Abstract

The transforming growth factor (TGF)-Betas are potent growth inhibitors of normal mammary epithelial cells. Constitutive overexpression of TGF- Beta1 in mammary epithelium of transgenic mice prevents carcinogen- and oncogene-induced mammary tumors. In established breast cancer cell systems, however, tumor cell TGF-Betas foster host/tumor interactions which indirectly support the viability and/or progression of carcinomas. In addition, high levels of TGF-Betas in human breast tumors have been associated with poor patient outcome and a more malignant breast cancer phenotype. Thus, we hypothesize that the net effect of TGF-Betas changes during stochastic mammary epithelial carcinogenesis. This net effect depends on the balance between autocrine growth inhibition, prevalent in normal breast cells, and a more permissive yet indirect role in transformed cells, associated or not with loss of endogenous TGF-Beta receptors. This proposal will therefore attempt to define the timing and mechanisms by which TGF-Betas modulate mammary carcinogenesis and, later, the progression of established tumors. In the first Aim, we will develop a transgenic mouse model in which levels of mammary epithelial TGF-Beta1 expression can be temporally controlled. In the second Aim, we will use this model to examine the effect of conditional expression of breast epithelial TGF-Beta1 on early and late stages of mammary transformation and tumor progression induced by carcinogens. In the third Aim, by using temporally-regulated active TGF-Beta1 or TGF- Beta2 as well as antisense TGF-Beta 1 or TGF-Beta2 in transfected human breast cancer cell lines in nude mice, we will test the effect of overexpression or elimination of TGF-Betas.
The fourth Aim will dissect the paracrine interactions between tumor cells and host immune, endothelial, and stromal cells, which we propose may account for the net effect of TGF-Betas on mammary tumorigenesis. Finally, the fifth Aim will examine how tumor cell TGF-Betas enhance resistance of breast tumor cells to chemotherapeutic drugs perhaps through interactions with stromal cells and the extracellular matrix. The results from these studies will lead us to re-examine the dynamic role of TGF-Betas in progressive mammary transformation and, on the basis, the conception of optimal chemoprevention strategies. In addition, a marked alteration in the natural history and drug resistance of experimental tumors by elimination of tumor cell TGF-Betas would suggest these molecules as rational and testable targets for novel antitumor interventions in patients with breast cancer.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Cancer Institute (NCI)
Type
Research Project (R01)
Project #
5R01CA062212-06
Application #
6150162
Study Section
Special Emphasis Panel (ZRG2-PTHB (01))
Program Officer
Mohla, Suresh
Project Start
1995-04-10
Project End
2004-01-31
Budget Start
2000-02-01
Budget End
2001-01-31
Support Year
6
Fiscal Year
2000
Total Cost
$264,176
Indirect Cost

  Institution

Name
Vanderbilt University Medical Center
Department
Internal Medicine/Medicine
Type
Schools of Medicine
DUNS #
004413456
City
Nashville
State
TN
Country
United States
Zip Code
37212

  Publications

Deeken, John F; Beumer, Jan H; Anders, Nicole M et al. (2015) Preclinical assessment of the interactions between the antiretroviral drugs, ritonavir and efavirenz, and the tyrosine kinase inhibitor erlotinib. Cancer Chemother Pharmacol 76:813-9
Beumer, J H; Venkataramanan, R; Rudek, M A (2014) Pharmacotherapy in cancer patients with HIV/AIDS. Clin Pharmacol Ther 95:370-2
Rudek, Michelle A; Chang, Cathy Y; Steadman, Kenneth et al. (2014) Combination antiretroviral therapy (cART) component ritonavir significantly alters docetaxel exposure. Cancer Chemother Pharmacol 73:729-36
Bauer, Joshua A; Ye, Fei; Marshall, Clayton B et al. (2010) RNA interference (RNAi) screening approach identifies agents that enhance paclitaxel activity in breast cancer cells. Breast Cancer Res 12:R41
Wang, S E; Yu, Y; Criswell, T L et al. (2010) Oncogenic mutations regulate tumor microenvironment through induction of growth factors and angiogenic mediators. Oncogene 29:3335-48
Rexer, Brent N; Engelman, Jeffrey A; Arteaga, Carlos L (2009) Overcoming resistance to tyrosine kinase inhibitors: lessons learned from cancer cells treated with EGFR antagonists. Cell Cycle 8:18-22
Wang, Shizhen Emily; Hinow, Peter; Bryce, Nicole et al. (2009) A mathematical model quantifies proliferation and motility effects of TGF-? on cancer cells. Comput Math Methods Med 10:71-83
Wang, Shizhen Emily; Xiang, Bin; Zent, Roy et al. (2009) Transforming growth factor beta induces clustering of HER2 and integrins by activating Src-focal adhesion kinase and receptor association to the cytoskeleton. Cancer Res 69:475-82
Wang, Shizhen Emily; Xiang, Bin; Guix, Marta et al. (2008) Transforming growth factor beta engages TACE and ErbB3 to activate phosphatidylinositol-3 kinase/Akt in ErbB2-overexpressing breast cancer and desensitizes cells to trastuzumab. Mol Cell Biol 28:5605-20
Criswell, Tracy L; Dumont, Nancy; Barnett, Joey V et al. (2008) Knockdown of the transforming growth factor-beta type III receptor impairs motility and invasion of metastatic cancer cells. Cancer Res 68:7304-12

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