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首页> 外文期刊>Developmental cell >GPI-Anchored Proteins Are Delivered to Recycling Endosomes via a Distinct cdc42-Regulated, Clathrin-Independent Pinocytic Pathway
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GPI-Anchored Proteins Are Delivered to Recycling Endosomes via a Distinct cdc42-Regulated, Clathrin-Independent Pinocytic Pathway

机译:GPI锚定的蛋白质通过一个独特的cdc42调控,网格蛋白独立的胞浆途径传递至回收内体。

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摘要

Endocytosis of cell-surface proteins via specific pathways is critical for their function. We show that multiple glycosylphosphatidylinositol-anchored proteins (GPI-APs) are endocytosed to the recycling endosomal compartment but not to the Golgi via a nonclathrin, noncaveolae mediated pathway. GPI anchoring is a positive signal for internalization into rab5-independent tubular-vesicular endosomes also responsible for a major fraction of fluid-phase uptake; molecules merely lacking cytoplasmic extensions are not included. Unlike the cytoplasmic extensions are not included. Unlike the internalization of detergent-resistant membrane (DRM)-associated interleukin 2 receptor, endocytosis of DRM-associated GPI-APs is unaffected by inhibition of RhoA or dynamin 2 activity. Inhibition of Rho family GTPase cdc42, but not Rac1, reduces fluid-phase uptake and redistributes GPI-APs to the clathrin-mediated pathway. These results describe a distinct constitutive pinocytic pathway, specifically regulated by cdc42.
机译:通过特定途径对细胞表面蛋白的内吞作用对其功能至关重要。我们显示,多个糖基磷脂酰肌醇锚定的蛋白(GPI-APs)被内吞到回收的内体隔室,而不是通过非clathrin,noncaveolae介导的途径到达高尔基体。 GPI锚定是内化到不依赖rab5的管状囊泡内体中的积极信号,这些内体也负责大部分的液相吸收。不包括仅缺乏胞质延伸的分子。与之不同的是,不包括胞质延伸。与耐去污剂膜(DRM)相关的白介素2受体的内在化不同,DRM相关的GPI-AP的内吞作用不受RhoA或dynamin 2活性的抑制。抑制Rho家族GTPase cdc42,而不抑制Rac1,可减少液相吸收并将GPI-AP重新分布到网格蛋白介导的途径。这些结果描述了独特的组成型胞吞途径,特别是由cdc42调节。

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