Abstract

Beta-catenin is a component of the Wnt signaling pathway that is disrupted by oncogenic mutations in many cancer types. We first demonstrated that beta-catenin was mutated in a subset of prostate cancer specimens. Emerging data from other laboratories have confirmed our findings and identified mutations in other components of the Wnt signaling pathway such as APC in prostate cancer. In prostate cancer cells mutant beta-catenin can potentiate androgen receptor (AR) signaling and broaden ligand specificity. Since increased AR activity and response to an expanded range of steroid hormones is a hallmark of advanced prostate cancer, beta-catenin mutations appear to be an additional mechanism by which prostate cancer cells enhance AR activity. This finding may have clinical implications for determining apropriate second-line hormonal therapy for prostate cancer patients. We now propose to elucidate the details of the direct intermolecular interactions between beta-catenin and androgen receptor. Our preliminary data indicate that beta-catenin binds to the AR ligand-binding domain. Moreover, LXXLL peptide motifs in the beta-catenin armadillo repeat region that resemble motifs in p160 steroid hormone coactivator molecules are important for beta-catenin/ AR interaction. Using a mammalian two-hybrid assay we will determine the regions of androgen receptor bound by beta-catenin and we will determine the regions of beta-catenin that bind androgen receptor. Using recombinant proteins we will demonstrate the direct physical interaction between AR and beta-catenin. We will also determine the ligand-dependence of this binding and the spectrum of ligands that support the interaction. We will determine if beta-catenin affects the interaction of androgen receptor with ligand by measuring dissociation of different ligands from androgen receptor. Lastly, we will determine the mechanism by which beta-catenin synergizes with p160 steroid receptor coactivator proteins to increase AR activity. These experiments will clearly establish as interaction between the Wnt signaling and steroid receptor pathways and thereby describe a new mechanism for prostate cancer progression, which is often dependent on enhancement of AR activity.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Cancer Institute (NCI)
Type
Research Project (R01)
Project #
5R01CA096854-02
Application #
6611392
Study Section
Metabolic Pathology Study Section (MEP)
Program Officer
Macleod, Carol L
Project Start
2002-07-15
Project End
2006-06-30
Budget Start
2003-07-01
Budget End
2004-06-30
Support Year
2
Fiscal Year
2003
Total Cost
$288,587
Indirect Cost

  Institution

Name
Georgetown University
Department
Type
Organized Research Units
DUNS #
049515844
City
Washington
State
DC
Country
United States
Zip Code
20057

  Publications

Song, Liang-Nian; Gelmann, Edward P (2008) Silencing mediator for retinoid and thyroid hormone receptor and nuclear receptor corepressor attenuate transcriptional activation by the beta-catenin-TCF4 complex. J Biol Chem 283:25988-99
Chen, Mengqian; Chen, Li-Mei; Lin, Chen-Yong et al. (2008) The epidermal growth factor receptor (EGFR) is proteolytically modified by the Matriptase-Prostasin serine protease cascade in cultured epithelial cells. Biochim Biophys Acta 1783:896-903
Shand, Randi L; Gelmann, Edward P (2006) Molecular biology of prostate-cancer pathogenesis. Curr Opin Urol 16:123-31
Zheng, S Lilly; Ju, Jeong-ho; Chang, Bao-li et al. (2006) Germ-line mutation of NKX3.1 cosegregates with hereditary prostate cancer and alters the homeodomain structure and function. Cancer Res 66:69-77
Song, Liang-Nian; Gelmann, Edward P (2005) Interaction of beta-catenin and TIF2/GRIP1 in transcriptional activation by the androgen receptor. J Biol Chem 280:37853-67
Mani, Aparna; Gelmann, Edward P (2005) The ubiquitin-proteasome pathway and its role in cancer. J Clin Oncol 23:4776-89
Gelmann, Edward P; Semmes, O John (2004) Expression of genes and proteins specific for prostate cancer. J Urol 172:S23-6; discussion S26-7
Song, Liang-Nian; Coghlan, Meghan; Gelmann, Edward P (2004) Antiandrogen effects of mifepristone on coactivator and corepressor interactions with the androgen receptor. Mol Endocrinol 18:70-85
Song, Liang-Nian; Herrell, Roger; Byers, Stephen et al. (2003) Beta-catenin binds to the activation function 2 region of the androgen receptor and modulates the effects of the N-terminal domain and TIF2 on ligand-dependent transcription. Mol Cell Biol 23:1674-87
Gelmann, Edward P (2002) Molecular biology of the androgen receptor. J Clin Oncol 20:3001-15