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Prediction of neo-epitope immunogenicity reveals TCR recognition determinants and provides insight into immunoediting.

Schmidt, J.
Smith, A.R.
Magnin, M.
Racle, J.
Devlin, J.R.
Bobisse, S.
Cesbron, J.
Bonnet, V.
Carmona, S.J.
Huber, F.
Ciriello, G.
Speiser, D.E.
Bassani-Sternberg, M.
Coukos, G.
Baker, B.M.
Harari, A.
Gfeller, D.

Publication date

February 2021

DOI

10.1016/j.xcrm.2021.100194

Language

English

Abstract

CD8+ T cell recognition of peptide epitopes plays a central role in immune responses against pathogens and tumors. However, the rules that govern which peptides are truly recognized by existing T cell receptors (TCRs) remain poorly understood, precluding accurate predictions of neo-epitopes for cancer immunotherapy. Here, we capitalize on recent (neo-)epitope data to train a predictor of immunogenic epitopes (PRIME), which captures molecular properties of both antigen presentation and TCR recognition. PRIME not only improves prioritization of neo-epitopes but also correlates with T cell potency and unravels biophysical determinants of TCR recognition that we experimentally validate. Analysis of cancer genomics data reveals that recurrent mu...

Extracted data

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Schmidt, J.
Croce, G.
Guillaume, P.
Bobisse, S.
Genolet, R.
Queiroz, L.
Cesbron, J.
Racle, J.
Harari, A.

January 2023

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