DNA damage-induced replication stress results in PA200-proteasome-mediated degradation of acetylated histones

Imke K. Mandemaker, Marit E. Geijer, Iris Kik, Karel Bezstarosti, Erikjan Rijkers, Anja Raams, Roel C. Janssens, Hannes Lans, Jan H.J. Hoeijmakers, Jeroen A.A. Demmers, Wim Vermeulen, Jurgen A. Marteijn

Research output: Contribution to journalArticlepeer-review

37 Citations (Scopus)


Histone acetylation influences protein interactions and chromatin accessibility and plays an important role in the regulation of transcription, replication, and DNA repair. Conversely, DNA damage affects these crucial cellular processes and induces changes in histone acetylation. However, a comprehensive overview of the effects of DNA damage on the histone acetylation landscape is currently lacking. To quantify changes in histone acetylation, we developed an unbiased quantitative mass spectrometry analysis on affinity-purified acetylated histone peptides, generated by differential parallel proteolysis. We identify a large number of histone acetylation sites and observe an overall reduction of acetylated histone residues in response to DNA damage, indicative of a histone-wide loss of acetyl modifications. This decrease is mainly caused by DNA damage-induced replication stress coupled to specific proteasome-dependent loss of acetylated histones. Strikingly, this degradation of acetylated histones is independent of ubiquitylation but requires the PA200-proteasome activator, a complex that specifically targets acetylated histones for degradation. The uncovered replication stress-induced degradation of acetylated histones represents an important chromatin-modifying response to cope with replication stress.

Original languageEnglish
Article numbere45566
JournalEMBO Reports
Issue number10
Publication statusPublished - Oct 2018


  • acetylation
  • DNA damage
  • histone
  • PA200-proteasome
  • replication stress


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