Abstract

The long term objective of these studies is to use transgenic mice to test the hypothesis that andromedins such as keratinocyte growth factor (KGF; FGF-7) and other members of the fibroblast growth factor (FGF) family can regulate the growth and metastasis of prostatic cancer in vivo. To meet these objectives, the rat probasin (PB) gene promoter will be used to target the expression of KGF, basic fibroblast growth factor (FGF-2) and FGF-receptor (FGFR) dominant-negative mutants (FGFRdnm) specifically to prostatic epithelium in transgenic mice. Dr. Greenberg, together with collaborators, has developed the rat probasin gene promoter system to direct expression of heterologous genes specifically to the prostate in transgenic mice in a hormonally- and developmentally- regulated fashion. Furthermore, in order to develop a transgenic animal prostate cancer model system, mice carrying a PB promoter - SV40 T antigen fusion transgene (PB-Tag) have recently been generated in Dr. Greenberg's laboratory. These mice develop prostatic epithelial hyperplasia by 6 months of age and specific emphasis will be placed upon the use of these established lines of mice in these studies. The rationale for these studies is based on the implication of KGF as an andromedin that can influence, via stromal-epithelial interactions, the differentiation, growth and development of the prostate gland, and that targeting KGF over expression to prostatic epithelium of transgenic mice will deregulate normal prostatic development via an autocrine stimulatory pathway that will lead to prostatic epithelial hyperplasia in these animals. In similar fashion, FGF2 will be targeted to the prostatic epithelium of transgenic mice, since it has been shown to be activated in stromal-independent malignant prostatic epithelial cells derived from Dunning tumors. When the PB-KGF and PB-FGF2 mice are crossed to the PB- Tag mice, it can be determined whether KGF or FGF2 over expression contribute to the development of adenocarcinoma of the prostate in vivo, with subsequent metastasis. Targeted expression of specific dominant- negative FGFR mutants in prostatic epithelium will be used to distinguish between the actions of FGF-1, FGF-2 and KGF on normal prostate development. In these later studies, the PB promoter will be used to target expression of FGFR1 (IIIc) and FGFR2 (IIIb) dominant-negative mutants (dnm) to the prostate epithelium in transgenic mice to abrogate the stromal-epithelial actions mediated by FGF-1/FGF-2 or FGF-1/KGF, respectively. When the PB-FGFRdnm mice are crossed to PB-Tag mice, it can be determined which of the andromedin signals, ablated singly or in combination, inhibits the development of prostatic epithelial hyperplasia. It is anticipated that these studies will also provide the basis for the rational design, development and testing of novel gene- based therapies for prostate cancer.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Cancer Institute (NCI)
Type
Research Project (R01)
Project #
5R01CA064851-04
Application #
2429822
Study Section
Special Emphasis Panel (SRC (88))
Project Start
1994-08-15
Project End
1998-05-31
Budget Start
1997-06-01
Budget End
1998-05-31
Support Year
4
Fiscal Year
1997
Total Cost
Indirect Cost

  Institution

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

  Publications

Huss, Wendy J; Gray, Danny R; Tavakoli, Keyvan et al. (2007) Origin of androgen-insensitive poorly differentiated tumors in the transgenic adenocarcinoma of mouse prostate model. Neoplasia 9:938-50
Winter, S F; Acevedo, V D; Gangula, R D et al. (2007) Conditional activation of FGFR1 in the prostate epithelium induces angiogenesis with concomitant differential regulation of Ang-1 and Ang-2. Oncogene 26:4897-907
Huss, Wendy J; Gray, Danny R; Greenberg, Norman M et al. (2005) Breast cancer resistance protein-mediated efflux of androgen in putative benign and malignant prostate stem cells. Cancer Res 65:6640-50
Huss, Wendy J; Lai, Lihua; Barrios, Roberto J et al. (2004) Retinoic acid slows progression and promotes apoptosis of spontaneous prostate cancer. Prostate 61:142-52
Jin, Chengliu; McKeehan, Kerstin; Guo, Wei et al. (2003) Cooperation between ectopic FGFR1 and depression of FGFR2 in induction of prostatic intraepithelial neoplasia in the mouse prostate. Cancer Res 63:8784-90
Hernandez, Inmaculada; Maddison, Lisette A; Wei, Yongli et al. (2003) Prostate-specific expression of p53(R172L) differentially regulates p21, Bax, and mdm2 to inhibit prostate cancer progression and prolong survival. Mol Cancer Res 1:1036-47
Huss, Wendy J; Barrios, Roberto J; Greenberg, Norman M (2003) SU5416 selectively impairs angiogenesis to induce prostate cancer-specific apoptosis. Mol Cancer Ther 2:611-6
Huss, Wendy J; Barrios, Roberto J; Foster, Barbara A et al. (2003) Differential expression of specific FGF ligand and receptor isoforms during angiogenesis associated with prostate cancer progression. Prostate 54:8-16
Kazansky, Alexander V; Spencer, David M; Greenberg, Norman M (2003) Activation of signal transducer and activator of transcription 5 is required for progression of autochthonous prostate cancer: evidence from the transgenic adenocarcinoma of the mouse prostate system. Cancer Res 63:8757-62
Uzgare, Aarti R; Kaplan, Paula J; Greenberg, Norman M (2003) Differential expression and/or activation of P38MAPK, erk1/2, and jnk during the initiation and progression of prostate cancer. Prostate 55:128-39

Showing the most recent 10 out of 21 publications