Publication | Open Access
Signal Transduction in Receptor for Advanced Glycation End Products (RAGE)
115
Citations
50
References
2011
Year
Mdia1-ctrage InteractionGlycobiologyImmunologyCellular PhysiologyMolecular PharmacologySignaling PathwayCell InteractionMetabolic SignalingCell SignalingMolecular SignalingGlycosylationMolecular PhysiologyMolecular NeuroscienceBiochemistryRage-dependent Signal TransductionMolecular PathwayG Protein-coupled ReceptorReceptor (Biochemistry)Diabetes ComplicationsPharmacologyCell BiologySignal TransductionFunctional SelectivityNatural SciencesCellular BiochemistryMedicine
The receptor for advanced glycation end products (RAGE) is a multiligand cell surface macromolecule that plays a central role in the etiology of diabetes complications, inflammation, and neurodegeneration. The cytoplasmic domain of RAGE (C-terminal RAGE; ctRAGE) is critical for RAGE-dependent signal transduction. As the most membrane-proximal event, mDia1 binds to ctRAGE, and it is essential for RAGE ligand-stimulated phosphorylation of AKT and cell proliferation/migration. We show that ctRAGE contains an unusual α-turn that mediates the mDia1-ctRAGE interaction and is required for RAGE-dependent signaling. The results establish a novel mechanism through which an extracellular signal initiated by RAGE ligands regulates RAGE signaling in a manner requiring mDia1.
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