Litcius/Paper detail

Identification of long non-coding RNAs in advanced prostate cancer associated with androgen receptor splicing factors

Ken‐ichi Takayama, Tetsuya Fujimura, Yutaka Suzuki, Satoshi Inoue

2020Communications Biology55 citationsDOIOpen Access PDF

Abstract

The molecular and cellular mechanisms of development of castration-resistant prostate cancer (CRPC) remain elusive. Here, we analyzed the comprehensive and unbiased expression profiles of both protein-coding and long non-coding RNAs (lncRNAs) using RNA-sequencing to reveal the clinically relevant molecular signatures in CRPC tissues. For protein-coding genes upregulated in CRPC, we found that mitochondria-associated pathway, androgen receptor (AR), and spliceosome associated genes were enriched. Moreover, we discovered AR-regulated lncRNAs, CRPC-Lncs, that are highly expressed in CRPC tissues. Notably, silencing of two lncRNAs (CRPC-Lnc #6: PRKAG2-AS1 and #9: HOXC-AS1) alleviated CRPC tumor growth, showing repression of AR and AR variant expression. Mechanistically, subcellular localization of the splicing factor, U2AF2, with an essential role in AR splicing machinery was modulated dependent on the expression level of CRPC-Lnc #6. Thus, our investigation highlights a cluster of lncRNAs which could serve as AR regulators as well as potential biomarkers in CRPC.

Topics & Concepts

Androgen receptorRNA splicingBiologyLong non-coding RNAProstate cancerGene silencingGeneAlternative splicingSpliceosomeComputational biologyCancer researchRNACell biologyMessenger RNAGeneticsCancerCancer-related molecular mechanisms researchProstate Cancer Treatment and ResearchRNA Research and Splicing