Comprehensive Mapping of p53 Pathway Alterations Reveals an Apparent Role for Both SNP309 and <i>MDM2</i> Amplification in Sarcomagenesis

Ito, Moriko; Barys, Louise; O’Reilly, Terence; Young, Sophie; Gorbatcheva, Bella; Monahan, John E.; Zumstein-Mecker, Sabine; Choong, Peter F. M.; Dickinson, Ian C.; Crowe, Philip; Hemmings, Chris; Desai, Jayesh; Thomas, David M.; Lisztwan, Joanna

doi:10.1158/1078-0432.ccr-10-2050

Cited by 99 publications

(91 citation statements)

References 49 publications

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“…According to our analyses, there is no association between MDM2 rs2279744 and osteosarcoma risk in the population used by Ito et al [3]. This contradicts the result shown by Wang et al [1] in their study.…”

contrasting

confidence: 96%

“…This contradicts the result shown by Wang et al [1] in their study. When we calculate the odds ratio (OR) value of Ito et al [3] samples, using the total of benign tumors (n=37) as controls, we obtain a different OR value. This contradictory result has been observed in all hereditary models (allele model, OR=1.46, 95 % CI 0.62-3.43; codominant model, OR=1.50, 95 % 0.29-7.65; recessive model, OR 1.11, 95 % CI 0.24-5.08; dominant model, OR=1.88, 95 % 0.59-6.01).…”

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confidence: 99%

“…The main problem we detect here is that Wang et al [1] specify neither the samples nor the genotype frequencies used for the meta-analyses. The only available data in the Ito et al [3] paper that can be used as controls come from the benign tumors. When we used these data (osteosarcoma, GG=3, GT=7, TT=7; benign tumors, GG=6, GT=10, TT= 21), no significant values were found.…”

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confidence: 99%

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Letter regarding Wang et al. entitled “Effects of murine double minute 2 polymorphisms on the risk and survival of osteosarcoma: a systematic review and meta-analysis”

2014

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We have read with interest the article by Wang et al. [1] in a recent issue of Tumor Biology. In this study, the authors conducted a systematic review and meta-analysis to assess the effects of two murine double minute 2 (MDM2) polymorphisms, rs2274799 and rs160916, on the risk and survival of osteosarcoma. The authors concluded that MDM2 polymorphisms had effects on the risk but had no effect on the survival of patients with osteosarcoma. In a recent letter to the editor, Liu et al. [2] detected several weaknesses in the meta-analysis. Firstly, they criticize the small number of papers included in the analyses, which could lead to false significant associations. They also point out the lack of information in the methods used to select the studies. Moreover, they comment the absence of Hardy-Weinberg equilibrium analysis in the control population. Finally, they question the quality of the selected studies. In the present letter, we would like to add some other inaccuracies found in the Wang et al.[1] meta-analysis.According to our analyses, there is no association between MDM2 rs2279744 and osteosarcoma risk in the population used by Ito et al. [3]. This contradicts the result shown by Wang et al. [1] in their study. When we calculate the odds ratio (OR) value of Ito et al. [3] samples, using the total of benign tumors (n=37) as controls, we obtain a different OR value. This contradictory result has been observed in all hereditary models (allele model, OR=1.46, codominant model, OR=1.50, recessive model, OR 1.11, dominant model, OR=1.88,

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confidence: 96%

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confidence: 99%

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confidence: 99%

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Letter regarding Wang et al. entitled “Effects of murine double minute 2 polymorphisms on the risk and survival of osteosarcoma: a systematic review and meta-analysis”

2014

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“…4,6,7,30 The hypothesis that MDM2 Ampl and TP53 Mut both provide inactivation of the p53 response has been challenged by the occasional report that the 2 aberrations may be found in the same tumor. 31 We found such apparent double mutations in 2 samples, LS03 and MFH53 (Fig. 2).…”

Section: Discussionmentioning

confidence: 64%

Correlation of TP53 and MDM2 genotypes with response to therapy in sarcoma

Ohnstad¹,

Castro²,

Sun³

et al. 2012

Cancer

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BACKGROUND: Relatively few sarcomas harbor TP53 (tumor protein p53) mutations, but in many cases, amplification of MDM2 (murine double minute 2) effectively inactivate p53. The p53 pathway activity can also be affected by normal genetic variation. METHODS: The mutation status of TP53 and expression of MDM2, TP53, and their genetic variants SNP309 and R72P (Arg72Pro) were investigated in 125 sarcoma patient samples and 18 sarcoma cell lines. Association of the different genotypes and gene aberrations with chemotherapy response and survival, as well as response to MDM2 antagonists in vitro was evaluated. RESULTS: Twenty-two percent of the tumors had mutant TP53 and 20% MDM2 gene amplification. Patients with wild-type TP53 (TP53 Wt ) tumors had improved survival (P < .001) and TP53 Wt was an independent prognostic factor (hazard ratio ¼ 0.41; 95% confidence interval ¼ 0.23-0.74; P ¼ .03). Interestingly, there was a trend toward longer time to progression after chemotherapy for tumors with the apoptosis-prone p53 variant R72 (P ¼ .07), which was strongest with doxorubicin/ifosfamide-based regimens (P ¼ .01). Liposarcomas had low R72 frequency (33% versus 56%), but increased levels of MDM2 and MDM4 (51% and 11%, P < .001). MDM2 overexpression on a TP53 Wt background predicted better response to MDM2 antagonist Nutlin-3a, irrespective of R72P or SNP309 status. CONCLUSIONS: Improved survival after chemotherapy was found in patients with TP53 Wt tumors harboring the R72 variant. MDM2 overexpression in TP53 Wt tumors predicted good response to MDM2 antagonists, irrespective of R72P or SNP309 status. Thus, detailed TP53 and MDM2 genotype analyses prior to

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“…MDM2 rs2279744, situated in the promoter region, was related to an increased risk of OS (GG vs. TT) in Italian population (211 OS patients and 250 controls) (5), being this association stronger in females. Moreover, a robust correlation between rs2279744 G allele enrichment and MDM2 amplification was found, suggesting the contribution of this polymorphism to OS tumorigenesis (12). However, this single nucleotide polymorphism (SNP) did not show any association in the North-American population (7).…”

Section: Systematic Review Nature Publishing Groupmentioning

confidence: 99%

A systematic review and meta-analysis of MDM2 polymorphisms in osteosarcoma susceptibility

et al. 2016

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Two polymorphisms in the murine double minute 2 (MDM2) gene (rs1690916 and rs2279744) have been associated with the risk of osteosarcoma (OS). When we analyzed these two polymorphisms in two new independents cohorts (Spanish and Slovenian), we found no association. In order to clarify this, we conducted a meta-analysis including six populations, with a total of 246 OS patients and 1,760 controls for rs1690916; and 433 OS patients and 1,959 controls for rs2279744. Pooled odds ratio risks and corresponding 95% CI were estimated to assess the possible associations. Our results showed that these two polymorphisms were not associated with the susceptibility of OS under any genetic model studied. In conclusion, the present meta-analysis indicates that MDM2 rs1690916 and rs2279744 cannot be considered as genetic risk factors for OS susceptibility in the different populations. Therefore, the influence of these two polymorphisms on the risk of OS may be less important than previously suggested. Future studies are needed to confirm these results.O steosarcoma (OS) is the most common primary malignant tumor of bone, mainly occurring in the second decade of life. The precise etiology of the disease remains partially unknown (1). Nevertheless, genetic factors might play a key role in its pathogenesis (2). To date diverse studies have reported associations of common genetic variants in biologically plausible pathways with OS risk (3-6). Among the analyzed variants, rs1690916 and rs2279744 in the murine double minute 2 gene (MDM2) are two of the most recurrently studied and associated with the susceptibility of OS (5,7-9). The MDM2 gene is especially interesting because it functions as an E3 ubiquitin ligase promoting p53 degradation (10,11).MDM2 rs1690916, located at the 3′ untranslated region of the gene, was significantly associated with the risk of OS in a large North-American population including 96 patients and 1,416 controls (7). They found that rs1690916 AA genotype decreased the risk of the disease. rs1690916 A allele was also found to be associated with a decreased risk of bone tumors in Russian population including 68 patients and 86 controls (9). However, this study only included 26 OS patients out of 68 analyzed. MDM2 rs2279744, situated in the promoter region, was related to an increased risk of OS (GG vs. TT) in Italian population (211 OS patients and 250 controls) (5), being this association stronger in females. Moreover, a robust correlation between rs2279744 G allele enrichment and MDM2 amplification was found, suggesting the contribution of this polymorphism to OS tumorigenesis (12). However, this single nucleotide polymorphism (SNP) did not show any association in the North-American population (7). A meta-analysis evaluating the association between these two polymorphisms and the risk of OS was performed, concluding that both SNPs influence the risk of OS (13). Nevertheless, some inaccuracies were detected in the study. Among others, the lack of information in the methods used to select the studies and extr...

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Comprehensive Mapping of p53 Pathway Alterations Reveals an Apparent Role for Both SNP309 and MDM2 Amplification in Sarcomagenesis

Cited by 99 publications

References 49 publications

Letter regarding Wang et al. entitled “Effects of murine double minute 2 polymorphisms on the risk and survival of osteosarcoma: a systematic review and meta-analysis”

Letter regarding Wang et al. entitled “Effects of murine double minute 2 polymorphisms on the risk and survival of osteosarcoma: a systematic review and meta-analysis”

Correlation of TP53 and MDM2 genotypes with response to therapy in sarcoma

A systematic review and meta-analysis of MDM2 polymorphisms in osteosarcoma susceptibility

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