Escape from nonsense-mediated decay associates with anti-tumor immunogenicity

Author:

Litchfield KevinORCID,Reading James L.ORCID,Lim Emilia L.,Xu Hang,Liu PoORCID,Al-Bakir Maise,Wong Yien Ning Sophia,Rowan Andrew,Funt Samuel A.ORCID,Merghoub Taha,Perkins David,Lauss Martin,Svane Inge Marie,Jönsson Göran,Herrero JavierORCID,Larkin James,Quezada Sergio A.ORCID,Hellmann Matthew D.ORCID,Turajlic SamraORCID,Swanton CharlesORCID

Abstract

AbstractFrameshift insertion/deletions (fs-indels) are an infrequent but highly immunogenic mutation subtype. Although fs-indels are degraded through the nonsense-mediated decay (NMD) pathway, we hypothesise that some fs-indels escape degradation and elicit anti-tumor immune responses. Using allele-specific expression analysis, expressed fs-indels are enriched in genomic positions predicted to escape NMD, and associated with higher protein expression, consistent with degradation escape (NMD-escape). Across four independent melanoma cohorts, NMD-escape mutations are significantly associated with clinical-benefit to checkpoint inhibitor (CPI) therapy (Pmeta = 0.0039). NMD-escape mutations are additionally found to associate with clinical-benefit in the low-TMB setting. Furthermore, in an adoptive cell therapy treated melanoma cohort, NMD-escape mutation count is the most significant biomarker associated with clinical-benefit. Analysis of functional T cell reactivity screens from personalized vaccine studies shows direct evidence of fs-indel derived neoantigens eliciting immune response, particularly those with highly elongated neo open reading frames. NMD-escape fs-indels represent an attractive target for biomarker optimisation and immunotherapy design.

Funder

Cancer Research UK

RCUK | Medical Research Council

Publisher

Springer Science and Business Media LLC

Subject

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

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