Inactivation of Mdm2 Restores Apoptosis Proficiency of Cooperativity Mutant P53 in Vivo

Overview

Journal Cell Cycle

Specialty Cell Biology

Date 2019 Nov 22

PMID 31749402

Citations 5

Authors

Boris Klimovich

Thorsten Stiewe

Oleg Timofeev

Affiliations

Soon will be listed here.

Abstract

mutations are found in 50% of all cancers and mutated status is considered poor for treatment. However, some mutations exhibit only partial loss-of-function (LOF), meaning they retain residual transcriptional and non-transcriptional activities that are potentially beneficial for therapy. Earlier we have characterized a knock-in mouse model for the partial LOF mutant (p53RR). Reduced DNA binding cooperativity of this mutant led to the loss of p53-dependent apoptosis, while p53 functions in cell cycle control, senescence, metabolism, and antioxidant defense remained intact. Concomitantly, tumor suppression was evident but strongly compromised compared to wild-type mice. Here we used the mouse as a model to investigate whether residual functions of mutant p53 can be engaged to induce cell death, which is considered the most desirable outcome of tumor therapy. We made use of knock-out in developing embryos as a sensitive tool for detecting remaining p53 activities. Genetic ablation of led to embryonic lethality in homozygotes at days 9.5-11.5. This effect was not rescued by concomitant p21-knockout, indicating its independence of p21-mediated cell cycle arrest. Instead, immunohistochemical analysis showed widespread apoptosis in tissues of defective embryos accompanied by persistent accumulation of p53RR protein. This led to partial restoration of the mutant's proficiency in transcriptional induction of the pro-apoptotic genes (Puma) and . These data indicate that increased quantity can compensate for qualitative defects of p53 mutants and suggest that Mdm2-targeting (potentially in combination with other drugs) might be effective against cells bearing p53 partial LOF mutants.

Citing Articles

Partial p53 reactivation is sufficient to induce cancer regression.

Klimovich B, Meyer L, Merle N, Neumann M, Konig A, Ananikidis N J Exp Clin Cancer Res. 2022; 41(1):80.

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Effect of Sperm Cryopreservation on miRNA Expression and Early Embryonic Development.

Xu X, Li W, Zhang L, Ji Y, Qin J, Wang L Front Cell Dev Biol. 2022; 9:749486.

PMID: 35004670 PMC: 8728010. DOI: 10.3389/fcell.2021.749486.

p53 partial loss-of-function mutations sensitize to chemotherapy.

Klimovich B, Merle N, Neumann M, Elmshauser S, Nist A, Mernberger M Oncogene. 2021; 41(7):1011-1023.

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Rely on Each Other: DNA Binding Cooperativity Shapes p53 Functions in Tumor Suppression and Cancer Therapy.

Timofeev O, Stiewe T Cancers (Basel). 2021; 13(10).

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Commensal microbes and p53 in cancer progression.

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