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- Title
Antigen processing by nardilysin and thimet oligopeptidase generates cytotoxic T cell epitopes.
- Authors
Kessler, Jan H; Khan, Selina; Seifert, Ulrike; Le Gall, Sylvie; Chow, K Martin; Paschen, Annette; Bres-Vloemans, Sandra A; de Ru, Arnoud; van Montfoort, Nadine; Franken, Kees L M C; Benckhuijsen, Willemien E; Brooks, Jill M; van Hall, Thorbald; Ray, Kallol; Mulder, Arend; Doxiadis, Ilias I N; van Swieten, Paul F; Overkleeft, Hermen S; Prat, Annik; Tomkinson, Birgitta; Neefjes, Jacques; Kloetzel, Peter M; Rodgers, David W; Hersh, Louis B; Drijfhout, Jan W; van Veelen, Peter A; Ossendorp, Ferry; Melief, Cornelis J M
- Abstract
Cytotoxic T lymphocytes (CTLs) recognize peptides presented by HLA class I molecules on the cell surface. The C terminus of these CTL epitopes is considered to be produced by the proteasome. Here we demonstrate that the cytosolic endopeptidases nardilysin and thimet oligopeptidase (TOP) complemented proteasome activity. Nardilysin and TOP were required, either together or alone, for the generation of a tumor-specific CTL epitope from PRAME, an immunodominant CTL epitope from Epstein-Barr virus protein EBNA3C, and a clinically important epitope from the melanoma protein MART-1. TOP functioned as C-terminal trimming peptidase in antigen processing, and nardilysin contributed to both the C-terminal and N-terminal generation of CTL epitopes. By broadening the antigenic peptide repertoire, nardilysin and TOP strengthen the immune defense against intracellular pathogens and cancer.
- Publication
Nature immunology, 2011, Vol 12, Issue 1, p45
- ISSN
1529-2916
- Publication type
Journal Article
- DOI
10.1038/ni.1974