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PAQR3 Regulates Endoplasmic Reticulum-to-Golgi Trafficking of COPII Vesicle via Interaction with Sec13/Sec31 Coat Proteins

机译:PAQR3通过与SEC13 / SEC31涂层蛋白的相互作用调节成分网状囊泡的内质网 - 高尔基贩运Copii囊泡

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Summary: Endoplasmic reticulum (ER)-to-Golgi anterograde transport is driven by COPII vesicles mainly composed of a Sec23/Sec24 inner shell and a Sec13/Sec31 outer cage. How COPII vesicles are tethered to the Golgi is not completely understood. We demonstrated here that PAQR3 can facilitate tethering of COPII vesicles to the Golgi. Proximity labeling using PAQR3 fused with APEX2 identified that many proteins involved in intracellular transport are in close proximity to PAQR3. ER-to-Golgi trafficking of N-acetylgalactosaminyltransferase-2 on removal of brefeldin A is delayed by PAQR3 deletion. RUSH assay also revealed that ER-to-Golgi trafficking is affected by PAQR3. The N-terminal end of PAQR3 can interact with the WD domains of Sec13 and Sec31A. PAQR3 enhances Golgi localization of Sec13 and Sec31A. Furthermore, PAQR3 is localized in the ERGIC and cis-Golgi structures, the acceptor sites for COPII vesicles. Taken together, our study uncovers a role for PAQR3 as a player in regulating ER-to-Golgi transport of COPII vesicles. : Molecular Biology Experimental Approach; Cell Biology; Functional Aspects of Cell Biology Subject Areas: Molecular Biology Experimental Approach, Cell Biology, Functional Aspects of Cell Biology
机译:发明内容:内质网(ER)-To-Golgi antograde传送由Copii囊泡驱动,主要由SEC23 / SEC24内壳和SEC13 / SEC31外笼组成。 Copii囊泡是如何完全理解到高尔基的。我们在此证明,PAQR3可以促进Copii囊泡的束缚到Golgi。使用与Apex2融合的PAQR3的接近标记鉴定出与细胞内传输中涉及的许多蛋白质紧密到PAQR3。通过PAQR3缺失延迟了在去除Brefeldin A时对N-乙酰卤酰氨基甲酰氨基转移酶-2的ER-to-golgi贩运。 Rush Assay还透露,ER-To-Golgi贩运受PAQR3的影响。 PAQR3的N末端端可以与SEC13和SEC31A的WD域相互作用。 PAQR3增强了SEC13和SEC31A的GOLGI定位。此外,PAQR3在ERGIC和CIS-GOLGI结构中定位,COPII囊泡的受体位点。我们的研究携带,我们的研究揭示了PAQR3作为调节COPII囊泡的ER-GOLGI运输的球员的作用。 :分子生物学实验方法;细胞生物学;细胞生物学对象领域的功能方面:分子生物学实验方法,细胞生物学,细胞生物学功能方面

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