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聚集诱导α2β1整合素从膜筏侧向重新分布至小窝,并随后发生蛋白激酶C依赖性内化。

Clustering induces a lateral redistribution of alpha 2 beta 1 integrin from membrane rafts to caveolae and subsequent protein kinase C-dependent internalization.

作者信息

Upla Paula, Marjomäki Varpu, Kankaanpää Pasi, Ivaska Johanna, Hyypiä Timo, Van Der Goot F Gisou, Heino Jyrki

机构信息

Cell Biology, University of Jyväskylä, FIN-40351 Jyväskylä, Finland.

出版信息

Mol Biol Cell. 2004 Feb;15(2):625-36. doi: 10.1091/mbc.e03-08-0588. Epub 2003 Dec 2.

Abstract

Integrin alpha 2 beta 1 mediates the binding of several epithelial and mesenchymal cell types to collagen. The composition of the surrounding plasma membrane, especially caveolin-1- and cholesterol-containing membrane structures called caveolae, may be important to integrin signaling. On cell surface alpha 2 beta 1 integrin was located in the raft like membrane domain, rich in GPI-anchored proteins, rather than in caveolae. However, when antibodies were used to generate clusters of alpha 2 beta 1 integrin, they started to move laterally on cell surface along actin filaments. During the lateral movement small clusters fused together. Finally alpha 2 beta 1 integrin was found inside caveolae and subsequently internalized into caveosome-like perinuclear structures. The internalization process, unlike cluster formation or lateral redistribution, was dependent on protein kinase C alpha activity. Caveolae are known to be highly immobile structures and alpha 2 beta 1 integrin clusters represent a previously unknown mechanism to activate endocytic trafficking via caveolae. The process was specific to alpha 2 beta 1 integrin, because the antibody-mediated formation of alpha V integrin clusters activated their internalization in coated vesicles and early endosomes. In addition to natural ligands human echovirus-1 (EV1) gains entry into the cell by binding to alpha 2 beta 1 and taking advantage of alpha 2 beta 1 internalization via caveolae.

摘要

整合素α2β1介导多种上皮细胞和间充质细胞类型与胶原蛋白的结合。周围质膜的组成,特别是富含小窝蛋白-1和胆固醇的膜结构(称为小窝),可能对整合素信号传导很重要。在细胞表面,α2β1整合素位于富含糖基磷脂酰肌醇(GPI)锚定蛋白的筏状膜结构域中,而不是在小窝中。然而,当使用抗体产生α2β1整合素簇时,它们开始沿着肌动蛋白丝在细胞表面横向移动。在横向移动过程中,小簇融合在一起。最终,α2β1整合素在小窝内被发现,随后被内化到类小窝体的核周结构中。与簇形成或横向重新分布不同,内化过程依赖于蛋白激酶Cα的活性。已知小窝是高度固定的结构,α2β1整合素簇代表了一种以前未知的通过小窝激活内吞运输的机制。该过程对α2β1整合素具有特异性,因为抗体介导的αV整合素簇的形成激活了它们在被膜小泡和早期内体中的内化。除了天然配体,人肠道病毒1型(EV1)通过与α2β1结合并利用α2β1通过小窝的内化进入细胞。

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