Estrogen therapy induces receptor-dependent DNA damage enhanced by PARP inhibition in ER+ breast cancer.

Nicole A TraphagenGary N SchwartzSteven TauAmanda JiangSarah R HosfordAbigail E GoenAlyssa M RobertsBianca A RomoAnneka L JohnsonEmily-Claire K DuffyEugene DemidenkoPaul HeverlyYaron MosessonShannon M SoucyFred KollingTodd W Miller

Published in: bioRxiv : the preprint server for biology (2023)

E2-induced ER activity drives DNA damage and growth inhibition in endocrine-resistant breast cancer cells. Inhibition of the DNA damage response using drugs such as PARP inhibitors can enhance therapeutic response to E2. These findings warrant clinical exploration of the combination of E2 with DNA damage response inhibitors in advanced ER+ breast cancer, and suggest that PARP inhibitors may synergize with therapeutics that exacerbate transcriptional stress.

Keyphrases

dna damage
dna damage response
dna repair
breast cancer cells
estrogen receptor
oxidative stress
endoplasmic reticulum
gene expression
small molecule
diabetic rats
transcription factor
mesenchymal stem cells
breast cancer risk
young adults
heat shock protein