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Intron retention is a hallmark and spliceosome represents a therapeutic vulnerability in aggressive prostate cancer.


ABSTRACT: The role of dysregulation of mRNA alternative splicing (AS) in the development and progression of solid tumors remains to be defined. Here we describe the first comprehensive AS landscape in the spectrum of human prostate cancer (PCa) evolution. We find that the severity of splicing dysregulation correlates with disease progression and establish intron retention as a hallmark of PCa stemness and aggressiveness. Systematic interrogation of 274 splicing-regulatory genes (SRGs) uncovers prevalent genomic copy number variations (CNVs), leading to mis-expression of ~68% of SRGs during PCa development and progression. Consequently, many SRGs are prognostic. Surprisingly, androgen receptor controls a splicing program distinct from its transcriptional regulation. The spliceosome modulator, E7107, reverses cancer aggressiveness and inhibits castration-resistant PCa (CRPC) in xenograft and autochthonous PCa models. Altogether, our studies establish aberrant AS landscape caused by dysregulated SRGs as a hallmark of PCa aggressiveness and the spliceosome as a therapeutic vulnerability for CRPC.

SUBMITTER: Zhang D 

PROVIDER: S-EPMC7190674 | biostudies-literature | 2020 Apr

REPOSITORIES: biostudies-literature

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Intron retention is a hallmark and spliceosome represents a therapeutic vulnerability in aggressive prostate cancer.

Zhang Dingxiao D   Hu Qiang Q   Liu Xiaozhuo X   Ji Yibing Y   Chao Hsueh-Ping HP   Liu Yan Y   Tracz Amanda A   Kirk Jason J   Buonamici Silvia S   Zhu Ping P   Wang Jianmin J   Liu Song S   Tang Dean G DG  

Nature communications 20200429 1


The role of dysregulation of mRNA alternative splicing (AS) in the development and progression of solid tumors remains to be defined. Here we describe the first comprehensive AS landscape in the spectrum of human prostate cancer (PCa) evolution. We find that the severity of splicing dysregulation correlates with disease progression and establish intron retention as a hallmark of PCa stemness and aggressiveness. Systematic interrogation of 274 splicing-regulatory genes (SRGs) uncovers prevalent g  ...[more]

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