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ALIX- and ESCRT-III–dependent sorting of tetraspanins to exosomes

机译:Alix-和Escrt-III依赖于四胞苷的四分色排序

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The intraluminal vesicles (ILVs) of endosomes mediate the delivery of activated signaling receptors and other proteins to lysosomes for degradation, but they also modulate intercellular communication when secreted as exosomes. The formation of ILVs requires four complexes, ESCRT-0, -I, -II, and -III, with ESCRT-0, -I, and -II presumably involved in cargo sorting and ESCRT-III in membrane deformation and fission. Here, we report that an active form of the ESCRT-associated protein ALIX efficiently recruits ESCRT-III proteins to endosomes. This recruitment occurs independently of other ESCRTs but requires lysobisphosphatidic acid (LBPA) in vivo, and can be reconstituted on supported bilayers in vitro. Our data indicate that this ALIX- and ESCRT-III–dependent pathway promotes the sorting and delivery of tetraspanins to exosomes. We conclude that ALIX provides an additional pathway of ILV formation, secondary to the canonical pathway, and that this pathway controls the targeting of exosomal proteins.
机译:胚乳的腔内囊泡(ILV)介导活化的信号受体和其他蛋白质的递送至溶酶体以进行降解,但它们也在分泌作为外泌体分泌时调节细胞间通信。 ILV的形成需要四个配合物,ESCRT-0,-I,-II,以及-III,与ESCRT-0,-I,-II,以及膜变形和裂变中的货物分选和ESCRT-III。在此,我们报告了ESCRT相关蛋白ALIX的活性形式,有效地促进ESCRT-III蛋白到内体。该募集性地发生独立于其他ESCRTS,但需要体内羟二磷脂酸(LBPA),并且可以在体外重构在负载的双层上。我们的数据表明,该依赖性依赖性途径促进了四苯胺的分选和递送给外泌体。我们得出结论,Alix提供额外的ILV形成途径,仲裁途径,并且该途径控制外泌体蛋白的靶向。

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