Abstract

ARF is the second most commonly inactivated gene in human cancer. It prevents oncogenic transformation by activating p53-dependent growth arrest or apoptosis, primarily by sequestering the Mdm2 oncogene in nucleoli and blocking Mdm2-mediated degradation of p53. Recent findings indicate that 1) other factors are required for p53-dependent growth arrest, and 2) ARF can inhibit growth through other pathways that do not involve p53 or Mdm2. This proposal aims to identify and characterize additional mediators and inhibitors of ARF-induced growth arrest. The ultimate objective is to delineate mechanisms of growth suppression by ARF.
Aim 1 will determine the role of identified ARF binding proteins, Mdm2 and two novel proteins (Parfs) that associate with ARF in nucleoli, in ARF-mediated growth suppression. The mechanism by which Mdm2 antagonizes p53-independent activities of ARF will be defined by assaying ARF function in p53/Mdm2-null cells expressing Mdm2 mutants. Interaction domains within Parfs and ARF will be identified through mutagenesis, while the hypothesis that Parfs are growth inhibitors required for ARF-induced growth arrest will be tested in cells which overexpress or lack functional Parfs.
Aim 2 will define the role of two ARE-associated phosphoproteins, p58 and p65, in ARF signaling pathways. We will test if p58 and p65 are phosphorylated in response to ARF and if they selectively bind to growth inhibitory forms of ARF in a p53-dependent manner. The identities of p58 and p65 will be determined by testing if p58 is the 58 kDa form of Mdm2 (since it is a phosphoprotein) and biochemically purifying ARF-associated proteins of 50-70 kDa by affinity chromatography.
In Aim 3, an unbiased genetic screen using retroviral cDNA libraries will be performed to identify and characterize novel genes that override p53-dependent and p53-independent ARF-induced arrest. These studies will advance our fundamental understanding of ARF function in the different signaling pathways, and as such, provide knowledge that is relevant to developing appropriate anticancer strategies.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Cancer Institute (NCI)
Type
Research Project (R01)
Project #
1R01CA090367-01A1
Application #
6439385
Study Section
Cell Development and Function Integrated Review Group (CDF)
Program Officer
Mietz, Judy
Project Start
2002-04-01
Project End
2007-03-31
Budget Start
2002-04-01
Budget End
2003-03-31
Support Year
1
Fiscal Year
2002
Total Cost
$258,481
Indirect Cost

  Institution

Name
University of Iowa
Department
Pharmacology
Type
Schools of Medicine
DUNS #
041294109
City
Iowa City
State
IA
Country
United States
Zip Code
52242

  Publications

Huang, J; Stewart, A; Maity, B et al. (2014) RGS6 suppresses Ras-induced cellular transformation by facilitating Tip60-mediated Dnmt1 degradation and promoting apoptosis. Oncogene 33:3604-11
Reed, Sara M; Hagen, Jussara; Tompkins, Van S et al. (2014) Nuclear interactor of ARF and Mdm2 regulates multiple pathways to activate p53. Cell Cycle 13:1288-98
Hagen, Jussara; Muniz, Viviane P; Falls, Kelly C et al. (2014) RABL6A promotes G1-S phase progression and pancreatic neuroendocrine tumor cell proliferation in an Rb1-dependent manner. Cancer Res 74:6661-70
Zhang, Xuefeng; Hagen, Jussara; Muniz, Viviane P et al. (2013) RABL6A, a novel RAB-like protein, controls centrosome amplification and chromosome instability in primary fibroblasts. PLoS One 8:e80228
Muniz, Viviane P; Askeland, Ryan W; Zhang, Xuefeng et al. (2013) RABL6A Promotes Oxaliplatin Resistance in Tumor Cells and Is a New Marker of Survival for Resected Pancreatic Ductal Adenocarcinoma Patients. Genes Cancer 4:273-84
Muniz, Viviane Palhares; Barnes, J Matthew; Paliwal, Seema et al. (2011) The ARF tumor suppressor inhibits tumor cell colonization independent of p53 in a novel mouse model of pancreatic ductal adenocarcinoma metastasis. Mol Cancer Res 9:867-77
di Tommaso, Anne; Hagen, Jussara; Tompkins, Van et al. (2009) Residues in the alternative reading frame tumor suppressor that influence its stability and p53-independent activities. Exp Cell Res 315:1326-35
Hagen, Jussara; Tompkins, Van; Dudakovic, Amel et al. (2008) Generation and characterization of monoclonal antibodies to NIAM: a nuclear interactor of ARF and Mdm2. Hybridoma (Larchmt) 27:159-66
Tompkins, Van S; Hagen, Jussara; Frazier, April A et al. (2007) A novel nuclear interactor of ARF and MDM2 (NIAM) that maintains chromosomal stability. J Biol Chem 282:1322-33
Korgaonkar, Chandrashekhar; Hagen, Jussara; Tompkins, Van et al. (2005) Nucleophosmin (B23) targets ARF to nucleoli and inhibits its function. Mol Cell Biol 25:1258-71

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