| Article ID | Journal | Published Year | Pages | File Type |
|---|---|---|---|---|
| 9137532 | Blood Cells, Molecules, and Diseases | 2005 | 5 Pages |
Abstract
Dendritic-cell-derived exosomes (DEX) secreted after dendritic cell loading with tumor peptides were found to mediate tumor rejection in mice. This observation prompted us to demonstrate that MHC class I/peptide complexes harbored onto exosomal membranes were capable of priming cytotoxic T cells and to mediate rejection of tumors expressing the relevant antigens. Moreover, DEX also promote NK cell activation in immunocompetent mice and NK cell-dependent antitumor effects. The first Phase I trial using DEX to immunize melanoma patients revealed the feasibility of DEX production in stage IV melanoma, their safety in long-term follow up and their bioactivity in vivo.
Keywords
TEXCross presentationDEXCTLMVBAPCHspASIGMPFDCHuman leukocyte antigenAntigen presenting cellsHLAExosomesimmunotherapyactive specific immunotherapymultivesicular bodyTumorDendritic cellsFollicular dendritic cellsMonocyte-derived dendritic cellsCytotoxic T lymphocytesMHCmajor histocompatibility complexHeat shock protein
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Authors
Nathalie Chaput, Julien Taïeb, Noël Schartz, Caroline Flament, Sophie Novault, Fabrice André, Laurence Zitvogel,