4.8 Article

RNA/DNA Hybrid Interactome Identifies DXH9 as a Molecular Player in Transcriptional Termination and R-Loop-Associated DNA Damage

Journal

CELL REPORTS
Volume 23, Issue 6, Pages 1891-1905

Publisher

CELL PRESS
DOI: 10.1016/j.celrep.2018.04.025

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Funding

  1. Ataxia UK
  2. Motor Neuron Disease Association studentship [Gromak/Jun11/6278]
  3. Dunn School of Pathology (University of Oxford)
  4. Lundbeck Foundation [R126-2012-12263]
  5. Royal Society University Research Fellowship [UF150656]
  6. MRC New Investigator Research Grant [MR/J007870/1]
  7. John Fell award [BVD07340, 133/090]
  8. MRC [MR/J007870/1] Funding Source: UKRI
  9. Ataxia UK [7126] Funding Source: researchfish
  10. Lundbeck Foundation [R126-2012-12263] Funding Source: researchfish
  11. Medical Research Council [MR/J007870/1] Funding Source: researchfish
  12. Motor Neurone Disease Association [Gromak/Jun11/6278] Funding Source: researchfish

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R-loops comprise an RNA/DNA hybrid and displaced single-stranded DNA. They play important biological roles and are implicated in pathology. Even so, proteins recognizing these structures are largely undefined. Using affinity purification with the S9.6 antibody coupled to mass spectrometry, we defined the RNA/DNA hybrid interactome in HeLa cells. This consists of known R-loop-associated factors SRSF1, FACT, and Top1, and yet uncharacterized interactors, including helicases, RNA processing, DNA repair, and chromatin factors. We validate specific examples of these interactors and characterize their involvement in R-loop biology. A top candidate DHX9 helicase promotes R-loop suppression and transcriptional termination. DHX9 interacts with PARP1, and both proteins prevent R-loop-associated DNA damage. DHX9 and other interactome helicases are overexpressed in cancer, linking R-loop-mediated DNA damage and disease. Our RNA/DNA hybrid interactome provides a powerful resource to study R-loop biology in health and disease.

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