Abstract

Signal transducers and activators of transcription (STATs) are transcription factors that were discovered as key signaling components involved in mediating responses to cytokine stimulation. Increasingly, evidence has been accumulating that points to the movement of STAT proteins in oncogenesis. Previously, we made the original observation that one STAT family member, STAT3, is constitutively activated in fibroblast cell lines transformed by the Src oncoprotein. Studies with dominant-negative STAT3 proteins further demonstrate that activation of STAT3 signaling by the Src oncoprotein leads to specific regulation of gene expression and is required for cell transformation. In addition, STAT3 signaling is activated with high frequency in cell lines and by others suggest that STAT3 signaling has an important role in breast carcinoma and various lymphoid malignancies. In this project, we propose to test the hypothesis that specific inhibitors of STAT3 signaling will reduce tumorigenicity in relevant human tumor models without inducing significant toxicity. This goal will be pursued through the following specific aims: (1) To identify candidate lead peptides that potentially disrupt STAT3 function, we will screen linear and cyclic peptide phage display libraries for sequences that bind to STAT3 protein. (2) Candidate lead peptides, together with peptidomimetics and combinatorial chemical libraries synthesized in Project 1, will be tested in vitro assays for their abilities to disrupt STAT3 dimerization and DNA- binding activity. Information on activities peptides and other compounds will be fed back to Project 1 for lead optimization. (3) Promising compounds will be assayed for their abilities to disrupt STAT3 signaling in intact cells and to block cell transformation by the Src oncoprotein. (4) Using cell culture and animal models of human cancers where STAT3 is frequently activated, compounds that disrupt STAT3 signaling will be evaluated for their anti-tumor efficacy and toxicity. In addition, these STAT3 disruptors will be used to explore the biological mechanisms of how STAT3 contributes to oncogenesis, including regulation of cell proliferation and apoptosis. Results of these studies will advance our understanding of the role of STAT3 in human cancer and assess the therapeutic potential of STAT3 inhibitors as novel anti-cancer drugs.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Cancer Institute (NCI)
Type
Research Program Projects (P01)
Project #
5P01CA078038-03
Application #
6435840
Study Section
Special Emphasis Panel (ZCA1)
Project Start
2001-03-09
Project End
2002-02-28
Budget Start
1998-10-01
Budget End
1999-09-30
Support Year
3
Fiscal Year
2001
Total Cost
$197,196
Indirect Cost

  Institution

Name
University of South Florida
Department
Type
DUNS #
City
Tampa
State
FL
Country
United States
Zip Code
33612

  Publications

Kayser-Bricker, Katherine J; Glenn, Matthew P; Lee, Sang Hoon et al. (2009) Non-peptidic substrate-mimetic inhibitors of Akt as potential anti-cancer agents. Bioorg Med Chem 17:1764-71
Gunning, Patrick T; Glenn, Matthew P; Siddiquee, Khandaker A Z et al. (2008) Targeting protein-protein interactions: suppression of Stat3 dimerization with rationally designed small-molecule, nonpeptidic SH2 domain binders. Chembiochem 9:2800-3
Gustafsdottir, Sigrun M; Wennstrom, Stefan; Fredriksson, Simon et al. (2008) Use of proximity ligation to screen for inhibitors of interactions between vascular endothelial growth factor A and its receptors. Clin Chem 54:1218-25
Engelman, Robert W; Jackson, Rosalind J; Coppola, Domenico et al. (2007) Loss of nuclear p21(Cip1/WAF1) during neoplastic progression to metastasis in gamma-irradiated p21 hemizygous mice. Exp Mol Pathol 82:234-44
Gunning, Patrick T; Katt, William P; Glenn, Matthew et al. (2007) Isoform selective inhibition of STAT1 or STAT3 homo-dimerization via peptidomimetic probes: structural recognition of STAT SH2 domains. Bioorg Med Chem Lett 17:1875-8
Xu, Qing; Briggs, Jon; Park, Sungman et al. (2005) Targeting Stat3 blocks both HIF-1 and VEGF expression induced by multiple oncogenic growth signaling pathways. Oncogene 24:5552-60
Nefedova, Yulia; Nagaraj, Srinivas; Rosenbauer, Amsler et al. (2005) Regulation of dendritic cell differentiation and antitumor immune response in cancer by pharmacologic-selective inhibition of the janus-activated kinase 2/signal transducers and activators of transcription 3 pathway. Cancer Res 65:9525-35
Nefedova, Yulia; Cheng, Pingyan; Gilkes, Daniele et al. (2005) Activation of dendritic cells via inhibition of Jak2/STAT3 signaling. J Immunol 175:4338-46
Sun, Jiazhi; Blaskovich, Michelle A; Jove, Richard et al. (2005) Cucurbitacin Q: a selective STAT3 activation inhibitor with potent antitumor activity. Oncogene 24:3236-45
Sun, Jiazhi; Wang, De-An; Jain, Rishi K et al. (2005) Inhibiting angiogenesis and tumorigenesis by a synthetic molecule that blocks binding of both VEGF and PDGF to their receptors. Oncogene 24:4701-9

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