SPRTN protease and checkpoint kinase 1 cross-activation loop safeguards DNA replication.
Swagata HalderIgnacio TorrecillaMartin D BurkhalterMarta PopovićJohn FieldenBruno VazJudith OehlerDomenic PilgerDavor LesselKatherine WisemanAbhay Narayan SinghIolanda VendrellRoman FischerMelanie PhilippKristijan RamadanPublished in: Nature communications (2019)
The SPRTN metalloprotease is essential for DNA-protein crosslink (DPC) repair and DNA replication in vertebrate cells. Cells deficient in SPRTN protease exhibit DPC-induced replication stress and genome instability, manifesting as premature ageing and liver cancer. Here, we provide a body of evidence suggesting that SPRTN activates the ATR-CHK1 phosphorylation signalling cascade during physiological DNA replication by proteolysis-dependent eviction of CHK1 from replicative chromatin. During this process, SPRTN proteolyses the C-terminal/inhibitory part of CHK1, liberating N-terminal CHK1 kinase active fragments. Simultaneously, CHK1 full length and its N-terminal fragments phosphorylate SPRTN at the C-terminal regulatory domain, which stimulates SPRTN recruitment to chromatin to promote unperturbed DNA replication fork progression and DPC repair. Our data suggest that a SPRTN-CHK1 cross-activation loop plays a part in DNA replication and protection from DNA replication stress. Finally, our results with purified components of this pathway further support the proposed model of a SPRTN-CHK1 cross-activation loop.
Keyphrases
- dna damage response
- transcription factor
- induced apoptosis
- dna damage
- genome wide
- gene expression
- cell cycle arrest
- protein kinase
- dna repair
- endoplasmic reticulum stress
- oxidative stress
- dna methylation
- tyrosine kinase
- cell proliferation
- stress induced
- signaling pathway
- artificial intelligence
- electronic health record
- cell cycle
- binding protein
- cell free
- circulating tumor cells