Literature DB >> 19497983

CD82 endocytosis and cholesterol-dependent reorganization of tetraspanin webs and lipid rafts.

Congfeng Xu1, Yanhui H Zhang, Muthusamy Thangavel, Mekel M Richardson, Li Liu, Bin Zhou, Yi Zheng, Rennolds S Ostrom, Xin A Zhang.   

Abstract

Tetraspanin CD82 suppresses cell migration, tumor invasion, and tumor metastasis. To determine the mechanism by which CD82 inhibits motility, most studies have focused on the cell surface CD82, which forms tetraspanin-enriched microdomains (TEMs) with other transmembrane proteins, such as integrins. In this study, we found that CD82 undergoes endocytosis and traffics to endosomes and lysosomes. To determine the endocytic mechanism of CD82, we demonstrated that dynamin and clathrin are not essential for CD82 internalization. Depletion or sequestration of sterol in the plasma membrane markedly inhibited the endocytosis of CD82. Despite the demand on Cdc42 activity, CD82 endocytosis is distinct from macropinocytosis and the documented dynamin-independent pinocytosis. As a TEM component, CD82 reorganizes TEMs and lipid rafts by redistributing cholesterol into these membrane microdomains. CD82-containing TEMs are characterized by the cholesterol-containing microdomains in the extreme light- and intermediate-density fractions. Moreover, the endocytosis of CD82 appears to alleviate CD82-mediated inhibition of cell migration. Taken together, our studies demonstrate that lipid-dependent endocytosis drives CD82 trafficking to late endosomes and lysosomes, and CD82 reorganizes TEMs and lipid rafts through redistribution of cholesterol.

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Year:  2009        PMID: 19497983      PMCID: PMC2747672          DOI: 10.1096/fj.08-123414

Source DB:  PubMed          Journal:  FASEB J        ISSN: 0892-6638            Impact factor:   5.191


  78 in total

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Authors:  Matthew Kirkham; Robert G Parton
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7.  CD82 restrains pathological angiogenesis by altering lipid raft clustering and CD44 trafficking in endothelial cells.

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8.  The regulation of cancer cell migration by lung cancer cell-derived exosomes through TGF-β and IL-10.

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Review 10.  Laminin-binding integrins and their tetraspanin partners as potential antimetastatic targets.

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