛋白(Teneurins,TENs)是细胞表面黏附蛋白,在组织发育和轴突导向中具有关键作用。在这里,我们报道了人腱糖蛋白 2 细胞外区(extracellular region,ECR)的 3.1Å 冷冻电镜结构,该结构与细菌 Tc 毒素具有惊人的相似性。ECR 包含一个大的β桶,部分包裹着一个 C 末端结构域,该结构域通过β桶中间区域的一个开口暴露在溶剂中。一个免疫球蛋白(immunoglobulin,Ig)样结构域封闭了桶的底部,而一个β推进器则以垂直的方向附着。我们进一步表明,β推进器内的一个选择性剪接区域充当开关,调节 TEN2 与跨细胞黏附素(latrophilin,LPHN)的细胞间黏附,LPHN 是一种已知在中枢神经系统中介导关键功能的跨膜受体。一种剪接变体以 LPHN 依赖的方式激活跨细胞信号,而另一种则诱导抑制性突触后分化。这些结果突出了 TENs 的异常结构组织,导致其具有多种功能。

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