Diagenode

The glucocorticoid receptor recruits the COMPASS complex to regulateinflammatory transcription at macrophage enhancers.


Greulich, Franziska et al.

Glucocorticoids (GCs) are effective anti-inflammatory drugs; yet, their mechanisms of action are poorly understood. GCs bind to the glucocorticoid receptor (GR), a ligand-gated transcription factor controlling gene expression in numerous cell types. Here, we characterize GR's protein interactome and find the SETD1A (SET domain containing 1A)/COMPASS (complex of proteins associated with Set1) histone H3 lysine 4 (H3K4) methyltransferase complex highly enriched in activated mouse macrophages. We show that SETD1A/COMPASS is recruited by GR to specific cis-regulatory elements, coinciding with H3K4 methylation dynamics at subsets of sites, upon treatment with lipopolysaccharide (LPS) and GCs. By chromatin immunoprecipitation sequencing (ChIP-seq) and RNA-seq, we identify subsets of GR target loci that display SETD1A occupancy, H3K4 mono-, di-, or tri-methylation patterns, and transcriptional changes. However, our data on methylation status and COMPASS recruitment suggest that SETD1A has additional transcriptional functions. Setd1a loss-of-function studies reveal that SETD1A/COMPASS is required for GR-controlled transcription of subsets of macrophage target genes. We demonstrate that the SETD1A/COMPASS complex cooperates with GR to mediate anti-inflammatory effects.

Tags
Antibody

Share this article

Published
February, 2021

Source

Products used in this publication

  • Mouse IgG
    C15200150
    H3K4me1 Antibody
  • Antibody ChIP icon
    C15200151
    H3K4me2 Antibody
  • cut and tag antibody icon
    C15200152
    H3K4me3 Antibody
  • cut and tag antibody icon
    C15410194
    H3K4me1 Antibody
  • Bioruptor Pico
    B01080010
    Bioruptor® Pico sonication device

Events

 See all events

 


       Site map   |   Contact us   |   Conditions of sales   |   Conditions of purchase   |   Privacy policy