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Publication : Calsyntenin-1 shelters APP from proteolytic processing during anterograde axonal transport.

First Author  Steuble M Year  2012
Journal  Biol Open Volume  1
Issue  8 Pages  761-74
PubMed ID  23213470 Mgi Jnum  J:186387
Mgi Id  MGI:5432260 Doi  10.1242/bio.20121578
Citation  Steuble M, et al. (2012) Calsyntenin-1 shelters APP from proteolytic processing during anterograde axonal transport. Biol Open 1(8):761-74
abstractText  Endocytosis of amyloid-beta precursor protein (APP) is thought to represent the major source of substrate for the production of the amyloidogenic Abeta peptide by the beta-secretase BACE1. The irreversible nature of proteolytic cleavage implies the existence of an efficient replenishment route for APP from its sites of synthesis to the cell surface. We recently found that APP exits the trans-Golgi network in intimate association with calsyntenin-1, a transmembrane cargo-docking protein for Kinesin-1-mediated vesicular transport. Here we characterized the function of calsyntenin-1 in neuronal APP transport using selective immunoisolation of intracellular trafficking organelles, immunocytochemistry, live-imaging, and RNAi. We found that APP is co-transported with calsyntenin-1 along axons to early endosomes in the central region of growth cones in carriers that exclude the alpha-secretase ADAM10. Intriguingly, calsyntenin-1/APP organelles contained BACE1, suggesting premature cleavage of APP along its anterograde path. However, we found that APP contained in calsyntenin-1/APP organelles was stable. We further analyzed vesicular trafficking of APP in cultured hippocampal neurons, in which calsyntenin-1 was reduced by RNAi. We found a markedly increased co-localization of APP and ADAM10 in axons and growth cones, along with increased proteolytic processing of APP and Abeta secretion in these neurons. This suggested that the reduced capacity for calsyntenin-1-dependent APP transport resulted in mis-sorting of APP into additional axonal carriers and, therefore, the premature encounter of unprotected APP with its ectodomain proteases. In combination, our results characterize calsyntenin-1/APP organelles as carriers for sheltered anterograde axonal transport of APP.
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