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P53 is an important tumor suppressor that, upon activation, induces growth arrest and cell death. Control of p53 is thus of prime importance for proliferating cells, but also for cancer therapy, where p53 activity contributes to the eradication of tumors. Mdm2 functionally inhibits p53 and targets the tumor suppressor protein for degradation. In a genetic screen, we identified TRIM25 as a novel regulator of p53 and Mdm2. TRIM25 increased p53 and Mdm2 abundance by inhibiting their ubiquitination and degradation in 26 S proteasomes. TRIM25 co-precipitated with p53 and Mdm2 and interfered with the association of p300 and Mdm2, a critical step for p53 polyubiquitination. Despite the increase in p53 levels, p53 activity was inhibited in the presence of TRIM25. Downregulation of TRIM25 resulted in an increased acetylation of p53 and p53-dependent cell death in HCT116 cells. Upon genotoxic insults, TRIM25 dampened the p53-dependent DNA damage response. The downregulation of TRIM25 furthermore resulted in massive apoptosis during early embryogenesis of medaka, which was rescued by the concomitant downregulation of p53, demonstrating the functional relevance of the regulation of p53 by TRIM25 in an organismal context.

Original publication

DOI

10.1038/onc.2015.21

Type

Journal article

Journal

Oncogene

Publication Date

11/2015

Volume

34

Pages

5729 - 5738

Addresses

Institute of Toxicology and Genetics, Karlsruhe Institute of Technology, Karlsruhe, Germany.

Keywords

Cell Line, Tumor, HCT116 Cells, Animals, Oryzias, Humans, DNA Damage, Proteasome Endopeptidase Complex, Ubiquitin-Protein Ligases, Transcription Factors, Apoptosis, Tumor Suppressor Protein p53, Proto-Oncogene Proteins c-mdm2, Ubiquitination, MCF-7 Cells, Tripartite Motif Proteins