| Literature DB >> 24514149 |
Pamela Bielli1, Roberta Busà, Savino M Di Stasi, Manuel J Munoz, Flavia Botti, Alberto R Kornblihtt, Claudio Sette.
Abstract
Alternative splicing (AS) is tightly coupled to transcription for the majority of human genes. However, how these two processes are linked is not well understood. Here, we unveil a direct role for the transcription factor FBI-1 in the regulation of AS. FBI-1 interacts with the splicing factor SAM68 and reduces its binding to BCL-X mRNA. This, in turn, results in the selection of the proximal 5' splice site in BCL-X exon 2, thereby favoring the anti-apoptotic BCL-XL variant and counteracting SAM68-mediated apoptosis. Conversely, depletion of FBI-1, or expression of a SAM68 mutant lacking the FBI-1 binding region, restores the ability of SAM68 to induce BCL-XS splicing and apoptosis. FBI-1's role in splicing requires the activity of histone deacetylases, whose pharmacological inhibition recapitulates the effects of FBI-1 knockdown. Our study reveals an unexpected function for FBI-1 in splicing modulation with a direct impact on cell survival.Entities:
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Year: 2014 PMID: 24514149 PMCID: PMC3989673 DOI: 10.1002/embr.201338241
Source DB: PubMed Journal: EMBO Rep ISSN: 1469-221X Impact factor: 8.807