AUTHOR=Immisch Lena , Papafotiou George , Gallarín Delgado Nerea , Scheuplein Vivian , Paschen Annette , Blankenstein Thomas , Willimsky Gerald 

TITLE=Targeting the recurrent Rac1P29S neoepitope in melanoma with heterologous high-affinity T cell receptors

JOURNAL=Frontiers in Immunology

VOLUME=14

YEAR=2023

URL=https://www.frontiersin.org/journals/immunology/articles/10.3389/fimmu.2023.1119498

DOI=10.3389/fimmu.2023.1119498

ISSN=1664-3224

ABSTRACT=<p>Recurrent neoepitopes are cancer-specific antigens common among groups of patients and therefore ideal targets for adoptive T cell therapy. The neoepitope F<bold>S</bold>GEYIPTV carries the Rac1P29S amino acid change caused by a c.85C&gt;T missense mutation, which is the third most common hotspot mutation in melanoma. Here, we isolated and characterized TCRs to target this HLA-A*02:01-binding neoepitope by adoptive T cell therapy. Peptide immunization elicited immune responses in transgenic mice expressing a diverse human TCR repertoire restricted to HLA-A*02:01, which enabled isolation of high-affinity TCRs. TCR-transduced T cells induced cytotoxicity against Rac1P29S expressing melanoma cells and we observed regression of Rac1P29S expressing tumors <italic>in vivo</italic> after adoptive T cell therapy (ATT). Here we found that a TCR raised against a heterologous mutation with higher peptide-MHC affinity (Rac2P29L) more efficiently targeted the common melanoma mutation Rac1P29S. Overall, our study provides evidence for the therapeutic potential of Rac1P29S-specific TCR-transduced T cells and reveal a novel strategy by generating more efficient TCRs by heterologous peptides.</p>