Presence of T cells directed against CD20-derived peptides in healthy individuals and lymphoma patients

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Milcent, Benoit | Josseaume, Nathalie | Riller, Quentin | Giglioli, Ilenia | Rabia, Emilia | Deligne, Claire | Latouche, Jean-Baptiste | Hamieh, Mohamad | Couture, Alexandre | Toutirais, Olivier | Lone, Yu-Chun | Jeger-Madiot, Raphaël | Graff-Dubois, Stéphanie | Amorim, Sandy | Loiseau, Pascale | Toubert, Antoine | Brice, Pauline | Thieblemont, Catherine | Teillaud, Jean-Luc | Sibéril, Sophie

Edité par CCSD ; Springer Verlag -

International audience. Preclinical and clinical studies have suggested that cancer treatment with antitumor antibodies induces a specific adaptive T cell response. A central role in this process has been attributed to CD4+ T cells, but the relevant T cell epitopes, mostly derived from non-mutated self-antigens, are largely unknown. In this study, we have characterized human CD20-derived epitopes restricted by HLA-DR1, HLA-DR3, HLA-DR4, and HLA-DR7, and investigated whether T cell responses directed against CD20-derived peptides can be elicited in human HLA-DR-transgenic mice and human samples. Based on in vitro binding assays to recombinant human MHC II molecules and on in vivo immunization assays in H-2 KO/HLA-A2+-DR1+ transgenic mice, we have identified 21 MHC II-restricted long peptides derived from intracellular, membrane, or extracellular domains of the human non-mutated CD20 protein that trigger in vitro IFN-γ production by PBMCs and splenocytes from healthy individuals and by PBMCs from follicular lymphoma patients. These CD20-derived MHC II-restricted peptides could serve as a therapeutic tool for improving and/or monitoring anti-CD20 T cell activity in patients treated with rituximab or other anti-CD20 antibodies.

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