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eRNAs are required for p53-dependent enhancer activity and gene transcription.

Translated title of the contribution: eRNAs are required for p53-dependent enhancer activity and gene transcription.
  • C.A. Melo
  • , J. Drost
  • , P.J. Wijchers
  • , H. van de Werken
  • , E. de Wit
  • , J.A. Ou de Vrielink
  • , R. Elkon
  • , S.A. Melo
  • , N. Leveille
  • , R. Kalluri
  • , W.L. de Laat
  • , R. Agami

Research output: Contribution to journalArticleAcademicpeer-review

Abstract

Binding within or nearby target genes involved in cell proliferation and survival enables the p53 tumor suppressor gene to regulate their transcription and cell-cycle progression. Using genome-wide chromatin-binding profiles, we describe binding of p53 also to regions located distantly from any known p53 target gene. Interestingly, many of these regions possess conserved p53-binding sites and all known hallmarks of enhancer regions. We demonstrate that these p53-bound enhancer regions (p53BERs) indeed contain enhancer activity and interact intrachromosomally with multiple neighboring genes to convey long-distance p53-dependent transcription regulation. Furthermore, p53BERs produce, in a p53-dependent manner, enhancer RNAs (eRNAs) that are required for efficient transcriptional enhancement of interacting target genes and induction of a p53-dependent cell-cycle arrest. Thus, our results ascribe transcription enhancement activity to p53 with the capacity to regulate multiple genes from a single genomic binding site. Moreover, eRNA production from p53BERs is required for efficient p53 transcription enhancement.
Translated title of the contributioneRNAs are required for p53-dependent enhancer activity and gene transcription.
Original languageUndefined/Unknown
Pages (from-to)524-35
Number of pages12
JournalMolecular Cell
Volume49
Issue number3
Publication statusPublished - 2013

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