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Eps15 mediates vesicle trafficking from the trans-Golgi network via an interaction with the clathrin adaptor AP-1

机译:Eps15通过与网格蛋白适配器AP-1的相互作用介导了跨高尔基网络的囊泡运输

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Eps15 (EGFR pathway substrate clone 15) is well known for its role in clathrin-coated vesicle formation at the plasma membrane through interactions with other clathrin adaptor proteins such as AP-2. Interestingly, we observed that in addition to its plasma membrane localization, Eps15 is also present at the trans-Golgi network (TGN). Therefore, we predicted that Eps15 might associate with clathrin adaptor proteins at the TGN and thereby mediate the formation of Golgi-derived vesicles. Indeed, we have found that Eps15 and the TGN clathrin adaptor AP-1 coimmunoprecipitate from rat liver Golgi fractions. Furthermore, we have identified a 14-amino acid motif near the AP-2-binding domain of Eps15 that is required for binding to AP-1, but not AP-2. Disruption of the Eps15-AP-1 interaction via siRNA knockdown of AP-1 or expression of mutant Eps15 protein, which lacks a 14-amino acid motif representing the AP-1 binding site of Eps15, significantly reduced the exit of secretory proteins from the TGN. Together, these findings indicate that Eps15 plays an important role in clathrin-coated vesicle formation not only at the plasma membrane but also at the TGN during the secretory process.
机译:Eps15(EGFR途径底物克隆15)因其通过与其他网格蛋白衔接蛋白(例如AP-2)相互作用而在质膜上形成网格蛋白包被的囊泡而发挥作用。有趣的是,我们观察到,除其质膜定位外,Eps15还存在于反高尔基网络(TGN)中。因此,我们预测Eps15可能与TGN上的网格蛋白衔接蛋白缔合,从而介导高尔基体来源的囊泡的形成。实际上,我们已经发现Eps15和TGN网格蛋白衔接子AP-1从大鼠肝脏高尔基体组分中共免疫沉淀。此外,我们已经发现,在Eps15的AP-2结合域附近有一个14个氨基酸的基序,它是与AP-1(而不是AP-2)结合所必需的。经由AP-1的siRNA敲低或突变的Eps15蛋白的表达中断了Eps15-AP-1相互作用,该蛋白缺少代表Eps15的AP-1结合位点的14个氨基酸的基序,从而显着减少了分泌蛋白从细胞中的退出。 TGN。在一起,这些发现表明,Eps15在网格蛋白涂层的囊泡形成过程中不仅在质膜上而且在分泌过程中在TGN上也起着重要作用。

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