The deubiquitinating enzyme USP2a regulates the p53 pathway by targeting Mdm2

Stevenson, Lauren; Sparks, Alison; Allende-Vega, Nerea; Xirodimas, Dimitris P.; Lane, David P.; Saville, Mark K.

doi:10.1038/sj.emboj.7601567

Cited by 253 publications

(247 citation statements)

References 53 publications

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“…Ectopic expression of USP2a results in elevated levels of Mdm2 and an increase in degradation of p53 (Stevenson et al, 2007). To determine the effect of USP2a on Mdm2-mediated degradation of MdmX, H1299 cells (p53 null) were co-transfected with plasmids expressing MdmX, Mdm2 and increasing amounts of plasmidexpressing USP2a.…”

Section: Usp2a Deubiquitinates Mdmxmentioning

confidence: 99%

“…These data indicate that there are at least two binding sites for MdmX in USP2a: one between amino acids 1-200 in its N-terminal extension and one between amino acids 403-503 in its catalytic core. Similarly, deletion of both the N and C-terminus of USP2a was required to prevent its binding to Mdm2 (Stevenson et al, 2007).…”

Section: Usp2a Forms a Complex With Mdmxmentioning

confidence: 99%

“…However, the balance of activity of endogenous HAUSP is such that its knockdown or knockout results in destabilization of Mdm2 and MdmX and stabilization of p53 (Li et al, 2002(Li et al, , 2004Cummins et al, 2004;Meulmeester et al, 2005). We have previously shown that USP2a can deubiquitinate Mdm2 without reversing Mdm2-mediated p53 ubiquitination (Stevenson et al, 2007). USP2a has oncogenic properties and its overexpression can prevent apoptosis induced by chemotherapeutic agents (Graner et al, 2004;Priolo et al, 2006).…”

Section: Introductionmentioning

confidence: 99%

“…USP2a has oncogenic properties and its overexpression can prevent apoptosis induced by chemotherapeutic agents (Graner et al, 2004;Priolo et al, 2006). USP2a knockdown results in increased p53 protein expression and upregulation of p53 target genes (Priolo et al, 2006;Stevenson et al, 2007). USP2a mRNA is expressed in a range of normal tissues, the highest level of expression being in the testis (Lin et al, 2001;Park et al, 2002;Gousseva and Baker, 2003).…”

Section: Introductionmentioning

confidence: 99%

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MdmX is a substrate for the deubiquitinating enzyme USP2a

et al. 2009

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It has previously been shown that ubiquitin-specific protease 2a (USP2a) is a regulator of the Mdm2/p53 pathway. USP2a binds to Mdm2 and can deubiquitinate Mdm2 without reversing Mdm2-mediated p53 ubiquitination. Overexpression of USP2a causes accumulation of Mdm2 and promotes p53 degradation. We now show that MdmX is also a substrate for USP2a. MdmX associates with USP2a independently of Mdm2. Ectopic expression of wild-type USP2a but not a catalytic mutant prevents Mdm2-mediated degradation of MdmX. This correlates with the ability of wild-type USP2a to deubiquitinate MdmX. siRNA-mediated knockdown of USP2a in NTERA-2 testicular embryonal carcinoma cells and MCF7 breast cancer cells causes destabilization of MdmX and results in a decrease in MdmX protein levels, showing that endogenous USP2a participates in the regulation of MdmX stability. The therapeutic drug, cisplatin decreases MdmX protein expression. USP2a mRNA and protein levels were also reduced after cisplatin exposure. The magnitude and time course of USP2a downregulation suggests that the reduction in USP2a levels could contribute to the decrease in MdmX expression following treatment with cisplatin. Knockdown of USP2a increases the sensitivity of NTERA-2 cells to cisplatin, raising the possibility that suppression of USP2a in combination with cisplatin may be an approach for cancer therapy.

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Section: Usp2a Deubiquitinates Mdmxmentioning

confidence: 99%

Section: Usp2a Forms a Complex With Mdmxmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

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MdmX is a substrate for the deubiquitinating enzyme USP2a

et al. 2009

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“…More recently, USP2a (ubiquitin-specific protease 2a) has been identified as a novel DUB that selectively targets Mdm2, unlike HAUSP, and thereby offers another potential approach of therapeutic intervention to reactivate WT p53 (Stevenson et al, 2007). Future studies will further address the importance of these DUBs as clinical targets and also the selectivity of their use based on tumour subtypes.…”

Section: Targeting the P53 -Mdm2 Interactionmentioning

confidence: 99%