DNMT and HDAC inhibition induces immunogenic neoantigens from human endogenous retroviral element-derived transcripts

Author:

Goyal Ashish,Bauer JensORCID,Hey JoschkaORCID,Papageorgiou Dimitris N.,Stepanova Ekaterina,Daskalakis MichaelORCID,Scheid JonasORCID,Dubbelaar MarissaORCID,Klimovich Boris,Schwarz DominicORCID,Märklin MelanieORCID,Roerden Malte,Lin Yu-Yu,Ma TobiasORCID,Mücke Oliver,Rammensee Hans-Georg,Lübbert MichaelORCID,Loayza-Puch FabricioORCID,Krijgsveld JeroenORCID,Walz Juliane S.ORCID,Plass ChristophORCID

Abstract

AbstractImmunotherapies targeting cancer-specific neoantigens have revolutionized the treatment of cancer patients. Recent evidence suggests that epigenetic therapies synergize with immunotherapies, mediated by the de-repression of endogenous retroviral element (ERV)-encoded promoters, and the initiation of transcription. Here, we use deep RNA sequencing from cancer cell lines treated with DNA methyltransferase inhibitor (DNMTi) and/or Histone deacetylase inhibitor (HDACi), to assemble a de novo transcriptome and identify several thousand ERV-derived, treatment-induced novel polyadenylated transcripts (TINPATs). Using immunopeptidomics, we demonstrate the human leukocyte antigen (HLA) presentation of 45 spectra-validated treatment-induced neopeptides (t-neopeptides) arising from TINPATs. We illustrate the potential of the identified t-neopeptides to elicit a T-cell response to effectively target cancer cells. We further verify the presence of t-neopeptides in AML patient samples after in vivo treatment with the DNMT inhibitor Decitabine. Our findings highlight the potential of ERV-derived neoantigens in epigenetic and immune therapies.

Funder

Deutsche Forschungsgemeinschaft

German-Israeli Helmholtz International Research School Cancer-TRAX (HIRS-0003).

Wilhelm Sander-Stiftung

José Carreras Leukämie-Stiftung

Deutsche Krebshilfe

Bundesministerium für Bildung und Forschung

Zentren für Personalisierte Medizin (ZPM). Fortüne Program of the University of Tübingen

Publisher

Springer Science and Business Media LLC

Subject

General Physics and Astronomy,General Biochemistry, Genetics and Molecular Biology,General Chemistry,Multidisciplinary

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