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Program Official
Howard L. Parnes, M.D.
Principal Investigator
Laura A Hansen
Awardee Organization

Creighton University
United States

Fiscal Year
2024
Activity Code
R01
Early Stage Investigator Grants (ESI)
Not Applicable
Project End Date
NIH RePORTER
For more information, see NIH RePORTER Project 5R01CA253573-05

Targeting aberrant anti-apoptotic signaling for prevention of skin cancer

Nonmelanoma skin cancer, which includes squamous cell carcinoma (SCC), is the most common cancer diagnosed in the United State,s with the overwhelming majority of cases resulting from ultraviolet (UV) irradiation. SCC usually develop from premalignant precursors, providing an opportunity for intervention to prevent malignant disease and metastatic progression. Treatment of clinically detectable malignant lesions and precursor actinic keratoses still relies largely on surgical excision. These procedures are invasive, carry a significant healthcare cost, and are often an insufficient means of preventing metastatic progression in immunocompromised patients. Consequently, there is a need for more effective mechanism-based treatments with no or minor side effects. In preliminary investigations, we showed that increased nuclear transporter exportin (XPO)1 drives aberrant localization of the scaffolding and signaling protein 14-3-3 to activate prosurvival pathways in SCC cells. Genetic deletion of the gene for 14-3-3 suppressed tumor development by 75% and blocked malignant progression while nontumorigenic skin cells were unaffected by the lack of 14-33. Consequently, our hypothesis is that inhibiting two key regulators that drive aberrant prosurvival signaling will provide a novel and effective means to prevent skin tumor growth and malignant progression with minimal toxicity to the surrounding normal skin. In the proposed research we will delineate the mechanisms and consequences of XPO1-driven aberrant 14-3-3 signaling for malignant keratinocytes (Aim 1), improve upon candidate agents we have developed that disrupt 14-3-3 prosurvival signaling (Aim 2), and provide proof-ofprinciple evidence of the efficacy of 14-3-3 and XPO1 inhibitors for the prevention of skin tumor development and progression using human patient derived (PDX) and UV irradiation-induced skin cancer models. Successful completion of this work is anticipated to lead to novel approaches for the prevention and treatment of skin cancer.

Publications

  • Fu Y, Agrawal S, Snyder DR, Yin S, Zhong N, Grunkemeyer JA, Dietz N, Corlett R, Hansen LA, Waddah AR, Nandipati KC, Xia J. Transcriptomic changes and gene fusions during the progression from Barrett's esophagus to esophageal adenocarcinoma. Biomarker research. 2024 Aug 7;12(1):78. PMID: 39113153
  • Kamayirese S, Maity S, Dieckman LM, Hansen LA, Lovas S. Optimizing Phosphopeptide Structures That Target 14-3-3ε in Cutaneous Squamous Cell Carcinoma. bioRxiv : the preprint server for biology. 2023 Oct 3. PMID: 37873379
  • Kamayirese S, Maity S, Hansen LA, Lovas S. The Development of CDC25A-Derived Phosphoseryl Peptides That Bind 14-3-3ε with High Affinities. International journal of molecular sciences. 2024 Apr 30;25. (9). PMID: 38732131
  • Kamayirese S, Hansen LA, Lovas S. Ligand recognition by 14-3-3 proteins requires negative charges but not necessarily phosphorylation. FEBS letters. 2025 Mar;599(6):838-847. Epub 2025 Jan 5. PMID: 39757510
  • Holmes TR, Al Matouq J, Holmes M, Sioda N, Rudd JC, Bloom C, Nicola L, Palermo NY, Madson JG, Lovas S, Hansen LA. Targeting 14-3-3ε activates apoptotic signaling to prevent cutaneous squamous cell carcinoma. Carcinogenesis. 2021 Feb 25;42(2):232-242. PMID: 32816038
  • Holmes TR, Al-Matouq J, Holmes M, Nicola L, Rudd JC, Lovas S, Hansen LA. Targeting 14-3-3ε-CDC25A interactions to trigger apoptotic cell death in skin cancer. Oncotarget. 2020 Sep 1;11(35):3267-3278. doi: 10.18632/oncotarget.27700. eCollection 2020 Sep 1. PMID: 32934772
  • Kamayirese S, Hansen LA, Lovas S. Negative Charges, Not Necessary Phosphorylation, are Required for Ligand Recognition by 14-3-3 Proteins. bioRxiv : the preprint server for biology. 2024 Nov 12. PMID: 39345434
  • Holmes TR, Dindu S, Hansen LA. Aberrant localization of signaling proteins in skin cancer: Implications for treatment. Molecular carcinogenesis. 2019 Sep;58(9):1631-1639. Epub 2019 May 6. PMID: 31062427
  • Kamayirese S, Maity S, Dieckman LM, Hansen LA, Lovas S. Optimizing Phosphopeptide Structures That Target 14-3-3ε in Cutaneous Squamous Cell Carcinoma. ACS omega. 2024 Jan 3;9(2):2719-2729. doi: 10.1021/acsomega.3c07740. eCollection 2024 Jan 16. PMID: 38250398