4.8 Article

A switch from hBrm to Brg1 at IFN gamma-activated sequences mediates the activation of human genes

Journal

CELL RESEARCH
Volume 20, Issue 12, Pages 1345-1360

Publisher

INST BIOCHEMISTRY & CELL BIOLOGY
DOI: 10.1038/cr.2010.155

Keywords

chromatin remodeling; hBrm; Brg1; Stat1; p300; heat-shock; IFN gamma

Categories

Funding

  1. National Natural Science Foundation of China [90408007, 30871382, 30721063]
  2. National Basic Research Program of China (973 Program) [2005CB522405]
  3. National Key Scientific Program [2011CB964902]
  4. Special Funds of State Key Laboratories [2060204]

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The SWI/SNF chromatin-remodeling complexes utilize energy from ATP hydrolysis to reposition nucleosomes and regulate the expression of human genes. Here, we studied the roles of human Brahma (hBrm) and Brahma-related gene 1 (Brg1), the ATPase subunits of the SWI/SNF complexes, in regulating human genes. Our results indicate that both hBrm and Brg1 interact with Signal transducer and activator of transcription (Stat) 1 in vitro. However, Stat1 in its native form only recruits hBrm to IFN gamma-activated sequences (GAS) of individual genes; by contrast, in a stress-induced phosphorylated form, Stat1 mainly binds to Brg1. Under basal conditions, hBrm is recruited by native Stat1 to the GAS and exists in a mSin3/HDAC co-repressor complex on the hsp90a gene, which shows a compact chromatin structure. Upon heat-shock, hBrm is acetylated by p300 and dissociates from the co-repressor complex, which the phosphorylated Stat1 is increased, and binds and recruits Brg1 to the GAS, leading to elevated induction of the gene. This hBrm/Brg1 switch also occurs at the GAS of all of the three examined immune genes in heat-shocked cells; however, this switch only occurs in specific cell types upon exposure to IFN gamma. Regardless of the stimulus, the hBrm/Brg1 switch at the GAS elicits an increase in gene activity. Our data are consistent with the hypothesis that the hBrm/Brg1 switch is an indicator of the responsiveness of a gene to heat-shock or IFN gamma stimulation and may represent an on-off switch of gene expression in vivo.

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