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COPII coat subunit interactions: Sec24p and Sec23p bind to adjacent regions of Sec16p.

机译:COPII外壳亚基相互作用:Sec24p和Sec23p绑定到Sec16p的相邻区域。

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摘要

Formation of COPII-coated vesicles at the endoplasmic reticulum (ER) requires assembly onto the membrane of five cytosolic coat proteins, Sec23p, Sec24p, Sec13p, Sec31p, and Sar1p. A sixth vesicle coat component, Sec16p, is tightly associated with the ER membrane and has been proposed to act as a scaffold for membrane association of the soluble coat proteins. We previously showed that Sec23p binds to the C-terminal region of Sec16p. Here we use two-hybrid and coprecipitation assays to demonstrate that the essential COPII protein Sec24p binds to the central region of Sec16p. In vitro reconstitution of binding with purified recombinant proteins demonstrates that the interaction of Sec24p with the central domain of Sec16p does not depend on the presence of Sec23p. However, Sec23p facilitates binding of Sec24p to Sec16p, and the three proteins can form a ternary complex in vitro. Truncations of Sec24p demonstrate that the N-terminal and C-terminal regions of Sec24p display different binding specificities. The C terminus binds to the central domain of Sec16p, whereas the N terminus of Sec24p binds to both the central domain of Sec16p and to Sec23p. These findings define binding to Sec16p as a new function for Sec24p and support the idea that Sec16p organizes assembly of the COPII coat.
机译:在内质网(ER)上形成COPII涂层的囊泡需要将五种胞浆外壳蛋白Sec23p,Sec24p,Sec13p,Sec31p和Sar1p组装到膜上。第六种囊泡衣壳成分Sec16p与ER膜紧密结合,已被提议充当可溶性外壳蛋白膜结合的支架。我们以前显示Sec23p绑定到Sec16p的C端区域。在这里,我们使用两种杂交和共沉淀测定法来证明必需的COPII蛋白Sec24p结合到Sec16p的中央区域。与纯化的重组蛋白结合的体外重建表明,Sec24p与Sec16p中央结构域的相互作用不取决于Sec23p的存在。但是,Sec23p促进Sec24p与Sec16p的结合,并且这三种蛋白质可以在体外形成三元复合物。 Sec24p的截短表明Sec24p的N端和C端区域显示不同的结合特异性。 C末端与Sec16p的中央域结合,而Sec24p的N末端与Sec16p的中央域和Sec23p结合。这些发现将对Sec16p的绑定定义为Sec24p的新功能,并支持Sec16p组织COPII涂层组装的想法。

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