| Literature DB >> 25557911 |
Ditte Kjærsgaard Klein1, Saskia Hoffmann1, Johanna K Ahlskog1, Karen O'Hanlon1, Marianne Quaas2, Brian D Larsen1, Baptiste Rolland1, Heike I Rösner1, David Walter1, Arne Nedergaard Kousholt1, Tobias Menzel1, Michael Lees1, Jens Vilstrup Johansen1, Juri Rappsilber3, Kurt Engeland2, Claus Storgaard Sørensen1.
Abstract
Cells respond to DNA damage by activating cell cycle checkpoints to delay proliferation and facilitate DNA repair. Here, to uncover new checkpoint regulators, we perform RNA interference screening targeting genes involved in ubiquitylation processes. We show that the F-box protein cyclin F plays an important role in checkpoint control following ionizing radiation. Cyclin F-depleted cells initiate checkpoint signalling after ionizing radiation, but fail to maintain G2 phase arrest and progress into mitosis prematurely. Importantly, cyclin F suppresses the B-Myb-driven transcriptional programme that promotes accumulation of crucial mitosis-promoting proteins. Cyclin F interacts with B-Myb via the cyclin box domain. This interaction is important to suppress cyclin A-mediated phosphorylation of B-Myb, a key step in B-Myb activation. In summary, we uncover a regulatory mechanism linking the F-box protein cyclin F with suppression of the B-Myb/cyclin A pathway to ensure a DNA damage-induced checkpoint response in G2.Entities:
Mesh:
Substances:
Year: 2015 PMID: 25557911 DOI: 10.1038/ncomms6800
Source DB: PubMed Journal: Nat Commun ISSN: 2041-1723 Impact factor: 14.919