Resolution of R-loops by INO80 promotes DNA replication and maintains cancer cell proliferation and viability.
Lisa PrendergastUrszula Lucja McClurgRossitsa HristovaRolando Berlinguer PalminiSarah GreenerKatie VeitchInmaculada HernandezPhilippe PaseroDaniel RicoJonathan M G HigginsAnastas GospodinovManolis Papamichos-ChronakisPublished in: Nature communications (2020)
Collisions between the DNA replication machinery and co-transcriptional R-loops can impede DNA synthesis and are a major source of genomic instability in cancer cells. How cancer cells deal with R-loops to proliferate is poorly understood. Here we show that the ATP-dependent chromatin remodelling INO80 complex promotes resolution of R-loops to prevent replication-associated DNA damage in cancer cells. Depletion of INO80 in prostate cancer PC3 cells leads to increased R-loops. Overexpression of the RNA:DNA endonuclease RNAse H1 rescues the DNA synthesis defects and suppresses DNA damage caused by INO80 depletion. R-loops co-localize with and promote recruitment of INO80 to chromatin. Artificial tethering of INO80 to a LacO locus enabled turnover of R-loops in cis. Finally, counteracting R-loops by INO80 promotes proliferation and averts DNA damage-induced death in cancer cells. Our work suggests that INO80-dependent resolution of R-loops promotes DNA replication in the presence of transcription, thus enabling unlimited proliferation in cancers.
Keyphrases
- dna damage
- prostate cancer
- single molecule
- cell proliferation
- dna repair
- oxidative stress
- transcription factor
- signaling pathway
- circulating tumor
- gene expression
- cell free
- squamous cell carcinoma
- genome wide
- copy number
- mouse model
- radical prostatectomy
- diabetic rats
- dna methylation
- young adults
- endothelial cells
- body composition
- circulating tumor cells
- pi k akt