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Putatively cancer-specific exon–exon junctions are shared across patients and present in developmental and other non-cancer cells

Julianne K. David, Sean K. Maden, Benjamin R. Weeder, Reid F. Thompson, Abhinav Nellore

2020NAR Cancer23 citationsDOIOpen Access PDF

Abstract

Abstract This study probes the distribution of putatively cancer-specific junctions across a broad set of publicly available non-cancer human RNA sequencing (RNA-seq) datasets. We compared cancer and non-cancer RNA-seq data from The Cancer Genome Atlas (TCGA), the Genotype-Tissue Expression (GTEx) Project and the Sequence Read Archive. We found that (i) averaging across cancer types, 80.6% of exon–exon junctions thought to be cancer-specific based on comparison with tissue-matched samples (σ = 13.0%) are in fact present in other adult non-cancer tissues throughout the body; (ii) 30.8% of junctions not present in any GTEx or TCGA normal tissues are shared by multiple samples within at least one cancer type cohort, and 87.4% of these distinguish between different cancer types; and (iii) many of these junctions not found in GTEx or TCGA normal tissues (15.4% on average, σ = 2.4%) are also found in embryological and other developmentally associated cells. These findings refine the meaning of RNA splicing event novelty, particularly with respect to the human neoepitope repertoire. Ultimately, cancer-specific exon–exon junctions may have a substantial causal relationship with the biology of disease.

Topics & Concepts

ExonCancerBiologyGeneticsCancer researchGeneCancer Genomics and DiagnosticsRNA Research and SplicingRNA modifications and cancer
Putatively cancer-specific exon–exon junctions are shared across patients and present in developmental and other non-cancer cells | Litcius