| Literature DB >> 21478910 |
A Terrinoni1, I S Pagani, I Zucchi, A M Chiaravalli, V Serra, F Rovera, S Sirchia, G Dionigi, M Miozzo, A Frattini, A Ferrari, C Capella, F Pasquali, F Lo Curto, F L Curto, A Albertini, G Melino, G Porta.
Abstract
The p53 transcription factor has a critical role in cell stress response and in tumor suppression. Wild-type p53 protein is a growth modulator and its inactivation is a critical event in malignant transformation. It has been recently demonstrated that wild-type p53 has developmental and differentiation functions. Indeed an over-expression of p53 in tumor cells induces asymmetrical division avoiding self-renewal of cancer stem cells (CSCs) and instead promoting their differentiation. In this study, 28 human breast carcinomas have been analyzed for expression of wild-type p53 and of a pool of non-clustered homeobox genes. We demonstrated that orthodenticle homolog 1 gene (OTX1) is transcribed in breast cancer. We established that the p53 protein directly induces OTX1 expression by acting on its promoter. OTX1 has been described as a critical molecule for axon refinement in the developing cerebral cortex of mice, and its activity in breast cancer suggests a synergistic function with p53 in CSC differentiation. Wild-type p53 may regulate cellular differentiation by an alternative pathway controlling OTX1 signaling only in breast cancer cells and not in physiological conditions.Entities:
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Year: 2011 PMID: 21478910 DOI: 10.1038/onc.2011.31
Source DB: PubMed Journal: Oncogene ISSN: 0950-9232 Impact factor: 9.867