Literature DB >> 18840648

Identification of ANKRD11 as a p53 coactivator.

Paul M Neilsen1, Kelly M Cheney, Chia-Wei Li, J Don Chen, Jacqueline E Cawrse, Renée B Schulz, Jason A Powell, Raman Kumar, David F Callen.   

Abstract

The ability of p53 to act as a transcription factor is critical for its function as a tumor suppressor. Ankyrin repeat domain 11, ANKRD11 (also known as ANR11 or ANCO1), was found to be a novel p53-interacting protein that enhanced the transcriptional activity of p53. ANKRD11 expression was shown to be downregulated in breast cancer cell lines. Restoration of ANKRD11 expression in MCF-7 (wild-type p53) and MDA-MB-468 (p53(R273H) mutant) cells suppressed their proliferative and clonogenic properties through enhancement of CDKN1A (p21(waf1)/CIP1) expression. ShRNA-mediated silencing of ANKRD11 expression reduced the ability of p53 to activate CDKN1A expression. ANKRD11 was shown to associate with the p53 acetyltransferases and cofactors, P/CAF and hADA3. Exogenous ANKRD11 expression enhanced the levels of acetylated p53 in both MCF-7 and MDA-MB-468 cells. ANKRD11 enhanced the DNA-binding properties of mutant p53(R273H) to the CDKN1A promoter, suggesting that ANKRD11 can mediate the restoration of normal p53 function in some cancer-related p53 mutations. In addition, ANKRD11 itself was found to be a novel p53 target gene. These findings demonstrate a role for ANKRD11 as a p53 coactivator and suggest the involvement of ANKRD11 in a regulatory feedback loop with p53.

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Year:  2008        PMID: 18840648     DOI: 10.1242/jcs.026351

Source DB:  PubMed          Journal:  J Cell Sci        ISSN: 0021-9533            Impact factor:   5.285


  31 in total

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5.  Neonatal genome-wide methylation patterns in relation to birth weight in the Norwegian Mother and Child Cohort.

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8.  Novel Mutations and Unreported Clinical Features in KBG Syndrome.

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10.  Mdm2 is a novel activator of ApoCIII promoter which is antagonized by p53 and SHP inhibition.

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