Human oncoprotein MDM2 activates the Akt signaling pathway through an interaction with the repressor element-1 silencing transcription factor conferring a survival advantage to cancer cells

Singh, S. K.; Ramamoorthy, Mahesh; Vaughan, Catherine; Yeudall, W. Andrew; Deb, Sumitra

doi:10.1038/cdd.2012.153

Cited by 35 publications

(33 citation statements)

References 40 publications

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“…Generation of plasmids, lentiviruses, and stable transfectants expressing GOF p53 or shRNA against GFP or p53 was carried out using pLKO.1 expression vector purchased from Open Biosystem following the supplier's protocols. Lung cells from mice were generated and cultured following standard protocols (28,62). CCNA2 promoter was a gift from Toshio Nikaido (63).…”

Section: Methodsmentioning

confidence: 99%

Mutant p53 establishes targetable tumor dependency by promoting unscheduled replication

Singh¹,

Vaughan²,

Frum³

et al. 2017

Journal of Clinical Investigation

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Section: Methodsmentioning

confidence: 99%

Mutant p53 establishes targetable tumor dependency by promoting unscheduled replication

Singh¹,

Vaughan²,

Frum³

et al. 2017

Journal of Clinical Investigation

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“…WI38 (WT p53) normal lung fibroblasts were purchased from ATCC and maintained in Eagle’s MEM (ATCC) plus 10% FBS. ABC1 cells (P278S) (adenocarcinoma) expressing shGFP or shMDM2 (18) were maintained in MEM plus 10% FBS and (1 ug/ml) puromycin (Gibco). H1793, H1975 (both R273H; NSCLC), MDA MB 231 (R280K; breast), U2OS (WT p53; osteosarcoma), and 293T cells (WT p53; human embryonic kidney) were purchased from ATCC and maintained in DMEM plus 10% FBS.…”

Section: Methodsmentioning

confidence: 99%

Constitutive Activation of DNA Damage Checkpoint Signaling Contributes to Mutant p53 Accumulation via Modulation of p53 Ubiquitination

Frum

Love

Damle

et al. 2016

Molecular Cancer Research

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Many mutant p53 proteins exhibit an abnormally long half-life and overall increased abundance compared to wild-type p53 in tumors, contributing to mutant p53’s gain-of-function oncogenic properties. Here a novel mechanism is revealed for the maintenance of mutant p53 abundance in cancer that is dependent on DNA damage checkpoint activation. High level mutant p53 expression in lung cancer cells was associated with preferential p53 mono vs. polyubiquitination, suggesting a role for the ubiquitin/proteasome system in regulation of mutant p53 abundance in cancer cells. Interestingly, mutant p53 ubiquitination status was regulated by ATM activation and downstream phosphorylation of mutant p53 (serine 15), both in resting and genotoxin-treated lung cancer cells. Specifically, either inhibition of ATM with caffeine or mutation of p53 (serine 15 to alanine) restored MDM2-dependent polyubiquitination of otherwise monoubiquitinated mutant p53. Caffeine treatment rescued MDM2-dependent proteasome degradation of mutant p53 in cells exhibiting active DNA damage signaling, and ATM knockdown phenocopied the caffeine effect. Importantly, in cells analyzed individually by flow cytometry, p53 levels were highest in cells exhibiting the greatest levels of DNA damage response, and interference with DNA damage signaling preferentially decreased the relative percentage of cells in a population with the highest levels of mutant p53. These data demonstrate that active DNA damage signaling contributes to high levels of mutant p53 via modulation of ubiquitin/proteasome activity toward p53. Implication The ability of DNA damage checkpoint signaling to mediate accumulation of mutant p53 suggests that targeting this signaling pathway may provide therapeutic gain.

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“…Generation of plasmids and lentiviral vectors (pLKO.1) expressing short hairpin (sh) RNA against MDM2 or non-endogenous green fluorescence protein (GFP) from U6 promoter and harboring a puromycin resistance gene has been described earlier (20,29). …”

Section: Methodsmentioning

confidence: 99%

The human oncoprotein MDM2 induces replication stress eliciting early intra-S-phase checkpoint response and inhibition of DNA replication origin firing

Frum

Singh

Vaughan

et al. 2013

Nucleic Acids Research

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Conventional paradigm ascribes the cell proliferative function of the human oncoprotein mouse double minute2 (MDM2) primarily to its ability to degrade p53. Here we report that in the absence of p53, MDM2 induces replication stress eliciting an early S-phase checkpoint response to inhibit further firing of DNA replication origins. Partially synchronized lung cells cultured from p53−/−:MDM2 transgenic mice enter S phase and induce S-phase checkpoint response earlier than lung cells from p53−/− mice and inhibit firing of DNA replication origins. MDM2 activates chk1 phosphorylation, elevates mixed lineage lymphoma histone methyl transferase levels and promotes checkpoint-dependent tri-methylation of histone H3 at lysine 4, known to prevent firing of late replication origins at the early S phase. In the absence of p53, a condition that disables inhibition of cyclin A expression by MDM2, MDM2 increases expression of cyclin D2 and A and hastens S-phase entry of cells. Consistently, inhibition of cyclin-dependent kinases, known to activate DNA replication origins during firing, inhibits MDM2-mediated induction of chk1 phosphorylation indicating the requirement of this activity in MDM2-mediated chk1 phosphorylation. Our data reveal a novel pathway, defended by the intra-S-phase checkpoint, by which MDM2 induces unscheduled origin firing and accelerates S-phase entry of cells in the absence of p53.

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Human oncoprotein MDM2 activates the Akt signaling pathway through an interaction with the repressor element-1 silencing transcription factor conferring a survival advantage to cancer cells

Cited by 35 publications

References 40 publications

Mutant p53 establishes targetable tumor dependency by promoting unscheduled replication

Mutant p53 establishes targetable tumor dependency by promoting unscheduled replication

Constitutive Activation of DNA Damage Checkpoint Signaling Contributes to Mutant p53 Accumulation via Modulation of p53 Ubiquitination

The human oncoprotein MDM2 induces replication stress eliciting early intra-S-phase checkpoint response and inhibition of DNA replication origin firing

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