2015
DOI: 10.1038/onc.2015.76
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MDM4/HIPK2/p53 cytoplasmic assembly uncovers coordinated repression of molecules with anti-apoptotic activity during early DNA damage response

Abstract: The p53 inhibitor, MDM4 (MDMX) is a cytoplasmic protein with p53-activating function under DNA damage conditions. Particularly, MDM4 promotes phosphorylation of p53 at Ser46, a modification that precedes different p53 activities. We investigated the mechanism by which MDM4 promotes this p53 modification and its consequences in untransformed mammary epithelial cells and tissues. In response to severe DNA damage, MDM4 stimulates p53Ser46P by binding and stabilizing serine–threonine kinase HIPK2. Under these cond… Show more

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Cited by 34 publications
(32 citation statements)
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“…This MDM4 function is in agreement with its pro-apoptotic activity under DNA damage and support a model of MDM4 with anti-oncogenic activities in stress conditions [43]. Furthermore, these data together with the previous report of MDM4 functioning as a bridge for phosphorylation of p53 [7], contribute to define MDM4 as a cytoplasmic scaffold ready to sense different stimuli – i.e. DNA damage, cell starvation – and to accordingly regulate cell growth by recruiting different partners.…”
Section: Discussionsupporting
confidence: 86%
“…This MDM4 function is in agreement with its pro-apoptotic activity under DNA damage and support a model of MDM4 with anti-oncogenic activities in stress conditions [43]. Furthermore, these data together with the previous report of MDM4 functioning as a bridge for phosphorylation of p53 [7], contribute to define MDM4 as a cytoplasmic scaffold ready to sense different stimuli – i.e. DNA damage, cell starvation – and to accordingly regulate cell growth by recruiting different partners.…”
Section: Discussionsupporting
confidence: 86%
“…The observation that the preferred response elicited by Pep3 is apoptosis is also in agreement with recent data from our and other labs that reported impairment of MDM4/MDM2 heterodimer function during apoptosis (22,(39)(40)(41). Importantly, this observation highlights the potential therapeutic value of targeting the MDM2/MDM4 heterodimers.…”
Section: Discussionsupporting
confidence: 80%
“…In agreement with these data, the lethality of the mdm4 and mdm2 KO mice is accomplished by an apoptotic outcome in the mdm2 KO and mostly by a growth arrest response in the mdm4 KO [23,24,25]. The dissociation of MDM4 from MDM2 increases the activation of p53 whereas the association of MDM2 to MDM4 counteracts the proapoptotic activity of the last [34]. …”
Section: Introductionmentioning
confidence: 82%