A Novel Therapeutic Strategy Targeting BACH1 for Triple-Negative Breast Cancer
Abstract
Breast cancer is the second most cancer among women with a chance of 15% in their life time. The most aggressive andlethal subtype of breast cancer is triple negative breast cancer (TNBC), as evidenced with higher rates of recurrence,metastasis, and therapy resistance. However, there is lack of approved targeted therapy for the patients with TNBC. The goalof my research is to provide a novel therapeutic regimen to give benefits to the patients with TNBC. My researchaccomplishment during the second year (2018-2019) is continued from the first year to (1) define how BACH1 regulatesmitochondrial membrane genes for metabolism of breast cancer using silencing BACH1-target genes, (2) Established whethercombination treatment using hemin and metformin is effective for breast cancer treatment in xenograft models. Mitochondrialmembrane genes including COX15 and UQCRC1 are direct target of BACH1 in breast cancer cells, thus silencing COX15 orUQCRC1 in BACH1-depleted cancer cells restored metformin sensitivity. Molecular mechanisms beyond is through restoredNAD+ levels as well as decreased mitochondrial respiration capacity indicated as oxygen consumption rate (OCR) usingSeahorse analysis. Importantly, metabolic flow of 13C-labeled glucose or glutamine was higher for glycolysis in BACH1-enriched cells relative to BACH1-depleted cells.
Document Details
- Document Type
- Technical Report
- Publication Date
- Jul 01, 2020
- Accession Number
- AD1110624
Entities
People
- Jiyoung Lee
- Marsha Rosner
Organizations
- University of Chicago