Abstract

The tumor suppressor protein p53 is a transcription factor that has been implicated in the cellular response to DNA damage and mediates either growth arrest or apoptosis. The tumor suppressor BRCA1 is less well- characterized but over-expression of BRCA1 was shown to also alternatively lead to growth arrest or apoptosis p53 and BRCA1 have been shown to interact both physically and functionally. The research proposed in the application is designed to explore the details of p53 and BRCA1-dependent transcriptional activation and elucidate whether the interaction of these tumor suppressor proteins has biological relevance. Preliminary studies have identified two classes of p53 response elements by examining the effect of monoclonal antibody moAb421 on the sequence-specific DNA binding of p53 in electrophoretic mobility shift assays. Incubation with moAb421 enhances the binding of p53 to one set of response elements by inhibits binding to another set, suggesting that different conformations of p53 may interact with each subset of response elements. BRCA1 selectively enhances p53-dependent activation of one subset of sites. Our studies have also shown that the ATF1 transcription factor can interact with BRCA1 protein both physically and functionally and that BRCA1 can augment transcription through a cyclic AMP response element (CRE). Promoters have been identified which contain both a CRE and a p53 binding site. Thus, the proposed aims include experiments to: (1) Determine the significance of distinct subsets of p53 response elements classified by the differential effect of monoclonal antibody moAb421. (2) Determine how BRCA1 alters transcription through the CRE and characterize the interaction of BRCA1 with members of the ATF1 and CREB transcription factors. (3) Characterize the interaction of BRCA1 and p53 on genes that contain both a CRE and a p53 site. (4) Determine the role of BRCA1 and ATF1 in the p53- mediated response to DNA damage. As p53 is mutated in up to 30% of cases of breast cancer and the BRCA1 gene is responsible for approximately 50% of inherited breast cancer, it will be important to determine whether these two tumor suppressor proteins play convergent roles in gene expression involved in the cellular response to DNA damage as well as in the pathogenesis of breast cancer.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Cancer Institute (NCI)
Type
Research Program Projects (P01)
Project #
1P01CA080058-01A1
Application #
6323779
Study Section
Subcommittee G - Education (NCI)
Project Start
2000-02-16
Project End
2005-01-31
Budget Start
Budget End
Support Year
1
Fiscal Year
2000
Total Cost
$237,979
Indirect Cost

  Institution

Name
Mount Sinai School of Medicine
Department
Type
DUNS #
City
New York
State
NY
Country
United States
Zip Code
10029

  Publications

Pappas, Kyrie; Xu, Jia; Zairis, Sakellarios et al. (2017) p53 Maintains Baseline Expression of Multiple Tumor Suppressor Genes. Mol Cancer Res 15:1051-1062
Mungamuri, Sathish Kumar; Qiao, Rui F; Yao, Shen et al. (2016) USP7 Enforces Heterochromatinization of p53 Target Promoters by Protecting SUV39H1 from MDM2-Mediated Degradation. Cell Rep 14:2528-37
Muñoz-Fontela, César; Mandinova, Anna; Aaronson, Stuart A et al. (2016) Emerging roles of p53 and other tumour-suppressor genes in immune regulation. Nat Rev Immunol 16:741-750
Ou, Yang; Wang, Shang-Jui; Li, Dawei et al. (2016) Activation of SAT1 engages polyamine metabolism with p53-mediated ferroptotic responses. Proc Natl Acad Sci U S A 113:E6806-E6812
Guernet, Alexis; Mungamuri, Sathish Kumar; Cartier, Dorthe et al. (2016) CRISPR-Barcoding for Intratumor Genetic Heterogeneity Modeling and Functional Analysis of Oncogenic Driver Mutations. Mol Cell 63:526-38
Meslamani, Jamel; Smith, Steven G; Sanchez, Roberto et al. (2016) Structural features and inhibitors of bromodomains. Drug Discov Today Technol 19:3-15
Hwang, So-Young; Deng, Xianming; Byun, Sanguine et al. (2016) Direct Targeting of ?-Catenin by a Small Molecule Stimulates Proteasomal Degradation and Suppresses Oncogenic Wnt/?-Catenin Signaling. Cell Rep 16:28-36
Shi, D; Dai, C; Qin, J et al. (2016) Negative regulation of the p300-p53 interplay by DDX24. Oncogene 35:528-36
Tavana, Omid; Li, Dawei; Dai, Chao et al. (2016) HAUSP deubiquitinates and stabilizes N-Myc in neuroblastoma. Nat Med 22:1180-1186
Wang, Donglai; Kon, Ning; Lasso, Gorka et al. (2016) Acetylation-regulated interaction between p53 and SET reveals a widespread regulatory mode. Nature 538:118-122

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