p38 pathway targets SWI-SNF chromatin-remodeling complex to muscle-specific loci

被引:0
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作者
Cristiano Simone
Sonia Vanina Forcales
David A Hill
Anthony N Imbalzano
Lucia Latella
Pier Lorenzo Puri
机构
[1] Laboratory of Gene Expression,Department of Cell Biology
[2] Dulbecco Telethon Institute at Fondazione A. Cesalpino,undefined
[3] Institute of Cell Biology and Tissue Engineering,undefined
[4] San Raffaele Biomedical Science Park of Rome,undefined
[5] The Salk Institute for Biological Studies,undefined
[6] Peptide Biology Laboratory,undefined
[7] University of Massachusetts Medical School,undefined
来源
Nature Genetics | 2004年 / 36卷
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摘要
During skeletal myogenesis, genomic reprogramming toward terminal differentiation is achieved by recruiting chromatin-modifying enzymes to muscle-specific loci1,2. The relative contribution of extracellular signaling cascades in targeting these enzymes to individual genes is unknown. Here we show that the differentiation-activated p38 pathway3,4,5 targets the SWI-SNF chromatin-remodeling complex to myogenic loci. Upon differentiation, p38 kinases were recruited to the chromatin of muscle-regulatory elements. Blockade of p38α/β repressed the transcription of muscle genes by preventing recruitment of the SWI-SNF complex at these elements without affecting chromatin binding of muscle-regulatory factors and acetyltransferases. The SWI-SNF subunit BAF60 could be phosphorylated by p38α-β in vitro, and forced activation of p38α/β in myoblasts by expression of a constitutively active MKK6 (refs. 5,6,7) promoted unscheduled SWI-SNF recruitment to the myogenin promoter. Conversely, inactivation of SWI-SNF enzymatic subunits abrogated MKK6-dependent induction of muscle gene expression. These results identify an unexpected function of differentiation-activated p38 in converting external cues into chromatin modifications at discrete loci, by selectively targeting SWI-SNF to muscle-regulatory elements.
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页码:738 / 743
页数:5
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