Abstract

Previous work by our lab (and by other groups) has determined that Mdm2 is the master regulator of the p53 tumor suppressor during development and in multiple tissues of neonates and adults. Mdm2 binds with p53 to block the p53's ability to alter transcription. In addition, Mdm2-p53 binding also promotes p53 ubiquitination, nuclear export, and proteosomal degradation, thereby inhibiting all p53 activities within the cell. Through these mechanisms, Mdm2 negatively regulates the ability of p53 to suppress tumorigenesis, and amplification and/or overexpression of the MDM2 gene is observed in a very significant percentage of human cancers. In this proposal, we summarize the progress we have made in our previous studies on p53 regulation by Mdm2 and its homologue, Mdm4 (MdmX). We describe recent studies examining the effects of ATM- mediated phosphorylation of Mdm2 on the regulation of p53 stability and activity, and discuss the generation of new Mdm2 alleles in mice that are compromised in their capacity to be phosphorylated by the DNA damage effector kinases ATM, c-Abl, or Akt. Based upon the preliminary data we present, we propose to utilize these models to examine in vivo the effects of Mdm2 phosphorylation on Mdm2-p53 signaling and on p53's ability to govern cell growth, the DNA damage response, cell metabolism, and to suppress tumorigenesis. As with our previous in vivo studies, this proposed research should greatly increase our understanding of the functional roles of the Mdm2-p53 signaling axis in regulating cell growth and death, and should help identify new targets for the treatment of radiation sickness and cancer.

Public Health Relevance

Mdm2 is a key negative regulator of the p53 tumor suppressor. Although much has been learned from biochemical assays and transfection studies regarding Mdm2 inhibition of p53 and the effects of DNA damage-induced kinases on Mdm2 post-translational modifications, analysis of genetically modified mice has proven critical in substantiating or refuting the numerous and often conflicting models derived from previous cell-based studies. Analysis of genetically altered mice has also led to new theories regarding Mdm2 functions and the role of Mdm2-p53 signaling in cancer. In this proposal, we will analyze several new mouse models we have generated to explore the effects of Mdm2 phosphorylation on Mdm2 and p53 levels and functions. Based upon our preliminary data, our proposed research should establish Mdm2 phosphorylation as the critical signaling event in the p53-mediated acute DNA damage response and in the regulation of p53 suppression of spontaneous and oncogene induced tumorigenesis. The results of these experiments have much clinical relevance, as an understanding of the regulatory mechanisms that control p53 activity in normal cell growth, in the acute DNA damage response, and in tumorigenesis is a critical prerequisite to developing new therapies to treat radiation-induced pathology and cancer.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Cancer Institute (NCI)
Type
Research Project (R01)
Project #
5R01CA077735-16
Application #
9060898
Study Section
Cancer Molecular Pathobiology Study Section (CAMP)
Program Officer
Johnson, Ronald L
Project Start
1999-03-01
Project End
2020-04-30
Budget Start
2016-05-01
Budget End
2017-04-30
Support Year
16
Fiscal Year
2016
Total Cost
Indirect Cost

  Institution

Name
University of Massachusetts Medical School Worcester
Department
Anatomy/Cell Biology
Type
Schools of Medicine
DUNS #
603847393
City
Worcester
State
MA
Country
United States
Zip Code

  Publications

Wang, Feng; McCannell, Kurtis N; Boškovi?, Ana et al. (2017) Rlim-Dependent and -Independent Pathways for X Chromosome Inactivation in Female ESCs. Cell Rep 21:3691-3699
Carr, Michael I; Jones, Stephen N (2016) Regulation of the Mdm2-p53 signaling axis in the DNA damage response and tumorigenesis. Transl Cancer Res 5:707-724
Carr, Michael I; Roderick, Justine E; Gannon, Hugh S et al. (2016) Mdm2 Phosphorylation Regulates Its Stability and Has Contrasting Effects on Oncogene and Radiation-Induced Tumorigenesis. Cell Rep 16:2618-2629
Carr, Michael I; Roderick, Justine E; Zhang, Hong et al. (2016) Phosphorylation of the Mdm2 oncoprotein by the c-Abl tyrosine kinase regulates p53 tumor suppression and the radiosensitivity of mice. Proc Natl Acad Sci U S A 113:15024-15029
Matijasevic, Z; Krzywicka-Racka, A; Sluder, G et al. (2016) The Zn-finger domain of MdmX suppresses cancer progression by promoting genome stability in p53-mutant cells. Oncogenesis 5:e262
Ghule, Prachi N; Xie, Rong-Lin; Colby, Jennifer L et al. (2015) p53 checkpoint ablation exacerbates the phenotype of Hinfp dependent histone H4 deficiency. Cell Cycle 14:2501-8
Lyle, Stephen; Hoover, Kathleen; Colpan, Cansu et al. (2014) Dicer cooperates with p53 to suppress DNA damage and skin carcinogenesis in mice. PLoS One 9:e100920
Shin, JongDae; Wallingford, Mary C; Gallant, Judith et al. (2014) RLIM is dispensable for X-chromosome inactivation in the mouse embryonic epiblast. Nature 511:86-9
Wan, Guohui; Zhang, Xinna; Langley, Robert R et al. (2013) DNA-damage-induced nuclear export of precursor microRNAs is regulated by the ATM-AKT pathway. Cell Rep 3:2100-12
van der Deen, Margaretha; Taipaleenmäki, Hanna; Zhang, Ying et al. (2013) MicroRNA-34c inversely couples the biological functions of the runt-related transcription factor RUNX2 and the tumor suppressor p53 in osteosarcoma. J Biol Chem 288:21307-19

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