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The adaptor protein Grb2 regulates cell surface Fas ligand in Schwann cells |
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| Authors: | Thornhill Peter B Cohn Jason B Stanford William L Desbarats Julie |
| Institution: | a Department of Physiology, McGill University, 3655 Promenade Sir William Osler, Montréal, Que., Canada H3G 1Y6 b Samuel Lunenfeld Research Institute, Mount Sinai Hospital, 600 University Avenue, Toronto, Ont., Canada M5G 1X5 c Department of Molecular Genetics, University of Toronto, Toronto, Ont., Canada M5S 1A8 d Institute for Biomaterials and Biomedical Engineering, University of Toronto, 164 College Street, Toronto, Ont., Canada M5S 3G99 |
| Abstract: | Fas Ligand (FasL, CD178) is a cytokine that may be secreted or expressed as a transmembrane ligand at the cell surface, and induces apoptosis by binding to the “death receptor” Fas (CD95). Here, we show that Grb2, an SH3 domain-containing adaptor protein, binds to the proline-rich domain of FasL and regulates its cell surface expression. We found that knocking down Grb2 expression decreased the amount of FasL at the cell surface and increased the abundance of intracellular vesicles containing FasL. Furthermore, we showed that Grb2 acts as an adaptor for FasL to interact with adaptin β, a molecule known to regulate trafficking. Our data reveal that Grb2 facilitates the association of FasL with adaptinβ, and promotes sorting of FasL to the cell surface. As FasL is a potent regulator of cell death, dynamic regulation of its cell surface localization is critical for controlling local tissue remodeling and inflammation. |
| Keywords: | Fas Ligand (CD178) Fas (CD95) Src homology 3 domain Grb2 Sorting nexin 18 Adaptin β Schwann cell Trafficking Subcellular localization Apoptosis |
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