p53 Modulates Notch Signaling in MCF-7 Breast Cancer Cells by Associating With the Notch Transcriptional Complex Via MAML1
- Authors
- Yun, Jieun; Espinoza, Ingrid; Pannuti, Antonio; Romero, Damian; Martinez, Luis; Caskey, Mary; Stanculescu, Adina; Bocchetta, Maurizio; Rizzo, Paola; Band, Vimla; Band, Hamid; Kim, Hwan Mook; Park, Song-Kyu; Kang, Keon Wook; Avantaggiati, Maria Laura; Gomez, Christian R.; Golde, Todd; Osborne, Barbara; Miele, Lucio
- Issue Date
- Dec-2015
- Publisher
- WILEY-BLACKWELL
- Citation
- JOURNAL OF CELLULAR PHYSIOLOGY, v.230, no.12, pp.3115 - 3127
- Journal Title
- JOURNAL OF CELLULAR PHYSIOLOGY
- Volume
- 230
- Number
- 12
- Start Page
- 3115
- End Page
- 3127
- URI
- https://scholarworks.bwise.kr/gachon/handle/2020.sw.gachon/9856
- DOI
- 10.1002/jcp.25052
- ISSN
- 0021-9541
- Abstract
- p53 and Notch-1 play important roles in breast cancer biology. Notch-1 inhibits p53 activity in cervical and breast cancer cells. Conversely, p53 inhibits Notch activity in T-cells but stimulates it in human keratinocytes. Notch co-activator MAML1 binds p53 and functions as a p53 co-activator. We studied the regulation of Notch signaling by p53 in MCF-7 cells and normal human mammary epithelial cells (HMEC). Results show that overexpression of p53 or activation of endogenous p53 with Nutlin-3 inhibits Notch-dependent transcriptional activity and Notch target expression in a dose-dependent manner. This effect could be partially rescued by transfection of MAML1 but not p300. Standard and quantitative co-immunoprecipitation experiments readily detected a complex containing p53 and Notch-1 in MCF-7 cells. Formation of this complex was inhibited by dominant negative MAML1 (DN-MAML1) and stimulated by wild-type MAML1. Standard and quantitative far-Western experiments showed a complex including p53, Notch-1, and MAML1. Chromatin immunoprecipitation (ChIP) experiments showed that p53 can associate with Notch-dependent HEY1 promoter and this association is inhibited by DN-MAML1 and stimulated by wild-type MAML1. Our data support a model in which p53 associates with the Notch transcriptional complex (NTC) in a MAML1-dependent fashion, most likely through a p53-MAML1 interaction. In our cellular models, the effect of this association is to inhibit Notch-dependent transcription. Our data suggest that p53-null breast cancers may lack this Notch-modulatory mechanism, and that therapeutic strategies that activate wild-type p53 can indirectly cause inhibition of Notch transcriptional activity. (C) 2015 Wiley Periodicals, Inc.
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