Jose Cabezas-Caballero, Anna Huhn, Mikhail A. Kutuzov, Violaine Andre, Alina Shomuradova, P. Anton van der Merwe, Omer Dushek

Abstract

Adoptive T cell therapy using T cells engineered with novel T cell receptors (TCRs) targeting tumorspecific peptides is a promising immunotherapy. However, these TCR-T cells can cross-react with off-target peptides, leading to severe autoimmune toxicities. Current efforts focus on identifying TCRs with reduced cross-reactivity. Here, we show that T cell cross-reactivity can be controlled by the co-signalling molecules CD5, CD8, and CD4, without modifying the TCR.We find the largest reduction in cytotoxic T-cell cross-reactivity by knocking out CD8 and expressing CD4. Cytotoxic T cells engineered with a CD8-to-CD4 co-receptor switch show reduced cross-reactivity to random and positional scanning peptide libraries, as well as to self-peptides, while maintaining their on-target potency. Therefore, co-receptor switching generates super selective T cells that reduce the risk of lethal off-target cross-reactivity, and offers a universal method to enhance the safety of T cell immunotherapies for any TCR.


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