Systematic discovery of neoepitope–HLA pairs for neoantigens shared among patients and tumor types

Author:

Gurung Hem R.ORCID,Heidersbach Amy J.,Darwish Martine,Chan Pamela Pui Fung,Li Jenny,Beresini Maureen,Zill Oliver A.ORCID,Wallace Andrew,Tong Ann-Jay,Hascall Dan,Torres Eric,Chang Andy,Lou Kenny ‘Hei-Wai’,Abdolazimi Yassan,Hammer Christian,Xavier-Magalhães Ana,Marcu AnaORCID,Vaidya Samir,Le Daniel D.,Akhmetzyanova Ilseyar,Oh Soyoung A.,Moore Amanda J.,Uche Uzodinma N.ORCID,Laur Melanie B.ORCID,Notturno Richard J.,Ebert Peter J. R.,Blanchette CraigORCID,Haley BenjaminORCID,Rose Christopher M.ORCID

Abstract

AbstractThe broad application of precision cancer immunotherapies is limited by the number of validated neoepitopes that are common among patients or tumor types. To expand the known repertoire of shared neoantigen–human leukocyte antigen (HLA) complexes, we developed a high-throughput platform that coupled an in vitro peptide–HLA binding assay with engineered cellular models expressing individual HLA alleles in combination with a concatenated transgene harboring 47 common cancer neoantigens. From more than 24,000 possible neoepitope–HLA combinations, biochemical and computational assessment yielded 844 unique candidates, of which 86 were verified after immunoprecipitation mass spectrometry analyses of engineered, monoallelic cell lines. To evaluate the potential for immunogenicity, we identified T cell receptors that recognized select neoepitope–HLA pairs and elicited a response after introduction into human T cells. These cellular systems and our data on therapeutically relevant neoepitopes in their HLA contexts will aid researchers studying antigen processing as well as neoepitope targeting therapies.

Publisher

Springer Science and Business Media LLC

Subject

Biomedical Engineering,Molecular Medicine,Applied Microbiology and Biotechnology,Bioengineering,Biotechnology

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