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Quantitative dissection of transcription in development yields evidence for transcription factor-driven chromatin accessibility

  • Elizabeth Eck
  • , Jonathan Liu
  • , Maryam Kazemzadeh-Atoufi
  • , Sydney Ghoreishi
  • , Shelby Blythe
  • , Hernan G. Garcia
  • University of California at Berkeley
  • Northwestern University
  • California Institute for Quantitative Biosciences

Research output: Contribution to journalArticlepeer-review

30 Scopus citations

Abstract

Thermodynamic models of gene regulation can predict transcriptional regulation in bacteria, but in eukaryotes chromatin accessibility and energy expenditure may call for a different framework. Here we systematically tested the predictive power of models of DNA accessibility based on the Monod-Wyman- Changeux (MWC) model of allostery, which posits that chromatin uctuates between accessible and inaccessible states. We dissected the regulatory dynamics of hunchback by the activator Bicoid and the pioneer-like transcription factor Zelda in living Drosophila embryos and showed that no thermodynamic or non-equilibrium MWC model can recapitulate hunchback transcription. Therefore, we explored a model where DNA accessibility is not the result of thermal uctuations but is catalyzed by Bicoid and Zelda, possibly through histone acetylation, and found that this model can predict hunchback dynamics. Thus, our theory-experiment dialogue uncovered potential molecular mechanisms of transcriptional regulatory dynamics, a key step toward reaching a predictive understanding of developmental decision-making.

Original languageEnglish
Article numbere56429
Pages (from-to)1-99
Number of pages99
JournaleLife
Volume9
DOIs
StatePublished - Oct 2020
Externally publishedYes

Keywords

  • Bicoid
  • Chromatin
  • Drosophila melanogaster
  • Hunchback
  • Live-imaging
  • Non-equilibrium models
  • Pioneer-factor
  • Thermodynamic models
  • Transcription
  • Zelda

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