Loss of p53 suppresses replication-stress-induced DNA breakage in G1/S checkpoint deficient cells.
Bente BenedictTanja van HarnMarleen DekkerSimone HermsenAsli KucukosmanogluWietske PietersElly Delzenne-GoetteJosephine C DorsmanEva PetermannFloris FoijerHein Te RielePublished in: eLife (2018)
In cancer cells, loss of G1/S control is often accompanied by p53 pathway inactivation, the latter usually rationalized as a necessity for suppressing cell cycle arrest and apoptosis. However, we found an unanticipated effect of p53 loss in mouse and human G1-checkpoint-deficient cells: reduction of DNA damage. We show that abrogation of the G1/S-checkpoint allowed cells to enter S-phase under growth-restricting conditions at the expense of severe replication stress manifesting as decelerated DNA replication, reduced origin firing and accumulation of DNA double-strand breaks. In this system, loss of p53 allowed mitogen-independent proliferation, not by suppressing apoptosis, but rather by restoring origin firing and reducing DNA breakage. Loss of G1/S control also caused DNA damage and activation of p53 in an in vivo retinoblastoma model. Moreover, in a teratoma model, loss of p53 reduced DNA breakage. Thus, loss of p53 may promote growth of incipient cancer cells by reducing replication-stress-induced DNA damage.
Keyphrases
- cell cycle arrest
- dna damage
- stress induced
- cell death
- pi k akt
- oxidative stress
- induced apoptosis
- signaling pathway
- circulating tumor
- dna repair
- endoplasmic reticulum stress
- single molecule
- cell free
- endothelial cells
- cell cycle
- cell proliferation
- immune response
- inflammatory response
- early onset
- drug induced
- nucleic acid