Abstract

This is a competitive renewal application for CA57179, a grant that was funded for the past 4 years and three months as the result of an RFA related to prostate cancer (PCA). Currently, this grant supports a collaborative effort among faculty interested in cytogenetics, molecular biology, pathology, and urology. The renewal application represents a continued pursuit of selected previous goals. The focus of this study is the use of PCA tissues derived from surgery (a) to attempt to define the factors that control the growth of PCAs and may cause the marked differences in aggressiveness observed in different patients and (b) to use the information derived from these studies and from other laboratories to devise conditions that will permit us to grow PCAs from tissues resected from most PCA patients. Until recently, most PCA work in research laboratories has relied on three cell lines: PC-3, DU 145, and LNCaP. Two of these lines, PC-3 and DU 145, lack evidence of functioning androgen receptors and fail to make prostate specific antigen, quantitatively the most abundant protein product of prostatic epithelial cells. While a few other models of PCA have been developed, they are (a) not generally available and (b) still very limited in their reflection of the broad spectrum of disease seen in PCA. Little is understood about the control of growth in PCA. The usually lengthy (5-20 years) survival of patients with PCA makes PCA a disease in which the ability to grow the tumors of individual patients might have unusual long-term translational significance. If we are able to achieve our goals, this approach might make it possible to develop knowledge of specific patients tumors that would facilitate a more specifically targeted approach to gene therapy, therapy directed against specific tyrosine kinases, antineoplastic chemotherapy, and immunotherapy. The long survival of these patients might allow one to refine these approaches to specific tumors before patients experience the protracted and severe bone pain that afflicts the majority of patients whose deaths are caused by prostate cancer.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Cancer Institute (NCI)
Type
Research Project (R01)
Project #
5R01CA057179-10
Application #
6475794
Study Section
Special Emphasis Panel (ZRG2-MEP (02))
Program Officer
Tricoli, James
Project Start
1992-07-23
Project End
2003-11-30
Budget Start
2001-12-01
Budget End
2003-11-30
Support Year
10
Fiscal Year
2002
Total Cost
$378,787
Indirect Cost

  Institution

Name
Case Western Reserve University
Department
Pathology
Type
Schools of Medicine
DUNS #
077758407
City
Cleveland
State
OH
Country
United States
Zip Code
44106

  Publications

Wu, Yi-Mi; Robinson, Dan R; Kung, Hsing-Jien (2004) Signal pathways in up-regulation of chemokines by tyrosine kinase MER/NYK in prostate cancer cells. Cancer Res 64:7311-20
Lee, Li-Fen; Louie, Maggie C; Desai, Sonal J et al. (2004) Interleukin-8 confers androgen-independent growth and migration of LNCaP: differential effects of tyrosine kinases Src and FAK. Oncogene 23:2197-205
Pretlow, Theresa P; Edelmann, Winfried; Kucherlapati, Raju et al. (2003) Spontaneous aberrant crypt foci in Apc1638N mice with a mutant Apc allele. Am J Pathol 163:1757-63
Yustein, Jason T; Xia, Liang; Kahlenburg, J Michelle et al. (2003) Comparative studies of a new subfamily of human Ste20-like kinases: homodimerization, subcellular localization, and selective activation of MKK3 and p38. Oncogene 22:6129-41
Xia, Liang; Robinson, Dan; Ma, Ai-Hong et al. (2002) Identification of human male germ cell-associated kinase, a kinase transcriptionally activated by androgen in prostate cancer cells. J Biol Chem 277:35422-33
Tepper, Clifford G; Boucher, David L; Ryan, Philip E et al. (2002) Characterization of a novel androgen receptor mutation in a relapsed CWR22 prostate cancer xenograft and cell line. Cancer Res 62:6606-14
Mousses, Spyro; Bubendorf, Lukas; Wagner, Urs et al. (2002) Clinical validation of candidate genes associated with prostate cancer progression in the CWR22 model system using tissue microarrays. Cancer Res 62:1256-60
Hao, X P; Pretlow, T G; Rao, J S et al. (2001) Inducible nitric oxide synthase (iNOS) is expressed similarly in multiple aberrant crypt foci and colorectal tumors from the same patients. Cancer Res 61:419-22
Hao, X P; Pretlow, T G; Rao, J S et al. (2001) Beta-catenin expression is altered in human colonic aberrant crypt foci. Cancer Res 61:8085-8
Mousses, S; Wagner, U; Chen, Y et al. (2001) Failure of hormone therapy in prostate cancer involves systematic restoration of androgen responsive genes and activation of rapamycin sensitive signaling. Oncogene 20:6718-23

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