Abstract

We have developed a unique transgenic mouse model system in which 100% of female mice carrying the C3(1)/Tag transgene develop mammary cancer and male mice develop lesions in the prostate ranging from prostatic intraepithelial neoplasia to invasive carcinomas. This model offers the opportunity to study the multistep progression of tumorigenesis in these two important organ systems and determine molecular events which may be common or unique to mammary and prostate cancer development. We have identified several oncogenes and suppressor genes whose expression is altered during tumorigenesis. The ras family of oncogenes may be particularly important in this process in both tumor types. In addition, comparative genomic hybridization has revealed specific chromosomal regions which are amplified during mammary cancer formation and we are currently studying these amplicfications as they relate to tumor progression. Genome wide LOH studies have also been initiated. Our work has focused on understanding shifts in the balance between cell proliferation and apoptosis during tumor progression in vivo. Changes in the levels of expression of various regulators of the cell cycle have been characterized and related to the functional status of key gatekeepers of the cell cycle. Alterations in levels of apoptosis during mammary tumorigenesis have also been analyzed and have revealed that there is a dramatic increase in apoptosis during the transition from the normal to the hyperplastic stage. However, this critical protective response is lost as the cells progress from hyperplasia to invasive mammary carcinomas. The regulation of apoptosis in the prostate during tumorigenesis does not appear to follow a similar course as that in the mammary gland, but apoptosis levels continue to rise during prostate cancer development. We are currently seeking to understand what molecular alterations may contribute to the regulation of apoptosis in these tumors. Our work has also demonstrated that hormone manipulations and pregnancy may affect the natural history of the disease processes in these transgenic mice which may, in part, result from alterations in the expression of particular oncogenes and suppressor genes. We are also attempting to determine whether the in vivo immune response against mammary and prostate tumors can be augmented and used as a model of immunotherapy in these animals. Although various efforts have been unsuccessful in breaking immune tolerance in these mice, the combination of Il-2 and IL-12 has resulted in significant mammary tumor regression. This may, in part, be mediated by immune and non-immune mechanisms which we are attempting to elucidate.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Cancer Institute (NCI)
Type
Intramural Research (Z01)
Project #
1Z01BC005740-05
Application #
6160960
Study Section
Special Emphasis Panel (LMO)
Project Start
Project End
Budget Start
Budget End
Support Year
5
Fiscal Year
1997
Total Cost
Indirect Cost

  Institution

Name
National Cancer Institute Division of Basic Sciences
Department
Type
DUNS #
City
State
Country
United States
Zip Code

  Publications

Abate-Shen, Cory; Brown, Powel H; Colburn, Nancy H et al. (2008) The untapped potential of genetically engineered mouse models in chemoprevention research: opportunities and challenges. Cancer Prev Res (Phila) 1:161-6
Zhang, Mei; Behbod, Fariba; Atkinson, Rachel L et al. (2008) Identification of tumor-initiating cells in a p53-null mouse model of breast cancer. Cancer Res 68:4674-82
Calvo, A; Catena, R; Noble, M S et al. (2008) Identification of VEGF-regulated genes associated with increased lung metastatic potential: functional involvement of tenascin-C in tumor growth and lung metastasis. Oncogene 27:5373-84
Barkan, Dalit; Kleinman, Hynda; Simmons, Justin L et al. (2008) Inhibition of metastatic outgrowth from single dormant tumor cells by targeting the cytoskeleton. Cancer Res 68:6241-50
Ohta, Shoichiro; Lai, Edwin W; Morris, John C et al. (2008) Metastasis-associated gene expression profile of liver and subcutaneous lesions derived from mouse pheochromocytoma cells. Mol Carcinog 47:245-51
Huh, Jung-Im; Qiu, Ting Hu; Chandramouli, Gadisetti V R et al. (2007) 2-methoxyestradiol induces mammary gland differentiation through amphiregulin-epithelial growth factor receptor-mediated signaling: molecular distinctions from the mammary gland of pregnant mice. Endocrinology 148:1266-77
Shoushtari, Alexander N; Michalowska, Aleksandra M; Green, Jeffrey E (2007) Comparing genetically engineered mouse mammary cancer models with human breast cancer by expression profiling. Breast Dis 28:39-51
Deeb, Kristin K; Michalowska, Aleksandra M; Yoon, Cheol-Yong et al. (2007) Identification of an integrated SV40 T/t-antigen cancer signature in aggressive human breast, prostate, and lung carcinomas with poor prognosis. Cancer Res 67:8065-80
Datta, Sonal; Hoenerhoff, Mark J; Bommi, Prashant et al. (2007) Bmi-1 cooperates with H-Ras to transform human mammary epithelial cells via dysregulation of multiple growth-regulatory pathways. Cancer Res 67:10286-95
Oakes, S R; Robertson, F G; Kench, J G et al. (2007) Loss of mammary epithelial prolactin receptor delays tumor formation by reducing cell proliferation in low-grade preinvasive lesions. Oncogene 26:543-53

Showing the most recent 10 out of 41 publications