. This proposal builds on our past studies of the human DEK gene, which is amplified and overexpressed, and thus implicated in many human cancer types including head and neck squamous cell carcinoma (HNSCC). HNSCC is the sixth most common malignancy worldwide - with dismal outcomes. Identification of biomarkers for early diagnosis and new drug targets remains imperative. DEK is a highly conserved protein that binds nucleic acids and regulates diverse nuclear processes, including transcription. We have shown that DEK is an oncogene, by reporting that DEK overexpression extends the life span of primary human keratinocytes, induces hyperplasia in 3D models of epidermis, cooperates with classical oncogenes to stimulate keratinocyte transformation, and promotes HPV+ and HPV? HNSCC and breast cancer cell proliferation and invasion. Our data also demonstrated that DEK overexpression increases ?-catenin activity, and this DEK-?-catenin axis is required and sufficient for some cancer phenotypes. A major hurdle in neoplastic transformation is the ability of cells to meet high bioenergetic and biosynthetic needs for sustained cancer cell growth. Recently, we reported that DEK overexpression increases transcription of key enzymes in glycolysis, lactate fermentation and cholesterol synthesis, and accumulation of metabolites that are glycolytic end products. However, it is not known whether ?-catenin is required for DEK-driven metabolic reprogramming, and we do not understand the role of glycolysis and cholesterol synthesis in DEK-driven cancer phenotypes. Finally, in preliminary studies, we discovered that DEK is uniquely targeted to mitochondria, and DEK overexpression stimulated cellular oxidative phosphorylation capacity. In the proposed 3 aims, we test 2 hypotheses. First, that DEK overexpression promotes HNSCC oncogenic phenotypes by 2 discrete pools of DEK which drive metabolic deregulation, one nuclear (Aim1) and one mitochondrial (Aim2). Second, that targeting either ?-catenin, or vulnerable nodes of the metabolic signature is an effective strategy to prevent HNSCC phenotypes. In partnership with an expert in stable isotope resolved metabolomics technologies, we will generate an atom-resolved map of metabolic networks controlled by DEK overexpression, and will then use this map to identify and validate novel metabolic flux vulnerabilities for drug targeting and diagnostic biomarkers (Aim3). Taken together, the proposed experiments represent a significant first step towards innovative prevention and treatment strategies to improve the outcomes of HNSCC via metabolic interventions.

Public Health Relevance

. For a cell to become cancerous, it must reprogram its metabolism in order to fuel unrestrained growth and progression to metastasis. Head and neck cancer is one of the most common cancers ? with low survival and treatment regimens that can leave patients (sometimes quite young) disfigured and unable to swallow or speak. As experts on a human protein known as ?DEK,? we have performed experiments that strongly suggest that DEK controls metabolic reprogramming in order to promote cancer development and metastatic dissemination. The proposed studies will determine whether this is the case, while also revealing and testing new metabolism-based strategies for head and neck cancer prevention and treatment.

Agency
National Institute of Health (NIH)
Institute
National Cancer Institute (NCI)
Type
Research Project (R01)
Project #
1R01CA239605-01A1
Application #
9914529
Study Section
Cancer Prevention Study Section (CPSS)
Program Officer
Willis, Kristine Amalee
Project Start
2019-12-01
Project End
2024-11-30
Budget Start
2019-12-01
Budget End
2020-11-30
Support Year
1
Fiscal Year
2020
Total Cost
Indirect Cost
Name
Cincinnati Children's Hospital Medical Center
Department
Type
DUNS #
071284913
City
Cincinnati
State
OH
Country
United States
Zip Code
45229