Mutational analysis of Mdm2 C-terminal tail suggests an evolutionarily conserved role of its length in Mdm2 activity toward p53 and indicates structural differences between Mdm2 homodimers and Mdm2/MdmX heterodimers

Doleželová, Pavlína; Cetkovská, Kateřina; Vousden, Karen H.; Uldrijan, Stjepan

doi:10.4161/cc.11.5.19445

Cited by 29 publications

(41 citation statements)

References 30 publications

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“…Consistent with the study mentioned above (27), we showed that ectopically expressed MDM2 with the antiterminating mutation is defective in its ability to degrade both ectopic and endogenous p53 in U2OS cells (Supplemental Figure 2, B and C). In fact, expression of mutant MDM2 led to increased levels of p53 protein in either case.…”

Section: Resultssupporting

confidence: 74%

“…Previous cell-based transfection studies have shown that the highly conserved extreme C-terminus of MDM2 is essential for its oligomerization and E3 ubiquitin ligase activity (25,26). In addition, a more recent study showed that the same MDM2 variant, when ectopically expressed, is unable to degrade coexpressed p53 in vitro (27).…”

Section: Resultsmentioning

confidence: 99%

“…Reports that defective E3 ligase activity due to mutations or extensions in the extreme C terminus of MDM2 can be partially rescued by coexpression of the MDM2 homolog MDMX could explain the viability of the Tyr487Ala mouse in comparison with the Cys462Ala mouse (25)(26)(27). However, since MDM2 variants with mutations in the last 5 amino acids of MDM2 share characteristic properties with those of antiterminating MDM2 mutations, it is surprising that the Tyr487Ala mouse does not display some segmental progeroid characteristics (25)(26)(27). We speculate that key differences between our index patient and Tyr487Ala mice could account for the different phenotypes.…”

Section: Methodsmentioning

confidence: 99%

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Dysfunction of the MDM2/p53 axis is linked to premature aging

Lessel

Trujillo

et al. 2017

Journal of Clinical Investigation

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Section: Resultssupporting

confidence: 74%

Section: Resultsmentioning

confidence: 99%

Section: Methodsmentioning

confidence: 99%

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Dysfunction of the MDM2/p53 axis is linked to premature aging

Lessel

Trujillo

et al. 2017

Journal of Clinical Investigation

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“…S9A,B). Consistent with other C ′ -terminal RING domain-containing proteins (Dolezelova et al 2012), there are exactly 13 amino acids following the final cysteine residue, and, as with HDM2 (Fang et al 2000), there are seven critical cysteine residues that are conserved for ubiquitin ligation activity and p53 degradation (Supplemental Fig. S10).…”

Section: Lj-mdm2 and Lj-mdm4 Genesmentioning

confidence: 57%

The p53–Mdm2 interaction and the E3 ligase activity of Mdm2/Mdm4 are conserved from lampreys to humans

et al. 2016

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The extant jawless vertebrates, represented by lampreys and hagfish, are the oldest group of vertebrates and provide an interesting genomic evolutionary pivot point between invertebrates and jawed vertebrates. Through genome analysis of one of these jawless vertebrates, the Japanese lamprey (Lethenteron japonicum), we identified all three members of the important p53 transcription factor family-Tp53, Tp63, and Tp73-as well as the Mdm2 and Mdm4 genes. These genes and their products are significant cellular regulators in human cancer, and further examination of their roles in this most distant vertebrate relative sheds light on their origin and coevolution. Their important role in response to DNA damage has been highlighted by the discovery of multiple copies of the Tp53 gene in elephants. Expression of lamprey p53, Mdm2, and Mdm4 proteins in mammalian cells reveals that the p53-Mdm2 interaction and the Mdm2/Mdm4 E3 ligase activity existed in the common ancestor of vertebrates and have been conserved for >500 million years of vertebrate evolution. Lamprey Mdm2 degrades human p53 with great efficiency, but this interaction is not blocked by currently available small molecule inhibitors of the human HDM2 protein, suggesting utility of lamprey Mdm2 in the study of the human p53 signaling pathway.

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“…However, recent studies have also implicated the extreme C-terminal amino acids of Mdm2 in E3 ligase function (Uldrijan et al 2007). Mutations of cysteine residues in human MDM2 (C447, C462, or C475) that are critical for the structure of the RING domain (Sharp et al 1999;Argentini et al 2000;Fang et al 2000) or changes in the C-terminal tail length by either deletion of five amino acids or extension of five residues (by bypassing the stop codon) substantially inhibit its E3 ligase activity (Poyurovsky et al 2010;Dolezelova et al 2012). Another important feature of the Mdm2 RING domain is that it interacts with an Mdm2-related protein, Mdm4 (Sharp et al 1999;Tanimura et al 1999).…”

Section: The Mdm2 E3 Ligasementioning

confidence: 99%

Limiting the power of p53 through the ubiquitin proteasome pathway

2014

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The ubiquitin proteasome pathway is critical in restraining the activities of the p53 tumor suppressor. Numerous E3 and E4 ligases regulate p53 levels. Additionally, deubquitinating enzymes that modify p53 directly or indirectly also impact p53 function. When alterations of these proteins result in increased p53 activity, cells arrest in the cell cycle, senesce, or apoptose. On the other hand, alterations that result in decreased p53 levels yield tumor-prone phenotypes. This review focuses on the physiological relevance of these important regulators of p53 and their therapeutic implications.

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Mutational analysis of Mdm2 C-terminal tail suggests an evolutionarily conserved role of its length in Mdm2 activity toward p53 and indicates structural differences between Mdm2 homodimers and Mdm2/MdmX heterodimers

Cited by 29 publications

References 30 publications

Dysfunction of the MDM2/p53 axis is linked to premature aging

Dysfunction of the MDM2/p53 axis is linked to premature aging

The p53–Mdm2 interaction and the E3 ligase activity of Mdm2/Mdm4 are conserved from lampreys to humans

Limiting the power of p53 through the ubiquitin proteasome pathway

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