HDAC inhibitors induce LIFR expression and promote a dormancy phenotype in breast cancer.
Miranda E ClementsLauren HoltslanderCourtney EdwardsVera ToddSamuel D R DooyemaKennady BullockKensey BergdorfCynthia A ZahnowRoisin M ConnollyRachelle W JohnsonPublished in: Oncogene (2021)
Despite advances in breast cancer treatment, residual disease driven by dormant tumor cells continues to be a significant clinical problem. Leukemia inhibitory factor receptor (LIFR) promotes a dormancy phenotype in breast cancer cells and LIFR loss is correlated with poor patient survival. Herein, we demonstrate that histone deacetylase inhibitors (HDACi), which are in phase III clinical trials for breast cancer, epigenetically induced LIFR and activated a pro-dormancy program in breast cancer cells. HDACi slowed breast cancer cell proliferation and reduced primary tumor growth. Primary breast tumors from HDACi-treated patients had increased LIFR levels and reduced proliferation rates compared to pre-treatment levels. Recent Phase II clinical trial data studying entinostat and azacitidine in metastatic breast cancer revealed that induction of several pro-dormancy genes post-treatment was associated with prolonged patient survival. Together, these findings suggest HDACi as a potential therapeutic avenue to promote dormancy, prevent recurrence, and improve patient outcomes in breast cancer.
Keyphrases
- clinical trial
- phase ii
- phase iii
- open label
- breast cancer cells
- histone deacetylase
- cell proliferation
- metastatic breast cancer
- double blind
- newly diagnosed
- case report
- ejection fraction
- study protocol
- free survival
- anti inflammatory
- genome wide
- placebo controlled
- transcription factor
- cell cycle
- dna methylation
- quality improvement
- poor prognosis
- long noncoding rna
- bone marrow
- oxidative stress
- breast cancer risk
- young adults
- randomized controlled trial
- drug induced
- prognostic factors
- machine learning
- artificial intelligence