Citation
- Authors: Batsche, E., Yaniv, M., Muchardt, C.
- Year: 2006
- Journal: Nat Struct Mol Biol 13 22-9
- Applications: in vitro / DNA, siRNA / jetPEI
- Cell types:
- Name: HeLa
Description: Human cervix epitheloid carcinoma cells - Name: MCF7
Description: Human breast adenocarcinoma cells
Known as: MCF-7, MCF 7
- Name: HeLa
Abstract
The SWI/SNF (mating-type switch/sucrose nonfermenting) complex involved in chromatin remodeling on promoters has also been detected on the coding region of genes. Here we show that SWI/SNF can function as a regulator of alternative splicing. We found that the catalytic subunit Brm favors inclusion of variant exons in the mRNA of several genes, including E-cadherin, BIM, cyclin D1 and CD44. Consistent with this, Brm associates with several components of the spliceosome and with Sam68, an ERK-activated enhancer of variant exon inclusion. Examination of the CD44 gene revealed that Brm induced accumulation of RNA polymerase II (RNAPII) with a modified CTD phosphorylation pattern on regions encoding variant exons. Altogether, our data suggest that on genes regulated by SWI/SNF, Brm contributes to the crosstalk between transcription and RNA processing by decreasing RNAPII elongation rate and facilitating recruitment of the splicing machinery to variant exons with suboptimal splice sites.