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VAMP8-mediated NOX2 recruitment to endosomes is necessary for antigen release.

Eur J Cell Biol. 2017; 
Dingjan I, Paardekooper LM, Verboogen DRJ, von Mollard GF, Ter Beest M, van den Bogaart G.
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Peptide Synthesis Cells were then washed and incubated with gp100 short (10 ␮M gp100 (residues 280–288); GenScript) or long (100 ␮M gp100 (residues 272–300); JPT) peptide ␮g/ml R-848 and poly(I:C); with T cell receptor stimulation mix (4 Enzo Life Sciences) for 4 h. Get A Quote

摘要

Cross-presentation of foreign antigen in major histocompatibility complex (MHC) class I by dendritic cells (DCs) requires activation of the NADPH-oxidase NOX2 complex. We recently showed that NOX2 is recruited to phagosomes by the SNARE protein VAMP8 where NOX2-produced reactive oxygen species (ROS) cause lipid oxidation and membrane disruption, promoting antigen translocation into the cytosol for cross-presentation. In this study, we extend these findings by showing that VAMP8 is also involved in NOX2 trafficking to endosomes. Moreover, we demonstrate in both human and mouse DCs that absence of VAMP8 leads to decreased ROS production, lipid peroxidation and antigen translocation, and that this impairs cross-pr... More

关键词

Cross-presentation; Dendritic cells; Lipid peroxidation; NOX2; VAMP8