Abstract

Although considerable evidence from chemical carcinogenesis experiments using mouse skin has established that the activation of the cellular Harvey ras (rasH) gene at codon 61 occurs frequently as an initiating event in this model, questions remain as to what additional events are required for subsequent stages that eventually lead to malignant conversion. Recent in vitro studies indicate that activated fos oncogenes can cooperate with the rasH oncogene in the malignant conversion of mouse epidermal cells. However, these in vitro systems cannot determine the influence of factors known to effect carcinogenesis in vivo such as blood supply, an intact immune system, humoral and cell-mediated growth controls, and physical barriers to cell growth. The ability to target the expression of genes with oncogenic potential to the epidermis of mice would allow the development of a genetically programmed in vivo model of skin carcinogenesis. Preliminary evidence is presented in this proposal documenting the feasibility of targeting gene expression to the epidermis of transgenic mice by the use of regulatory sequences of a keratin gene which are expressed exclusively in the epidermis at a late stage of development and in cells with proliferative potential. Through the use of this unique targeting ability, the oncogenic potential of expression of the v-rasH and v-fos oncogenes in the epidermis of mice as well as effects on the proliferation and differentiation states of epidermal cells will be determined. The availability of strains of mice expressing individual oncogenes will allow mating experiments that will determine if these genes act synergistically with each other during different stages of carcinogenesis or with other genes with oncogenic potential, which have previously been shown to transform epidermal cells in vitro. Due to the accessibility of the epidermis, it will also be possible to determine the potential role of chemical and physical carcinogens as well as tumor promoters in this process. Finally, differentiation-state specific promoters will be used to determine the effects of oncogenes on post- mitotic epidermal cells. The production of transgenic mice which exclusively express oncogenes in the skin could be useful for screening environmental agents to detect carcinogen or tumor promoters, for defining new compounds to act as cancer chemopreventive agents, and to develop insights into a variety of diseases of the skin which are associated with abnormal regulation of growth.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Cancer Institute (NCI)
Type
Research Project (R01)
Project #
5R01CA052607-02
Application #
3197399
Study Section
Chemical Pathology Study Section (CPA)
Project Start
1990-08-01
Project End
1993-07-31
Budget Start
1991-08-01
Budget End
1992-07-31
Support Year
2
Fiscal Year
1991
Total Cost
Indirect Cost

  Institution

Name
Baylor College of Medicine
Department
Type
Schools of Medicine
DUNS #
074615394
City
Houston
State
TX
Country
United States
Zip Code
77030

  Publications

Yang, N; Leung, E L-H; Liu, C et al. (2017) INTU is essential for oncogenic Hh signaling through regulating primary cilia formation in basal cell carcinoma. Oncogene 36:4997-5005
Lee, Sangjun; Rodriguez-Villanueva, Julio; McDonnell, Timothy (2017) Restrained Terminal Differentiation and Sustained Stemness in Neonatal Skin by Ha-Ras and Bcl-2. Am J Dermatopathol 39:199-203
Liu, Ying; Snedecor, Elizabeth R; Zhang, Xu et al. (2016) Correction of Hair Shaft Defects through Allele-Specific Silencing of Mutant Krt75. J Invest Dermatol 136:45-51
Riemondy, Kent; Wang, Xiao-jing; Torchia, Enrique C et al. (2015) MicroRNA-203 represses selection and expansion of oncogenic Hras transformed tumor initiating cells. Elife 4:
Torchia, Enrique C; Zhang, Lei; Huebner, Aaron J et al. (2013) Aurora kinase-A deficiency during skin development impairs cell division and stratification. J Invest Dermatol 133:78-86
White, Ruth A; Neiman, Jill M; Reddi, Anand et al. (2013) Epithelial stem cell mutations that promote squamous cell carcinoma metastasis. J Clin Invest 123:4390-404
Torchia, E C; Caulin, C; Acin, S et al. (2012) Myc, Aurora Kinase A, and mutant p53(R172H) co-operate in a mouse model of metastatic skin carcinoma. Oncogene 31:2680-90
Chen, Jiang; Roop, Dennis R (2012) Mimicking hair disorders by genetic manipulation of organ-cultured human hair follicles. J Invest Dermatol 132:2312-2314
Terzian, Tamara; Dumble, Melissa; Arbab, Farinaz et al. (2011) Rpl27a mutation in the sooty foot ataxia mouse phenocopies high p53 mouse models. J Pathol 224:540-52
Honeycutt, Kimberly A; Waikel, Rebekah L; Koster, Maranke I et al. (2010) The effect of c-myc on stem cell fate influences skin tumor phenotype. Mol Carcinog 49:315-9

Showing the most recent 10 out of 58 publications