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Pan-cancer pervasive upregulation of 3' UTR splicing drives tumourigenesis.

Authors :: Chan JJ
Zhang B
Chew XH
Salhi A
Kwok ZH
Lim CY
Desi N
Subramaniam N
Siemens A
Kinanti T
Ong S
Sanchez-Mejias A
Ly PT
An O
Sundar R
Fan X
Wang S
Siew BE
Lee KC
Chong CS
Lieske B
Cheong WK
Goh Y
Fam WN
Ooi MG
Koh BTH
Iyer SG
Ling WH
Chen J
Yoong BK
Chanwat R
Bonney GK
Goh BKP
Zhai W
Fullwood MJ
Wang W
Tan KK
Chng WJ
Dan YY
Pitt JJ
Roca X
Guccione E
Vardy LA
Chen L
Gao X
Chow PKH
Yang H
Tay Y
Source :: Nature cell biology [Nat Cell Biol] 2022 Jun; Vol. 24 (6), pp. 928-939. Date of Electronic Publication: 2022 May 26.
Publication Year :: 2022
Abstract: Most mammalian genes generate messenger RNAs with variable untranslated regions (UTRs) that are important post-transcriptional regulators. In cancer, shortening at 3' UTR ends via alternative polyadenylation can activate oncogenes. However, internal 3' UTR splicing remains poorly understood as splicing studies have traditionally focused on protein-coding alterations. Here we systematically map the pan-cancer landscape of 3' UTR splicing and present this in SpUR ( http://www.cbrc.kaust.edu.sa/spur/home/ ). 3' UTR splicing is widespread, upregulated in cancers, correlated with poor prognosis and more prevalent in oncogenes. We show that antisense oligonucleotide-mediated inhibition of 3' UTR splicing efficiently reduces oncogene expression and impedes tumour progression. Notably, CTNNB1 3' UTR splicing is the most consistently dysregulated event across cancers. We validate its upregulation in hepatocellular carcinoma and colon adenocarcinoma, and show that the spliced 3' UTR variant is the predominant contributor to its oncogenic functions. Overall, our study highlights the importance of 3' UTR splicing in cancer and may launch new avenues for RNA-based anti-cancer therapeutics.<br /> (© 2022. The Author(s).)