| Literature DB >> 26842708 |
Samar Alsafadi1, Alexandre Houy1, Aude Battistella1, Tatiana Popova1, Michel Wassef2, Emilie Henry3, Franck Tirode1, Angelos Constantinou4, Sophie Piperno-Neumann5, Sergio Roman-Roman3, Martin Dutertre6, Marc-Henri Stern1.
Abstract
Hotspot mutations in the spliceosome gene SF3B1 are reported in ∼20% of uveal melanomas. SF3B1 is involved in 3'-splice site (3'ss) recognition during RNA splicing; however, the molecular mechanisms of its mutation have remained unclear. Here we show, using RNA-Seq analyses of uveal melanoma, that the SF3B1(R625/K666) mutation results in deregulated splicing at a subset of junctions, mostly by the use of alternative 3'ss. Modelling the differential junctions in SF3B1(WT) and SF3B1(R625/K666) cell lines demonstrates that the deregulated splice pattern strictly depends on SF3B1 status and on the 3'ss-sequence context. SF3B1(WT) knockdown or overexpression do not reproduce the SF3B1(R625/K666) splice pattern, qualifying SF3B1(R625/K666) as change-of-function mutants. Mutagenesis of predicted branchpoints reveals that the SF3B1(R625/K666)-promoted splice pattern is a direct result of alternative branchpoint usage. Altogether, this study provides a better understanding of the mechanisms underlying splicing alterations induced by mutant SF3B1 in cancer, and reveals a role for alternative branchpoints in disease.Entities:
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Year: 2016 PMID: 26842708 PMCID: PMC4743009 DOI: 10.1038/ncomms10615
Source DB: PubMed Journal: Nat Commun ISSN: 2041-1723 Impact factor: 17.694