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Retrograde trafficking of β-dystroglycan from the plasma membrane to the nucleus

机译:将β-dystroglycan从质膜逆向运输到细胞核

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摘要

β-Dystroglycan (β-DG) is a transmembrane protein with critical roles in cell adhesion, cytoskeleton remodeling and nuclear architecture. This functional diversity is attributed to the ability of β-DG to target to, and conform specific protein assemblies at the plasma membrane (PM) and nuclear envelope (NE). Although a classical NLS and importin α/β mediated nuclear import pathway has already been described for β-DG, the intracellular trafficking route by which β-DG reaches the nucleus is unknown. In this study, we demonstrated that β-DG undergoes retrograde intracellular trafficking from the PM to the nucleus via the endosome-ER network. Furthermore, we provided evidence indicating that the translocon complex Sec61 mediates the release of β-DG from the ER membrane, making it accessible for importins and nuclear import. Finally, we show that phosphorylation of β-DG at Tyr890 is a key stimulus for β-DG nuclear translocation. Collectively our data describe the retrograde intracellular trafficking route that β-DG follows from PM to the nucleus. This dual role for a cell adhesion receptor permits the cell to functionally connect the PM with the nucleus and represents to our knowledge the first example of a cell adhesion receptor exhibiting retrograde nuclear trafficking and having dual roles in PM and NE.
机译:β-Dystroglycan(β-DG)是一种跨膜蛋白,在细胞粘附,细胞骨架重塑和核结构中起关键作用。这种功能多样性归因于β-DG靶向并符合质膜(PM)和核膜(NE)处的特定蛋白质装配体的能力。尽管已经针对β-DG描述了经典的NLS和importinα/β介导的核输入途径,但β-DG到达细胞核的细胞内运输途径尚不清楚。在这项研究中,我们证明了β-DG通过内体-ER网络经历了从PM到细胞核的逆行细胞内运输。此外,我们提供的证据表明,translocon复合物Sec61介导了β-DG从ER膜的释放,使其可用于importins和核输入。最后,我们表明在Tyr890处β-DG的磷酸化是β-DG核易位的关键刺激。我们的数据共同描述了β-DG从PM到细胞核的逆行细胞内运输途径。细胞粘附受体的这种双重作用使细胞能够将PM与细胞核功能性连接,并且据我们所知,这是细胞粘附受体表现出逆行核运输并在PM和NE中起双重作用的第一个例子。

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