BRD4 prevents the accumulation of R-loops and protects against transcription–replication collision events and DNA damage Journal Articles uri icon

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abstract

  • AbstractProper chromatin function and maintenance of genomic stability depends on spatiotemporal coordination between the transcription and replication machinery. Loss of this coordination can lead to DNA damage from increased transcription-replication collision events. We report that deregulated transcription following BRD4 loss in cancer cells leads to the accumulation of RNA:DNA hybrids (R-loops) and collisions with the replication machinery causing replication stress and DNA damage. Whole genome BRD4 and γH2AX ChIP-Seq with R-loop IP qPCR reveals that BRD4 inhibition leads to accumulation of R-loops and DNA damage at a subset of known BDR4, JMJD6, and CHD4 co-regulated genes. Interference with BRD4 function causes transcriptional downregulation of the DNA damage response protein TopBP1, resulting in failure to activate the ATR-Chk1 pathway despite increased replication stress, leading to apoptotic cell death in S-phase and mitotic catastrophe. These findings demonstrate that inhibition of BRD4 induces transcription-replication conflicts, DNA damage, and cell death in oncogenic cells.

authors

  • Lam, Fred C
  • Kong, Yi Wen
  • Huang, Qiuying
  • Vu Han, Tu-Lan
  • Maffa, Amanda D
  • Kasper, Ekkehard
  • Yaffe, Michael B

publication date

  • August 14, 2020

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