Centre for Mechanochemical Cell Biology, Warwick Medical School, Coventry, UK.
Wellcome Trust Centre for Cell-Matrix Research, Faculty of Biology, Medicine and Health, University of Manchester, Manchester Academic Health Science Centre, Manchester, UK.
J Cell Biol. 2021 Oct 4;220(10). doi: 10.1083/jcb.202009028. Epub 2021 Jul 21.
Membrane traffic is an important regulator of cell migration through the endocytosis and recycling of cell surface receptors such as integrin heterodimers. Intracellular nanovesicles (INVs) are transport vesicles that are involved in multiple membrane trafficking steps, including the recycling pathway. The only known marker for INVs is tumor protein D54 (TPD54/TPD52L2), a member of the TPD52-like protein family. Overexpression of TPD52-like family proteins in cancer has been linked to poor prognosis and an aggressive metastatic phenotype, which suggests cell migration may be altered under these conditions. Here, we show that TPD54 directly binds membrane and associates with INVs via a conserved positively charged motif in its C terminus. We describe how other TPD52-like proteins are also associated with INVs, and we document the Rab GTPase complement of all INVs. Depletion of TPD52-like proteins inhibits cell migration and invasion, while their overexpression boosts motility. We show that inhibition of migration is likely due to altered recycling of α5β1 integrins in INVs.
膜运输是细胞迁移的重要调节剂,通过细胞表面受体(如整合素异二聚体)的内吞作用和再循环来实现。细胞内纳米囊泡(INV)是参与多个膜运输步骤的运输囊泡,包括再循环途径。INV 的唯一已知标志物是肿瘤蛋白 D54(TPD54/TPD52L2),它是 TPD52 样蛋白家族的成员。癌症中 TPD52 样家族蛋白的过表达与不良预后和侵袭性转移表型有关,这表明在这些条件下细胞迁移可能会发生改变。在这里,我们表明 TPD54 通过其 C 端保守的正电荷基序直接结合膜并与 INV 相关联。我们描述了其他 TPD52 样蛋白如何与 INV 相关联,并记录了所有 INV 的 Rab GTPase 成分。TPD52 样蛋白的耗竭抑制细胞迁移和侵袭,而其过表达则增强迁移能力。我们表明,迁移的抑制可能是由于 INV 中 α5β1 整合素的再循环发生改变所致。
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