Tumor-wide RNA splicing aberrations generate immunogenic public neoantigens

Author:

Kwok Darwin W.ORCID,Stevers Nicholas O.,Nejo Takahide,Chen Lee H.,Etxeberria Inaki,Jung Jangham,Okada Kaori,Cove Maggie Colton,Lakshmanachetty Senthilnath,Gallus Marco,Barpanda Abhilash,Hong Chibo,Chan Gary K.L.,Wu Samuel H.,Ramos Emilio,Yamamichi Akane,Liu Jerry,Watchmaker Payal,Ogino Hirokazu,Saijo Atsuro,Du Aidan,Grishanina Nadia,Woo James,Diaz Aaron,Chang Susan M.,Phillips Joanna J.,Wiita Arun P.ORCID,Klebanoff Christopher A.,Costello Joseph F.,Okada HidehoORCID

Abstract

SummaryT-cell-mediated immunotherapies are limited by the extent to which cancer-specific antigens are homogenously expressed throughout a tumor. We reasoned that recurrent splicing aberrations in cancer represent a potential source of tumor-wide and public neoantigens, and to test this possibility, we developed a novel pipeline for identifying neojunctions expressed uniformly within a tumor across diverse cancer types. Our analyses revealed multiple neojunctions that recur across patients and either exhibited intratumor heterogeneity or, in some cases, were tumor-wide. We identified CD8+ T-cell clones specific for neoantigens derived from tumor-wide and conserved neojunctions inGNASandRPL22, respectively. TCR-engineered CD8+T-cells targeting these mutations conferred neoantigen-specific tumor cell eradication. Furthermore, we revealed that cancer-specific dysregulation in splicing factor expression leads to recurrent neojunction expression. Together, these data reveal that a subset of neojunctions are both intratumorally conserved and public, providing the molecular basis for novel T-cell-based immunotherapies that address intratumoral heterogeneity.

Publisher

Cold Spring Harbor Laboratory

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