| Literature DB >> 33621493 |
Kumar Somyajit1, Julian Spies2, Fabian Coscia3, Ufuk Kirik4, Maj-Britt Rask2, Ji-Hoon Lee5, Kai John Neelsen2, Andreas Mund3, Lars Juhl Jensen4, Tanya T Paull5, Matthias Mann3, Jiri Lukas6.
Abstract
Homology-directed repair (HDR) safeguards DNA integrity under various forms of stress, but how HDR protects replicating genomes under extensive metabolic alterations remains unclear. Here, we report that besides stalling replication forks, inhibition of ribonucleotide reductase (RNR) triggers metabolic imbalance manifested by the accumulation of increased reactive oxygen species (ROS) in cell nuclei. This leads to a redox-sensitive activation of the ATM kinase followed by phosphorylation of the MRE11 nuclease, which in HDR-deficient settings degrades stalled replication forks. Intriguingly, nascent DNA degradation by the ROS-ATM-MRE11 cascade is also triggered by hypoxia, which elevates signaling-competent ROS and attenuates functional HDR without arresting replication forks. Under these conditions, MRE11 degrades daughter-strand DNA gaps, which accumulate behind active replisomes and attract error-prone DNA polymerases to escalate mutation rates. Thus, HDR safeguards replicating genomes against metabolic assaults by restraining mutagenic repair at aberrantly processed nascent DNA. These findings have implications for cancer evolution and tumor therapy.Entities:
Keywords: BRCA1/2; cancer evolution; genome instability; homology-directed repair; hypoxia; nascent DNA degradation; reactive oxygen species; replication stress; ribonucleotide reductase; translesion DNA synthesis
Year: 2021 PMID: 33621493 DOI: 10.1016/j.devcel.2021.01.011
Source DB: PubMed Journal: Dev Cell ISSN: 1534-5807 Impact factor: 12.270