Abstract

An understanding of oncogene activation during tumor progression would add to our knowledge of the molecular basis of neoplasia and could aid in terms of diagnosis, prevention and treatment of cancer. The unique mouse skin model of tumor progression in which there are defined stable intermediate stages and lesions will be used in these studies. Using this unique model and molecular biology techniques, genes which are activated by point mutation or over-expression during tumor progression will be identified and their functional role in tumorigenesis will be assessed. Alterations in the expression of known oncogenes will be studied by northern hybridization in tumor promoter dependent and independent papillomas, non-metastasizing and metastasizing squamous cell carcinomas compared to normal epidermis, as well as acutely and chronically tumor promoter treated epidermis. Changes in known cellular oncogene organization in terms of methylation, rearrangement and amplification will be studied in DNA isolated from these various lesions. To identify and clone genes that are responsible for acquisition of the """"""""initiated"""""""" or malignant phenotype by DNA transfection, genomic DNAs from carcinomas, papillomas and """"""""putatively initiated"""""""" cells will be co-transfected with the pSV2 neo plasmid into primary epidermal cells or """"""""putatively initiated"""""""" cells and/or papilloma cells. The method of suppressor rescue for isolation of eukaryotic genes using the supF fragment as a marker will be used to clone the gene(s). To identify which genes are upregulated during skin tumor progression, cDNA libraries, enriched for stage specific mRNAs by selective hybridization techniques, will be prepared and screened by dot hybridization for genes whose expression are stage specific. An attempt will be made to obtain full-length cDNA copies of these upregulated genes in an Okayama-Berg expression vector to determine the functional significance of the upregulated genes by transfection of normal epidermal cells, """"""""putatively initiated"""""""" cells and papilloma cells. If oncogenes either with or without homology to the known retroviral oncogenes are activated in the progression of chemically induced skin tumors in mice, this experimental approach will identify those genes.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Cancer Institute (NCI)
Type
Research Project (R01)
Project #
1R01CA040584-01
Application #
3180759
Study Section
Pathology B Study Section (PTHB)
Project Start
1985-07-01
Project End
1988-06-30
Budget Start
1985-07-01
Budget End
1986-06-30
Support Year
1
Fiscal Year
1985
Total Cost
Indirect Cost

  Institution

Name
University of Arizona
Department
Type
Schools of Medicine
DUNS #
City
Tucson
State
AZ
Country
United States
Zip Code
85722

  Publications

Demetriou, Manolis C; Kwei, Kevin A; Powell, Marianne B et al. (2008) Integrin A6 Cleavage in Mouse Skin Tumors. Open Cancer J 2:1-4
Zhang, Jack; Tsaprailis, George; Bowden, G Tim (2008) Nucleolin stabilizes Bcl-X L messenger RNA in response to UVA irradiation. Cancer Res 68:1046-54
Hanke, Neale T; Finch, Joanne S; Bowden, G Timothy (2008) Loss of catalase increases malignant mouse keratinocyte cell growth through activation of the stress activated JNK pathway. Mol Carcinog 47:349-60
Zhang, Jack; Bowden, G Tim (2007) Targeting Bcl-X(L) for prevention and therapy of skin cancer. Mol Carcinog 46:665-70
Finch, Joanne S; Tome, Margaret E; Kwei, Kevin A et al. (2006) Catalase reverses tumorigenicity in a malignant cell line by an epidermal growth factor receptor pathway. Free Radic Biol Med 40:863-75
Kwei, Kevin A; Finch, Joanne S; Ranger-Moore, James et al. (2006) The role of Rac1 in maintaining malignant phenotype of mouse skin tumor cells. Cancer Lett 231:326-38
Kwei, Kevin A; Finch, Joanne S; Thompson, Eric J et al. (2004) Transcriptional repression of catalase in mouse skin tumor progression. Neoplasia 6:440-8
Butts, Brent D; Kwei, Kevin A; Bowden, G Tim et al. (2003) Elevated basal reactive oxygen species and phospho-Akt in murine keratinocytes resistant to ultraviolet B-induced apoptosis. Mol Carcinog 37:149-57
Finch, S; Joseloff, E; Bowden, T (2002) JunB negatively regulates AP-1 activity and cell proliferation of malignant mouse keratinocytes. J Cancer Res Clin Oncol 128:3-10
Thompson, Eric J; MacGowan, Jacalyn; Young, Matthew R et al. (2002) A dominant negative c-jun specifically blocks okadaic acid-induced skin tumor promotion. Cancer Res 62:3044-7

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