| Literature DB >> 33152268 |
Vladislav O Sviderskiy1, Lili Blumenberg2, Elizabeth Gorodetsky1, Triantafyllia R Karakousi1, Nicole Hirsh1, Samantha W Alvarez1, Erdem M Terzi1, Efiyenia Kaparos1, Gabrielle C Whiten1, Shakirah Ssebyala1, Peter Tonzi3, Hannan Mir1, Benjamin G Neel2, Tony T Huang3, Sylvia Adams4, Kelly V Ruggles2, Richard Possemato5.
Abstract
Knowledge of fundamental differences between breast cancer subtypes has driven therapeutic advances; however, basal-like breast cancer (BLBC) remains clinically intractable. Because BLBC exhibits alterations in DNA repair enzymes and cell-cycle checkpoints, elucidation of factors enabling the genomic instability present in this subtype has the potential to reveal novel anti-cancer strategies. Here, we demonstrate that BLBC is especially sensitive to suppression of iron-sulfur cluster (ISC) biosynthesis and identify DNA polymerase epsilon (POLE) as an ISC-containing protein that underlies this phenotype. In BLBC cells, POLE suppression leads to replication fork stalling, DNA damage, and a senescence-like state or cell death. In contrast, luminal breast cancer and non-transformed mammary cells maintain viability upon POLE suppression but become dependent upon an ATR/CHK1/CDC25A/CDK2 DNA damage response axis. We find that CDK1/2 targets exhibit hyperphosphorylation selectively in BLBC tumors, indicating that CDK2 hyperactivity is a genome integrity vulnerability exploitable by targeting POLE.Entities:
Keywords: CDK2; Cancer Metabolism; DNA damage; DNA replication; Iron-sulfur clusters; NFS1; POLE1; breast cancer
Mesh:
Substances:
Year: 2020 PMID: 33152268 PMCID: PMC7687292 DOI: 10.1016/j.molcel.2020.10.016
Source DB: PubMed Journal: Mol Cell ISSN: 1097-2765 Impact factor: 17.970