Adenovirus-mediated transfer of wild-type p53 gene sensitizes TNF resistant MCF7 derivatives to the cytotoxic effect of this cytokine: relationship with c-myc and Rb

Ameyar, Maya; Shatrov, V A; Bouquet, Céline; Capoulade, Corinne; Cai, Zhenzi; Stancou, Rodica; Badie, Christophe; Haddada, Hédi; Chouaı̈b, Salem

doi:10.1038/sj.onc.1202919

Cited by 33 publications

(29 citation statements)

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“…30 More recently, we have shown that adenovirus -based transfer of wtp53 gene increased sensitivity of cells with mutant p53 to the cytotoxic effect of TNF 31 by a mechanism independent of Bax and Bcl -2 expression but involving ROS production. 43 In the present study, we further examined the molecular basis of tumor resistance to the cytotoxic action of TNF and explored the wtp53-induced sensitization of TNF -resistant cells to the cytotoxic action of TNF.…”

Section: Discussionmentioning

confidence: 99%

“…31 Several reports indicate that p53 can induce or potentiate apoptosis through a variety of mechanisms, e.g., by regulating the expression of genes that participate in the apoptotic response at the mitochondrial level, 45,46 a transcription -dependent p53 -induced alteration in the redox balance, 47 and /or through transcription -independent effects, 28,48,49 which may involve the translocation of p53 to mitochondrial membranes, facilitating their permeabilization. 50 Caspase activation (caspases-3 and -9) has also been connected to p53 -mediated cell death.…”

Section: Discussionmentioning

confidence: 99%

“…31 Efficiency of Adwtp53 to transfer and direct expression of wtp53 was analysed on p53 -negative SAOS cells using specific monoclonal antibody 36 hours after infection with Adwtp53. The expression of functional p53 in Adwtp53-infected cells was then analysed using the p53 functional assay in yeast as described.…”

Section: Cell Lines and Culturementioning

confidence: 99%

“…30 Moreover, we have demonstrated that the transfer of wtp53 using an adenoviral vector ( Adwtp53) reestablishes TNF sensitivity in TNF -resistant cells. 31 In the present study, we investigated the mechanisms of the p53 -mediated restoration of TNF sensitivity. It appears that the p53 effect involves the reestablishment of the TNF -mediated proapoptotic signal transduction cascade, including the activation of caspase -8 and mitochondrial membrane permeabilization.…”

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Wild-type p53 induced sensitization of mutant p53 TNF-resistant cells: Role of caspase-8 and mitochondria

et al. 2002

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In the present study, we have investigated the mechanisms by which the restoration of wild -type ( wt ) p53 functions in p53 mutant cells increases their susceptibility to the cytotoxic action of tumor necrosis factor ( TNF ). Our data indicate that the resistance of p53 -mutated cl.1001 cells to TNF -induced cell death was not due to a defect in the expression of TRADD and FADD, yet correlated with a reduced caspase -8 activation as well as a deficient mitochondrial membrane permeabilization. Moreover, cl.1001 cells failed to translocate the mitochondrial AIF and cytochrome c to the nucleus and to the cytosol, respectively, in response to TNF. Sensitization of these cells, following infection with a recombinant adenovirus encoding wtp53, to TNF -induced cytotoxicity resulted in the restoration of caspase -8 cleavage and the reestablishment of mitochondrial signs of apoptosis. These findings suggest that the crosstalk between p53 and TNF -induced cell death depends on mitochondria and that the combination of TNF and Adwtp53 may be a potential strategy to sensitize mutant p53 TNF -resistant tumors to the cytotoxic action of this cytokine.

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Section: Discussionmentioning

confidence: 99%

Section: Discussionmentioning

confidence: 99%

Section: Cell Lines and Culturementioning

confidence: 99%

mentioning

confidence: 99%

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Wild-type p53 induced sensitization of mutant p53 TNF-resistant cells: Role of caspase-8 and mitochondria

et al. 2002

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“…The replication-deficient adenovirus vector Adwtp53 that harbors a human p53 gene driven by a SV40 virus early promoter in place of the E1 region has been described previously (19). The conditionally replicative adenovirus AdD24 that lacks 24 bp corresponding to amino acids 122 to 129 in the CR2 domain of E1A necessary for binding to Rb protein (20) and has a deleted E3 region and its derivative AdD24-p53 that carries a SV40 virus early-p53 expression cassette inserted in place of the deleted E3 region were described before (17).…”

Section: Nutlins and Recombinant Adenovirusesmentioning

confidence: 99%

Enhanced tumor cell kill by combined treatment with a small-molecule antagonist of mouse double minute 2 and adenoviruses encoding p53

Graat

Carette

Schagen

et al. 2007

Molecular Cancer Therapeutics

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Strategies to treat cancer by restoring p53 tumor suppressor functions are being actively investigated. These approaches range from expressing an exogenous p53 gene in p53 mutant cancers to antagonizing a p53 inhibitor in p53 wild-type (WT) cancer cells. In addition, exogenous p53 is used to strengthen the anticancer efficacy of oncolytic adenoviruses. Many cancers express high levels of the major negative regulator of p53, mouse double minute 2 (MDM2) protein. Recently, a novel class of highly potent and specific MDM2 antagonists, the Nutlins, was identified. We envisioned that Nutlins could protect both endogenous and exogenous p53 from MDM2-mediated inactivation. We therefore investigated treating human cancer cells with a combination of adenovirus-mediated p53 gene therapy and Nutlin. Combination treatment resulted in broadly effective cell kill of p53 WT and p53-negative cancer cells. Cytotoxicity was associated with profound cell cycle checkpoint activation and apoptosis induction. We also tested Nutlin in combination with oncolytic adenoviruses. Nutlin treatment accelerated viral progeny burst from oncolytic adenovirus-infected cancer cells and caused an estimated 10-to 1,000-fold augmented eradication of p53 WT cancer cells. These findings suggest that Nutlins are promising compounds to be combined with p53 gene therapy and oncolytic virotherapy for cancer.

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AdΔ24 and the p53‐expressing variant AdΔ24‐p53 achieve potent anti‐tumor activity in glioma when combined with radiotherapy

Idema

Lamfers

Beusechem

et al. 2007

The Journal of Gene Medicine

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Adenovirus-mediated transfer of wild-type p53 gene sensitizes TNF resistant MCF7 derivatives to the cytotoxic effect of this cytokine: relationship with c-myc and Rb

Cited by 33 publications

References 50 publications

Wild-type p53 induced sensitization of mutant p53 TNF-resistant cells: Role of caspase-8 and mitochondria

Wild-type p53 induced sensitization of mutant p53 TNF-resistant cells: Role of caspase-8 and mitochondria

Enhanced tumor cell kill by combined treatment with a small-molecule antagonist of mouse double minute 2 and adenoviruses encoding p53

AdΔ24 and the p53‐expressing variant AdΔ24‐p53 achieve potent anti‐tumor activity in glioma when combined with radiotherapy

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