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Active transcription and epigenetic reactions synergistically regulate meso-scale genomic organization.

Aayush KantZixian GuoVinayak VinayakMaria Victoria NeguemborWing Shun LiVasundhara AgrawalEmily PujadasLuay Matthew AlmassalhaVadim BackmanMelike LakadamyaliMaria Pia CosmaVivek B Shenoy
Published in: Nature communications (2024)
In interphase nuclei, chromatin forms dense domains of characteristic sizes, but the influence of transcription and histone modifications on domain size is not understood. We present a theoretical model exploring this relationship, considering chromatin-chromatin interactions, histone modifications, and chromatin extrusion. We predict that the size of heterochromatic domains is governed by a balance among the diffusive flux of methylated histones sustaining them and the acetylation reactions in the domains and the process of loop extrusion via supercoiling by RNAPII at their periphery, which contributes to size reduction. Super-resolution and nano-imaging of five distinct cell lines confirm the predictions indicating that the absence of transcription leads to larger heterochromatin domains. Furthermore, the model accurately reproduces the findings regarding how transcription-mediated supercoiling loss can mitigate the impacts of excessive cohesin loading. Our findings shed light on the role of transcription in genome organization, offering insights into chromatin dynamics and potential therapeutic targets.
Keyphrases
  • transcription factor
  • gene expression
  • genome wide
  • dna damage
  • dna methylation
  • oxidative stress
  • physical activity
  • body mass index
  • weight gain
  • climate change
  • photodynamic therapy
  • risk assessment