PROMID ED. The tumor suppressor ARF is mutated or deregulated (by hypermethylation) in a variety of cancers. ARF is critical in the context of oncogenic activation and stress-induced senescence. It is believed that, following oncogenic activation, ARF induces senescence or apoptosis to protect cells from tumorigenic consequences. How does ARF dominate over the oncogenes? Previous studies suggested that the function of ARF is mediated through p53. However, recent genetic analyses provided evidence for additional p53- independent activities of ARF. Studies described in this proposal are based on the observation that ARF regulates multiple proliferation-associated proteins. ARF induces proteolysis of E2F1 and DP1; and sequesters c-Myc in the nucleolus. Oncogenic Ha-Ras, which induces cellular senescence in mouse embryonic fibroblasts by stimulating the expression of ARF, causes a relocalization of DP1 in the nucleolus. The objectives of the proposal are to investigate the mechanism by which ARF regulates E2F/DP1 and test the hypothesis that the E2F/DPl-regulatory function is related to the tumor suppression and the senescence-induction functions of ARF. Since the E2F-family of factors (E2Fs) are key mediators of oncogenic activation and cell-proliferation, our studies will establish a novel and potentially dominant mechanism of tumor suppression. Also, the studies will establish a role of E2F/DPl-regulation in cellular senescence induced by ARF. The hypotheses stated above will be investigated through the following aims: 1. Is the DP1- regulatory activity required for the cell cycle-inhibition by ARF? 2. How does ARF induce proteolysis of DP1 and E2FI? 3. What is the role of the E2F/DPl-regulation in the ARF-induced tumor suppression and senescence?

Agency
National Institute of Health (NIH)
Institute
National Cancer Institute (NCI)
Type
Research Project (R01)
Project #
3R01CA100035-05S1
Application #
7631964
Study Section
Tumor Cell Biology Study Section (TCB)
Program Officer
Ogunbiyi, Peter
Project Start
2004-07-01
Project End
2010-05-31
Budget Start
2008-06-01
Budget End
2010-05-31
Support Year
5
Fiscal Year
2008
Total Cost
$37,228
Indirect Cost
Name
University of Illinois at Chicago
Department
Biochemistry
Type
Schools of Medicine
DUNS #
098987217
City
Chicago
State
IL
Country
United States
Zip Code
60612
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Dominguez-Brauer, Carmen; Brauer, Patrick M; Chen, Yi-Ju et al. (2010) Tumor suppression by ARF: gatekeeper and caretaker. Cell Cycle 9:86-9
Petrovic, Vladimir; Costa, Robert H; Lau, Lester F et al. (2010) Negative regulation of the oncogenic transcription factor FoxM1 by thiazolidinediones and mithramycin. Cancer Biol Ther 9:1008-16
Park, Hyun Jung; Carr, Janai R; Wang, Zebin et al. (2009) FoxM1, a critical regulator of oxidative stress during oncogenesis. EMBO J 28:2908-18
Dominguez-Brauer, Carmen; Chen, Yi-Ju; Brauer, Patrick M et al. (2009) ARF stimulates XPC to trigger nucleotide excision repair by regulating the repressor complex of E2F4. EMBO Rep 10:1036-42
Park, H J; Wang, Z; Costa, R H et al. (2008) An N-terminal inhibitory domain modulates activity of FoxM1 during cell cycle. Oncogene 27:1696-704
Wang, I-Ching; Chen, Yi-Ju; Hughes, Douglas E et al. (2008) FoxM1 regulates transcription of JNK1 to promote the G1/S transition and tumor cell invasiveness. J Biol Chem 283:20770-8
Park, Hyun Jung; Costa, Robert H; Lau, Lester F et al. (2008) Anaphase-promoting complex/cyclosome-CDH1-mediated proteolysis of the forkhead box M1 transcription factor is critical for regulated entry into S phase. Mol Cell Biol 28:5162-71
Tan, Yongjun; Raychaudhuri, Pradip; Costa, Robert H (2007) Chk2 mediates stabilization of the FoxM1 transcription factor to stimulate expression of DNA repair genes. Mol Cell Biol 27:1007-16
Datta, Abhishek; Sen, Jayita; Hagen, Jussara et al. (2005) ARF directly binds DP1: interaction with DP1 coincides with the G1 arrest function of ARF. Mol Cell Biol 25:8024-36

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