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p53 rapidly restructures 3D chromatin organization to trigger a transcriptional response. | LitMetric

AI Article Synopsis

  • The study investigates how the p53 tumor suppressor influences gene transcription during cellular stress, revealing that it alters genome structure in significant ways shortly after activation.
  • Researchers identified 340 genes that p53 directly regulates, many of which were previously unknown, highlighting the extensive impact of p53 on gene expression.
  • The findings suggest that p53 works through specific mechanisms, including the formation of enhancer-promoter loops, to control gene transcription, which could inform future cancer treatment strategies.

Article Abstract

Activation of the p53 tumor suppressor triggers a transcriptional program to control cellular response to stress. However, the molecular mechanisms by which p53 controls gene transcription are not completely understood. Here, we uncover the critical role of spatio-temporal genome architecture in this process. We demonstrate that p53 drives direct and indirect changes in genome compartments, topologically associating domains, and DNA loops prior to one hour of its activation, which escort the p53 transcriptional program. Focusing on p53-bound enhancers, we report 340 genes directly regulated by p53 over a median distance of 116 kb, with 74% of these genes not previously identified. Finally, we showcase that p53 controls transcription of distal genes through newly formed and pre-existing enhancer-promoter loops in a cohesin dependent manner. Collectively, our findings demonstrate a previously unappreciated architectural role of p53 as regulator at distinct topological layers and provide a reliable set of new p53 direct target genes that may help designs of cancer therapies.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC10984980PMC
http://dx.doi.org/10.1038/s41467-024-46666-1DOI Listing

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