Abstract

MDM2 was initially identified and characterized as an oncogene in murine fibroblasts. It was later demonstrated that the mdm2gene was amplified in approximately 30 percentof soft tissue sarcomas, establishing its role in human cancer. The ability of MDM2 to bind, inactivate and facilitate degradation of the p53 tumor suppressor protein has been well characterized; but the transforming phenotype of MDM2 appears to be, at least in part, independent of p53. In contrast to this growth-promoting anti-apoptotic function of MDM2, a growth inhibitory phenotype has also been demonstrated, inconsistent with the action of an oncogene. In addition, novel data presented in this proposal demonstrate an apoptotic function that is also in contrast to its transforming potential. We propose to evaluate, in Aim 1, which domains of the MDM2 protein are necessary for its apoptotic function and whether the oncogenic alternatively spliced isoforms of MDM2 that are often found in human tumors, have deleted these regions.
In Aim 2 we will investigate the mechanism by which MDM2 induces apoptosis and in Aim 3 we will evaluate whether the alternatively spliced isoforms of MDM2 found in tumor cells influence MDM2-induced apoptosis or the cellular response to chemotherapeutic agents. We expect that data generated from this work will resolve some of the conflicting published reports with respect to MDM2 function and will determine the importance of full-length versus alternatively spliced isoforms of MDM2 in the cellular response to chemotherapeutic agents.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Cancer Institute (NCI)
Type
Research Project (R01)
Project #
1R01CA092401-01A1
Application #
6469446
Study Section
Experimental Therapeutics Subcommittee 1 (ET)
Program Officer
Blair, Donald G
Project Start
2002-03-05
Project End
2007-02-28
Budget Start
2002-03-05
Budget End
2003-02-28
Support Year
1
Fiscal Year
2002
Total Cost
$213,275
Indirect Cost

  Institution

Name
St. Jude Children's Research Hospital
Department
Type
DUNS #
067717892
City
Memphis
State
TN
Country
United States
Zip Code
38105

  Publications

Volk, Erin L; Schuster, Katja; Nemeth, Katie M et al. (2009) MDM2-A, a common Mdm2 splice variant, causes perinatal lethality, reduced longevity and enhanced senescence. Dis Model Mech 2:47-55
Volk, Erin L; Fan, Liying; Schuster, Katja et al. (2009) The MDM2-a splice variant of MDM2 alters transformation in vitro and the tumor spectrum in both Arf- and p53-null models of tumorigenesis. Mol Cancer Res 7:863-9
Schuster, Katja; Fan, Liying; Harris, Linda C (2007) MDM2 splice variants predominantly localize to the nucleoplasm mediated by a COOH-terminal nuclear localization signal. Mol Cancer Res 5:403-12
Schuster, Katja; Harris, Linda C (2007) Selection for mutations in the cDNAs of transgenic mice upon expression of an embryonic lethal protein. Transgenic Res 16:527-30
Taylor, Alan C; Schuster, Katja; McKenzie, Pamela P et al. (2006) Differential cooperation of oncogenes with p53 and Bax to induce apoptosis in rhabdomyosarcoma. Mol Cancer 5:53
Harris, L C (2005) MDM2 splice variants and their therapeutic implications. Curr Cancer Drug Targets 5:21-6
Bartel, Frank; Harris, Linda C; Wurl, Peter et al. (2004) MDM2 and its splice variant messenger RNAs: expression in tumors and down-regulation using antisense oligonucleotides. Mol Cancer Res 2:29-35
McKenzie, Pamela P; McPake, Christina R; Ashford, Amy A et al. (2002) MDM2 does not influence p53-mediated sensitivity to DNA-damaging drugs. Mol Cancer Ther 1:1097-104
Bartel, Frank; Taubert, Helge; Harris, Linda C (2002) Alternative and aberrant splicing of MDM2 mRNA in human cancer. Cancer Cell 2:9-15