Literature DB >> 15064742

A post-ubiquitination role for MDM2 and hHR23A in the p53 degradation pathway.

Chrystelle Brignone1, Kathleen E Bradley, Alexei F Kisselev, Steven R Grossman.   

Abstract

Abrogation of ubiquitin/proteasome-dependent turnover of p53 is critical for its activation. UbL-UBA proteins, including human homolog of Rad23 (hHR23) proteins, may regulate proteasomal degradation of substrates such as p53, due to their ability to interact with both ubiquitinated substrates and the proteasome. siRNA-mediated depletion of hHR23A or hHR23B in human cell lines accelerated p53 degradation. In contrast, overexpression of hHR23 proteins led to the accumulation of ubiquitinated p53, and purified hHR23 proteins also blocked p53 proteasome degradation in vitro. An hHR23-MDM2 complex was identified, suggesting that MDM2 and hHR23 cooperate in the regulation of p53 proteasome degradation. Consistent with this hypothesis, an MDM2 mutant that demonstrated increased binding in vivo to hHR23A was able to ubiquitinate, but not degrade p53. Moreover, the defective phenotype of this MDM2 mutant was rescued by siRNA knockdown of hHR23A. Our data indicate that MDM2 acts at a step in the p53 degradation pathway after ubiquitination, to counteract hHR23 inhibition of p53 turnover. Moreover, our data suggest the possibility that ubiquitin ligase/UbL-UBA protein complexes, as exemplified by the MDM2/hHR23 complex, may serve a general role in regulating substrate degradation by the proteasome.

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Year:  2004        PMID: 15064742     DOI: 10.1038/sj.onc.1207540

Source DB:  PubMed          Journal:  Oncogene        ISSN: 0950-9232            Impact factor:   9.867


  26 in total

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2.  Glycogen synthase kinase 3-dependent phosphorylation of Mdm2 regulates p53 abundance.

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4.  hHR23B is required for genotoxic-specific activation of p53 and apoptosis.

Authors:  M Kaur; M Pop; D Shi; C Brignone; S R Grossman
Journal:  Oncogene       Date:  2006-08-21       Impact factor: 9.867

5.  Ubiquitination and degradation of mutant p53.

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9.  Physiological and pathophysiological characteristics of ataxin-3 isoforms.

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Journal:  J Biol Chem       Date:  2018-11-19       Impact factor: 5.157

10.  Structure of the XPC binding domain of hHR23A reveals hydrophobic patches for protein interaction.

Authors:  Mariusz Kamionka; Juli Feigon
Journal:  Protein Sci       Date:  2004-09       Impact factor: 6.725

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