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The Structure of the Sec13/31 COPII Cage Bound to Sec23

机译:该sec13 / 31 COpII笼绑定到sec23结构

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摘要

Structural studies have revealed some of the organizing principles and mechanisms involved in the assembly of the COPII coat including the location of the Sec23/24 adapter layer. Previous studies, however, were unable to unambiguously determine the positions of Sec23 and Sec24 in the coat. Here we have determined a cryogenic electron microscopic structure of Sec13/31 together with Sec23. Electron tomography revealed that the binding of Sec23 induces Sec13/31 to form a variety of different geometries including a cuboctahedron, as was previously characterized for Sec13/31 alone. Single particle reconstruction of the Sec13/31-23 cuboctahedra revealed that the binding of Sec23 induces a conformational change in Sec13/31 resulting in a more extended conformation. Docking Sec23 crystal structures into the EM map suggested that Sec24 projects its cargo binding surface out into the large open faces of the coat. These results have implications for the mechanisms by which COPII transports large cargos, cargos with large intracellular domains, and for tethering complexes that must project out of the coat in order to interact with their binding partners. Furthermore, Sec23 binds Sec13/31 at two unique sites in the coat, which suggests that each site may have unique roles in the mechanisms of COPII vesiculation.
机译:结构研究揭示了在Copii涂层组装中涉及的一些组织原则和机制,包括SEC23 / 24适配器层的位置。然而,以前的研究无法毫不含糊地确定涂层中的SEC23和SEC24的位置。在这里,我们已经确定了SEC13 / 31的低温电子显微镜结构与SEC23一起。电子断层扫描显示SEC23的结合诱导SEC13 / 31,形成包括副叶酰二合一的各种不同几何形状,如先前对SEC13 / 31的特征在于SEC13 / 31。 SEC13 / 31-23 Cuboctahedra的单粒子重建揭示了SEC23的结合在SEC13 / 31中诱导构象变化,从而产生更长时间的构象。将Sec23 Crystal Structores进入EM图建议Sec24将其货物装订表面突出到外套的大开关中。这些结果对Copii传输大型尸体的机制具有巨大的细胞内结构域的机制,以及必须从涂层中突出的束缚复合物以与其结合伴侣相互作用。此外,SEC23在涂层中的两个独特位点结合Sec13 / 31,这表明每个位点可能具有独特的作用在Copii混凝土机制中。

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