Pathway-guided analysis identifies Myc-dependent alternative pre-mRNA splicing in aggressive prostate cancers

Author:

Phillips John W.,Pan Yang,Tsai Brandon L.,Xie Zhijie,Demirdjian Levon,Xiao Wen,Yang Harry T.ORCID,Zhang Yida,Lin Chia Ho,Cheng Donghui,Hu Qiang,Liu Song,Black Douglas L.ORCID,Witte Owen N.,Xing Yi

Abstract

We sought to define the landscape of alternative pre-mRNA splicing in prostate cancers and the relationship of exon choice to known cancer driver alterations. To do so, we compiled a metadataset composed of 876 RNA-sequencing (RNA-Seq) samples from five publicly available sources representing a range of prostate phenotypes from normal tissue to drug-resistant metastases. We subjected these samples to exon-level analysis with rMATS-turbo, purpose-built software designed for large-scale analyses of splicing, and identified 13,149 high-confidence cassette exon events with variable incorporation across samples. We then developed a computational framework, pathway enrichment-guided activity study of alternative splicing (PEGASAS), to correlate transcriptional signatures of 50 different cancer driver pathways with these alternative splicing events. We discovered that Myc signaling was correlated with incorporation of a set of 1,039 cassette exons enriched in genes encoding RNA binding proteins. Using a human prostate epithelial transformation assay, we confirmed the Myc regulation of 147 of these exons, many of which introduced frameshifts or encoded premature stop codons. Our results connect changes in alternative pre-mRNA splicing to oncogenic alterations common in prostate and many other cancers. We also establish a role for Myc in regulating RNA splicing by controlling the incorporation of nonsense-mediated decay-determinant exons in genes encoding RNA binding proteins.

Funder

UCLA Tumor Cell Biology Training Grant

Office of the Assistant Secretary of Defense for Health Affairs Prostate Cancer Research Program

HHS | NIH | National Cancer Institute

Parker Institute for Cancer Immunotherapy

Publisher

Proceedings of the National Academy of Sciences

Subject

Multidisciplinary

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