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Targeting of cancer neoantigens with donor-derived T cell receptor repertoires.

Erlend Strønen ,
Mireille Toebes ,
Sander Kelderman ,
Marit M van Buuren ,
Weiwen Yang ,
Nienke van Rooij ,
Marco Donia ,
Maxi-Lu Böschen ,
Fridtjof Lund-Johansen ,
Johanna Olweus ,
Ton N Schumacher

Abstract

Accumulating evidence suggests that clinically efficacious cancer immunotherapies are driven by T cell reactivity against DNA mutation-derived neoantigens. However, among the large number of predicted neoantigens, only a minority is recognized by autologous patient T cells, and strategies to broaden neoantigen-specific T cell responses are therefore attractive. We found that naïve T cell repertoires of healthy blood donors provide a source of neoantigen-specific T cells, responding to 11 of 57 predicted human leukocyte antigen (HLA)-A*02:01-binding epitopes from three patients. Many of the T cell reactivities involved epitopes that in vivo were neglected by patient autologous tumor-infiltrating lymphocytes. Finally, T cells redirected with T cell receptors identified from donor-derived T cells efficiently recognized patient-derived melanoma cells harboring the relevant mutations, providing a rationale for the use of such "outsourced" immune responses in cancer immunotherapy.

More about this publication

Science (New York, N.Y.)

Volume 352
Issue nr. 6291
Pages 1337-41
Publication date 10-06-2016

Full text links

Publisher website (DOI) 10.1126/science.aaf2288
Europe PubMed Central 27198675
Pubmed 27198675

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