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Abstract
Tetraspanins are clustered in specific microdomains (named tetraspanin-enriched microdomains, or TERM) in the plasma membrane and regulate the functions of associated transmembrane receptors, including integrins and receptor tyrosine kinases. We have identified syntenin-1, a PDZ domain-containing protein, as a new component of TERM and show that syntenin-1 specifically interacts with the tetraspanin CD63. Detailed biochemical and heteronuclear magnetic resonance spectroscopy (NMR) studies have demonstrated that the interaction is mediated by the C-terminal cytoplasmic region of the tetraspanin and the PDZ domains of syntenin-1. Upon interaction, NMR chemical shift perturbations were predominantly localized to residues around the binding pocket of PDZ1, indicating a specific mode of recognition of the cytoplasmic tail of CD63. In addition, the C terminus of syntenin-1 has a stabilizing role in the CD63-syntenin-1 association, as deletion of the last 17 amino acids abolished the interaction. The CD63-syntenin-1 complex is abundant on the plasma membrane, and the elevated expression of the wild-type syntenin-1 slows down constitutive internalization of the tetraspanin. Furthermore, internalization of CD63 was completely blocked in cells expressing a syntenin-1 mutant lacking the first 100 amino acids. Previous results have shown that CD63 is internalized via AP-2-dependent mechanisms. Hence, our data indicate that syntenin-1 can counteract the AP-2-dependent internalization and identify this tandem PDZ protein as a new regulator of endocytosis.
We are very grateful to all our colleagues for their generous gifts of the reagents that were used in this study. We acknowledge HWB-NMR, University of Birmingham, for NMR spectrometer access, and we thank Felican Dancea for useful discussions. The backbone 1H and 15N assignments of the syntenin-1 PDZ12 domain were kindly provided by Tomasz Cierpicki (University of Virginia School of Medicine).
This work was supported by CR UK grants C1322/A2945 and C1322/A5705 (to F.B.), the BBSRC grant 2003:574 (to N.A.H. and F.B.), and grants from the BBSRC (10714) and Wellcome Trust (071684) (to M.O.).