Immunopeptidomics of colorectal cancer organoids reveals a sparse HLA class I neoantigen landscape and no increase in neoantigens with interferon or MEK-inhibitor treatment.
Alice NeweyBeatrice GriffithsJustine MichauxHui Song PakBrian J StevensonAndrew WoolstonMaria SemiannikovaGeorgia SpainLouise J BarberNik MatthewsSheela RaoDavid WatkinsIan ChauGeorge CoukosJulien RacleDavid GfellerNaureen StarlingDavid CunninghamMichal Bassani-SternbergMarco GerlingerPublished in: Journal for immunotherapy of cancer (2019)
Only 3 out of 612 non-silent mutations encoded for neoantigens that were detectable by MS. Although MS has sensitivity limits and biases, and likely underestimated the true neoantigen burden, this established a lower bound of the percentage of non-silent mutations that encode for presented neoantigens, which may be as low as 0.5%. This could be a reason for the poor responses of non-hypermutated CRCs to immune checkpoint inhibitors. MEK-inhibitors recently failed to improve checkpoint-inhibitor efficacy in CRC and the observed lack of HLA upregulation or improved peptide presentation may explain this.