SUBCELLULAR ROUTING OF SORTILIN AND SORLA
Center for Molecular Neurobiology Hamburg, University Medical Center Hamburg-Eppendorf
Presentation
Date TBA
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Poster Board
PS05-09AM-240
Poster
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The functions of monomeric forms of both receptors have been extensively studied, whereas much less is known about their dimerization. Homodimerization of Sortilin and SorLA is thought to modulate the receptor function, such as ligand-binding. Biophysical evidence support that Sortilin dimerizes via its ectodomain in acidic intracellular compartments, although this has not yet been conclusively demonstrated in cells under physiological conditions. In contrast dimerization of SorLA remains less well understood, as specific domains and subcellular sites mediating dimerization have not been fully described.
Having established biological tools for visualization and detailed analysis of dimerization, we employ protein interaction assays and imaging approaches to validate homodimerization of both receptors under physiological conditions. Studying the trafficking of monomeric and dimeric Sortilin and SorLA, we aim to gain mechanistic insights of receptor function in the context of AD.
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