Mouse double minute antagonist Nutlin-3a enhances chemotherapy-induced apoptosis in cancer cells with mutant p53 by activating E2F1

Ambrosini, Grazia; Sambol, Elliot B.; Carvajal, Daisy; Vassilev, Lyubomir T.; Singer, Samuel; Schwartz, Gary K.

doi:10.1038/sj.onc.1210136

Cited by 145 publications

(141 citation statements)

References 33 publications

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“…This relative difference in Nutlin efficacy based on p53 status is consistent with previous reports (Van Maerken et al, 2006;Ambrosini et al, 2007). Although the inhibition constant (K i ) is reported to be 0.09 mM for Nutlin-3a (Vassilev et al, 2004) and 0.7 mM for Nutlin-3 (Laurie et al, 2006) in p53 wt cells in vitro, numerous studies have reported that 10 mM of Nutlin-3 or Nutlin-3a is needed to disrupt the p53-HDM2 complex and elicit maximal downstream effects in vivo (Vassilev et al, 2004;Laurie et al, 2006;Patton et al, 2006;Tovar et al, 2006;Larusch et al, 2007).…”

Section: Discussionsupporting

confidence: 92%

“…In contrast, our Nutlin-3 activates p73 LMS Lau et al data demonstrate that Nutlin-3 alone induces p73 protein stabilization as well as enhanced TAp73 transcriptional activity. Thus, the increase in E2F-1 transcriptional activity and p73 protein levels reported by Ambrosini et al (2007) is likely due to the combination treatment with cisplatin chemotherapy and Nutlin-3 since chemotherapies including cisplatin and doxorubicin are known to activate both E2F1 and TAp73 (Irwin, 2004).…”

Section: Discussionmentioning

confidence: 98%

“…We have previously shown that E2F-1, a transcription factor and an N-terminal HDM2-binding protein, can induce apoptosis independent of p53 by inducing p73 transcription (Irwin et al, 2000). Interestingly, Nutlin-3 has recently been shown to inhibit E2F-1 binding to HDM2, leading to activation of E2F-1 and potentiation of chemotherapy-induced apoptosis in p53-mutant but not wt cells (Ambrosini et al, 2007). However, in our model using Nutlin-3 alone, we did not observe increased p73 transcription or activation of an E2F-1-responsive p73 promoter.…”

Section: Discussionmentioning

confidence: 99%

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HDM2 antagonist Nutlin-3 disrupts p73-HDM2 binding and enhances p73 function

et al. 2007

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Nutlin-3, a small molecule inhibitor, activates p53 by disrupting p53-HDM2 association. In this study, we found that Nutlin-3 suppressed cell growth and induced apoptosis in the absence of wild-type p53, suggesting a p53-independent mechanism for Nutlin-3-induced cell death. Like p53, its homolog p73 transactivates proapoptotic genes and induces cell death. Since HDM2, a key negative regulator of p53, also binds to and inhibits p73, we asked whether p73 could mediate Nutlin-3-induced apoptosis. We demonstrate that Nutlin-3 inhibits endogenous binding between the proapoptotic p73 isoform TAp73a and HDM2 in p53-null cells. Dissociation of p73 and HDM2 leads to increased p73 transcriptional activity with upregulation of p73 target genes noxa, puma and p21, as well as enhanced apoptosis. p73 knockdown by siRNA results in rescue of Nutlin-3-treated cells, indicating that Nutlin-3-induced apoptosis is, at least in part, p73 dependent. In addition, Nutlin-3 treatment increases TAp73a protein levels with prolongation of p73 half-life. These results provide the first evidence that Nutlin-3 disrupts endogenous p73-HDM2 interaction and enhances the stability and proapoptotic activities of p73 and thus, provides a rationale for the use of Nutlin-3 in the large number of human tumors in which p53 is inactivated.

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Section: Discussionsupporting

confidence: 92%

Section: Discussionmentioning

confidence: 98%

Section: Discussionmentioning

confidence: 99%

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HDM2 antagonist Nutlin-3 disrupts p73-HDM2 binding and enhances p73 function

et al. 2007

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“…25,26 E2F-1 differs from that of other E2F family members due to its ability to regulate not only cell-cycle progression but also apoptosis as it directly induces the expression of p73, of caspase 3 and 7 and of some pro-apoptotic Bcl-2 family members. [27][28][29][30][31][32][33][34] We show here that E2F-1 is a major contributor of caspase-dependent induction of Noxa in response to ABT-737 treatment. Caspases cleave the E2F-1 regulator pRb in ABT-737-treated cells, giving rise to a p68Rb truncated form, which has a direct role in Noxa and cell death inductions together with E2F-1.…”

mentioning

confidence: 51%

“…As treatment with the Mdm2 inhibitor Nutlin-3a was shown to enhance the pRb/E2F-1 pathway, 33,34 we reasoned that it may increase cell sensitivity to ABT-737, provided pRb is present. We found that combination of Nutlin-3a to ABT-737, but not treatment with anyone alone, induced dramatic cell death in the breast cancer cell lines MDA-MB-231 and MDA-MB-468, cells that carry p53 mutations (R280K and R273H, respectively) and constitutively express low levels of pRb (Figures 8a and b).…”

mentioning

confidence: 99%

pRb/E2F-1-mediated caspase-dependent induction of Noxa amplifies the apoptotic effects of the Bcl-2/Bcl-xL inhibitor ABT-737

et al. 2013

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Although Bcl-2 family members control caspase activity by regulating mitochondrial permeability, caspases can, in turn, amplify the apoptotic process upstream of mitochondria by ill-characterized mechanisms. We herein show that treatment with a potent inhibitor of Bcl-2 and Bcl-xL, ABT-737, triggers caspase-dependent induction of the BH3-only protein, Mcl-1 inhibitor, Noxa. RNA interference experiments reveal that induction of Noxa, and subsequent cell death, rely not only on the transcription factor E2F-1 but also on its regulator pRb. In response to ABT-737, pRb is cleaved by caspases into a p68Rb form that still interacts with E2F-1. Moreover, pRb occupies the noxa promoter together with E2F-1, in a caspase-dependent manner upon ABT-737 treatment. Thus, caspases contribute to trigger the mitochondrial apoptotic pathway by coupling Bcl-2/Bcl-xL inhibition to that of Mcl-1, via the pRb/E2F-1-dependent induction of Noxa.

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The TP73 complex network: Ready for clinical translation in cancer?

Soldevilla

Millán

Bonilla

et al. 2013

Genes Chromosomes & Cancer

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TP73 is a member of the TP53 family, whose deregulated expression has been reported in a wide variety of cancers and linked to patients' outcome. The fact that TP73 encodes a complex number of isoforms (TAp73 and ΔTAp73) with opposing functions and the cross-talk with other members of the family (TP53 and TP63) make it difficult to determine its clinical relevance. Here, we review the molecular mechanisms driving TAp73 and ΔTAp73 expression and how these variants inhibit or promote carcinogenesis. We also highlight the intricate interplay between TP53 family members. In addition, we comment on current pharmacological approaches targeting the TP73 pathway and those affecting the TAp73/ΔTAp73 ratio. Finally, we discuss the current data available in the literature that provide evidence on the role of TP73 variants in predicting prognosis. To date, most of the studies that evaluate the status levels of TP73 isoforms have been based on limited-size series. Despite this limitation, these publications highlight the correlation between high levels of the oncogenic forms and failure to respond to chemotherapy and/or shorter survival. Finally, we emphasize the need for studies to evaluate the significance of combining the deregulation of various members of the TP53 family in order to define patient outcome or their responsiveness to specific therapies.

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Mouse double minute antagonist Nutlin-3a enhances chemotherapy-induced apoptosis in cancer cells with mutant p53 by activating E2F1

Cited by 145 publications

References 33 publications

HDM2 antagonist Nutlin-3 disrupts p73-HDM2 binding and enhances p73 function

HDM2 antagonist Nutlin-3 disrupts p73-HDM2 binding and enhances p73 function

pRb/E2F-1-mediated caspase-dependent induction of Noxa amplifies the apoptotic effects of the Bcl-2/Bcl-xL inhibitor ABT-737

The TP73 complex network: Ready for clinical translation in cancer?

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