Frontiers in Genetics (Jul 2023)

Glucocorticoid stimulation induces regionalized gene responses within topologically associating domains

  • Christophe Tav,
  • Christophe Tav,
  • Christophe Tav,
  • Éric Fournier,
  • Éric Fournier,
  • Éric Fournier,
  • Michèle Fournier,
  • Michèle Fournier,
  • Fatemeh Khadangi,
  • Fatemeh Khadangi,
  • Audrey Baguette,
  • Maxime C. Côté,
  • Maxime C. Côté,
  • Maruhen A. D. Silveira,
  • Maruhen A. D. Silveira,
  • Félix-Antoine Bérubé-Simard,
  • Félix-Antoine Bérubé-Simard,
  • Guillaume Bourque,
  • Guillaume Bourque,
  • Arnaud Droit,
  • Arnaud Droit,
  • Arnaud Droit,
  • Arnaud Droit,
  • Steve Bilodeau,
  • Steve Bilodeau,
  • Steve Bilodeau,
  • Steve Bilodeau

DOI
https://doi.org/10.3389/fgene.2023.1237092
Journal volume & issue
Vol. 14

Abstract

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Transcription-factor binding to cis-regulatory regions regulates the gene expression program of a cell, but occupancy is often a poor predictor of the gene response. Here, we show that glucocorticoid stimulation led to the reorganization of transcriptional coregulators MED1 and BRD4 within topologically associating domains (TADs), resulting in active or repressive gene environments. Indeed, we observed a bias toward the activation or repression of a TAD when their activities were defined by the number of regions gaining and losing MED1 and BRD4 following dexamethasone (Dex) stimulation. Variations in Dex-responsive genes at the RNA levels were consistent with the redistribution of MED1 and BRD4 at the associated cis-regulatory regions. Interestingly, Dex-responsive genes without the differential recruitment of MED1 and BRD4 or binding by the glucocorticoid receptor were found within TADs, which gained or lost MED1 and BRD4, suggesting a role of the surrounding environment in gene regulation. However, the amplitude of the response of Dex-regulated genes was higher when the differential recruitment of the glucocorticoid receptor and transcriptional coregulators was observed, reaffirming the role of transcription factor-driven gene regulation and attributing a lesser role to the TAD environment. These results support a model where a signal-induced transcription factor induces a regionalized effect throughout the TAD, redefining the notion of direct and indirect effects of transcription factors on target genes.

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