Wild-type p53 oligomerizes more efficiently than p53 hot-spot mutants and overcomes mutant p53 gain-of-function via a “dominant-positive” mechanism

Dawid Walerych; Magdalena Pruszko; Lukasz Zyla; Michalina Wezyk; Katarzyna Gaweda-Walerych; Alicja Zylicz

doi:10.18632/oncotarget.25944

Mutant p53 Sequestration of the MDM2 Acidic Domain Inhibits E3 Ligase Activity

Molecular and Cellular Biology ◽

10.1128/mcb.00375-18 ◽

2018 ◽

Vol 39 (4) ◽

Cited By ~ 3

Author(s):

Leixiang Yang ◽

Tanjing Song ◽

Qian Cheng ◽

Lihong Chen ◽

Jiandong Chen

Keyword(s):

Tumor Cells ◽

Recent Work ◽

Intramolecular Interaction ◽

E3 Ligase ◽

Mutant P53 ◽

Wild Type ◽

Gain Of Function ◽

Core Domain ◽

Acidic Domain ◽

Wild Type P53

ABSTRACT Missense p53 mutants often accumulate in tumors and drive progression through gain of function. MDM2 efficiently degrades wild-type p53 but fails to degrade mutant p53 in tumor cells. Previous studies revealed that mutant p53 inhibits MDM2 autoubiquitination, suggesting that the interaction inhibits MDM2 E3 activity. Recent work showed that MDM2 E3 activity is stimulated by intramolecular interaction between the RING and acidic domains. Here, we show that in the mutant p53-MDM2 complex, the mutant p53 core domain binds to the MDM2 acidic domain with significantly higher avidity than wild-type p53. The mutant p53-MDM2 complex is deficient in catalyzing ubiquitin release from the activated E2 conjugating enzyme. An MDM2 construct with extra copies of the acidic domain is resistant to inhibition by mutant p53 and efficiently promotes mutant p53 ubiquitination and degradation. The results suggest that mutant p53 interferes with the intramolecular autoactivation mechanism of MDM2, contributing to reduced ubiquitination and increased accumulation in tumor cells.

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Mutant p53 Disrupts MCF-10A Cell Polarity in Three-dimensional Culture via Epithelial-to-mesenchymal Transitions

Journal of Biological Chemistry ◽

10.1074/jbc.m110.214585 ◽

2011 ◽

Vol 286 (18) ◽

pp. 16218-16228 ◽

Cited By ~ 60

Author(s):

Yanhong Zhang ◽

Wensheng Yan ◽

Xinbin Chen

Keyword(s):

Cell Polarity ◽

Expression Patterns ◽

Ectopic Expression ◽

Three Dimensional ◽

Mutant P53 ◽

Wild Type ◽

Gain Of Function ◽

Three Dimensional Culture ◽

Wild Type P53 ◽

E Cadherin

Mutant p53 is not only deficient in tumor suppression but also acquires additional activity, called gain of function. Mutant p53 gain of function is recapitulated in knock-in mice that carry one null allele and one mutant allele of the p53 gene. These knock-in mice develop aggressive tumors compared with p53-null mice. Recently, we and others showed that tumor cells carrying a mutant p53 are addicted to the mutant for cell survival and resistance to DNA damage. To further define mutant p53 gain of function, we used the MCF-10A three-dimensional model of mammary morphogenesis. MCF-10A cells in three-dimensional culture undergo a series of morphological changes and form polarized and growth-arrested spheroids with hollow lumen, which resembles normal glandular architectures in vivo. Here, we found that endogenous wild-type p53 in MCF-10A cells was not required for acinus formation, but knockdown of endogenous wild-type p53 (p53-KD) led to partial clearance of cells in the lumen due to decreased apoptosis. Consistent with this, p53-KD altered expression patterns of the cell adhesion molecule E-cadherin, the cytoskeletal marker β-catenin, and the extracellular matrix protein laminin V. We also found that ectopic expression of the mutant G245S led to a phenotype similar to p53-KD, whereas a combination of ectopic expression of siRNA-resistant G245S with p53-KD led to a less cleared lumen. In contrast, ectopic expression of mutant R248W, R175H, and R273H disrupted normal acinus architectures with filled lumen and led to formation of irregular and multiacinus structures regardless of p53-KD. In addition, these mutants altered normal expression patterns and/or levels of E-cadherin, β-catenin, laminin V, and tight junction marker ZO-1. Furthermore, epithelial-to-mesenchymal transitions (EMT) markers, Snail, Slug, and Twist, were highly induced by mutant p53 and/or p53-KD. Together, we postulate that EMT represents a mutant p53 gain of function and mutant p53 alters cell polarity via EMT.

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Mutant p53: Gain-of-Function Oncoproteins and Wild-Type p53 Inactivators

Biological Chemistry ◽

10.1515/bc.1999.108 ◽

1999 ◽

Vol 380 (7-8) ◽

Cited By ~ 55

Author(s):

K. Roemer

Keyword(s):

Mutant P53 ◽

Wild Type ◽

Gain Of Function ◽

Wild Type P53

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Gain-of-function mutant p53 in cancer progression and therapy

Journal of Molecular Cell Biology ◽

10.1093/jmcb/mjaa040 ◽

2020 ◽

Vol 12 (9) ◽

pp. 674-687 ◽

Cited By ~ 4

Author(s):

Cen Zhang ◽

Juan Liu ◽

Dandan Xu ◽

Tianliang Zhang ◽

Wenwei Hu ◽

...

Keyword(s):

Cancer Progression ◽

P53 Gene ◽

Amino Acid Difference ◽

Protein Accumulation ◽

Mutant P53 ◽

P53 Mutations ◽

Wild Type ◽

Gain Of Function ◽

Human Cancers ◽

Wild Type P53

Abstract p53 is a key tumor suppressor, and loss of p53 function is frequently a prerequisite for cancer development. The p53 gene is the most frequently mutated gene in human cancers; p53 mutations occur in >50% of all human cancers and in almost every type of human cancers. Most of p53 mutations in cancers are missense mutations, which produce the full-length mutant p53 (mutp53) protein with only one amino acid difference from wild-type p53 protein. In addition to loss of the tumor-suppressive function of wild-type p53, many mutp53 proteins acquire new oncogenic activities independently of wild-type p53 to promote cancer progression, termed gain-of-function (GOF). Mutp53 protein often accumulates to very high levels in cancer cells, which is critical for its GOF. Given the high mutation frequency of the p53 gene and the GOF activities of mutp53 in cancer, therapies targeting mutp53 have attracted great interest. Further understanding the mechanisms underlying mutp53 protein accumulation and GOF will help develop effective therapies treating human cancers containing mutp53. In this review, we summarize the recent advances in the studies on mutp53 regulation and GOF as well as therapies targeting mutp53 in human cancers.

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The effects of wild-type p53 tumor suppressor activity and mutant p53 gain-of-function on cell growth

Gene ◽

10.1016/s0378-1119(01)00696-5 ◽

2001 ◽

Vol 277 (1-2) ◽

pp. 15-30 ◽

Cited By ~ 151

Author(s):

Craig Cadwell ◽

Gerard P Zambetti

Keyword(s):

Cell Growth ◽

Tumor Suppressor ◽

Mutant P53 ◽

Wild Type ◽

Gain Of Function ◽

Suppressor Activity ◽

P53 Tumor Suppressor ◽

Tumor Suppressor Activity ◽

Wild Type P53

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Inhibitory effects of antagonists of growth hormone releasing hormone on experimental prostate cancers are associated with upregulation of wild-type p53 and decrease in p21 and mutant p53 proteins

The Prostate ◽

10.1002/pros.21458 ◽

2011 ◽

Vol 72 (5) ◽

pp. 555-565 ◽

Cited By ~ 22

Author(s):

Anton Stangelberger ◽

Andrew V. Schally ◽

Ferenc G. Rick ◽

Jozsef L. Varga ◽

Benjamin Baker ◽

...

Keyword(s):

Growth Hormone ◽

Mutant P53 ◽

Growth Hormone Releasing Hormone ◽

Wild Type ◽

Inhibitory Effects ◽

Releasing Hormone ◽

Wild Type P53 ◽

Prostate Cancers

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Site-specific binding of wild-type p53 to cellular DNA is inhibited by SV40 T antigen and mutant p53.

Genes & Development ◽

10.1101/gad.6.10.1886 ◽

1992 ◽

Vol 6 (10) ◽

pp. 1886-1898 ◽

Cited By ~ 143

Author(s):

J Bargonetti ◽

I Reynisdottir ◽

P N Friedman ◽

C Prives

Keyword(s):

Specific Binding ◽

T Antigen ◽

Mutant P53 ◽

Wild Type ◽

Sv40 T Antigen ◽

Site Specific ◽

Wild Type P53 ◽

Cellular Dna

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Human p53 and CDC2Hs genes combine to inhibit the proliferation of Saccharomyces cerevisiae

Molecular and Cellular Biology ◽

10.1128/mcb.12.3.1357-1365.1992 ◽

1992 ◽

Vol 12 (3) ◽

pp. 1357-1365

Author(s):

J M Nigro ◽

R Sikorski ◽

S I Reed ◽

B Vogelstein

Keyword(s):

Saccharomyces Cerevisiae ◽

Growth Inhibition ◽

Mammalian Cells ◽

P53 Protein ◽

Inducible Promoter ◽

Mutant P53 ◽

Wild Type ◽

Growth Inhibitory Activity ◽

Wild Type P53 ◽

P53 Genes

Human wild-type and mutant p53 genes were expressed under the control of a galactose-inducible promoter in Saccharomyces cerevisiae. The growth rate of the yeast was reduced in cells expressing wild-type p53, whereas cells transformed with mutant p53 genes derived from human tumors were less affected. Coexpression of the normal p53 protein with the human cell cycle-regulated protein kinase CDC2Hs resulted in much more pronounced growth inhibition that for p53 alone. Cells expressing p53 and CDC2Hs were partially arrested in G1, as determined by morphological analysis and flow cytometry. p53 was phosphorylated when expressed in the yeast, but differences in phosphorylation did not explain the growth inhibition attributable to coexpression of p53 and CDC2Hs. These results suggest that wild-type p53 has a growth-inhibitory activity in S. cerevisiae similar to that observed in mammalian cells and suggests that this yeast may provide a useful model for defining the pathways through which p53 acts.

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Crosstalk between p53 and TGF-β Signalling

Journal of Signal Transduction ◽

10.1155/2012/294097 ◽

2012 ◽

Vol 2012 ◽

pp. 1-10 ◽

Cited By ~ 55

Author(s):

Rebecca Elston ◽

Gareth J. Inman

Keyword(s):

Transcriptional Activation ◽

Cancer Biology ◽

Target Genes ◽

Tumour Progression ◽

Signal Transduction Pathway ◽

Mirna Biogenesis ◽

Mutant P53 ◽

Wild Type ◽

P53 Family ◽

Wild Type P53

Wild-type p53 and TGF-β are key tumour suppressors which regulate an array of cellular responses. TGF-β signals in part via the Smad signal transduction pathway. Wild-type p53 and Smads physically interact and coordinately induce transcription of a number of key tumour suppressive genes. Conversely mutant p53 generally subverts tumour suppressive TGF-β responses, diminishing transcriptional activation of key TGF-β target genes. Mutant p53 can also interact with Smads and this enables complex formation with the p53 family member p63 and blocks p63-mediated activation of metastasis suppressing genes to promote tumour progression. p53 and Smad function may also overlap during miRNA biogenesis as they can interact with the same components of the Drosha miRNA processing complex to promote maturation of specific subsets of miRNAs. This paper investigates the crosstalk between p53 and TGF-β signalling and the potential roles this plays in cancer biology.

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The mdm-2 oncogene can overcome wild-type p53 suppression of transformed cell growth

Molecular and Cellular Biology ◽

10.1128/mcb.13.1.301-306.1993 ◽

1993 ◽

Vol 13 (1) ◽

pp. 301-306 ◽

Cited By ~ 1

Author(s):

C A Finlay

Keyword(s):

P53 Protein ◽

Mutant P53 ◽

Wild Type ◽

Rat Embryo ◽

Ras Gene ◽

Double Minute ◽

Murine Double Minute ◽

Low Levels ◽

Wild Type P53 ◽

P53 Genes

Expression of a p53-associated protein, Mdm-2 (murine double minute-2), can inhibit p53-mediated transactivation. In this study, overexpression of the Mdm-2 protein was found to result in the immortalization of primary rat embryo fibroblasts (REFs) and, in conjunction with an activated ras gene, in the transformation of REFs. The effect of wild-type p53 on the transforming properties of mdm-2 was determined by transfecting REFs with ras, mdm-2, and normal p53 genes. Transfection with ras plus mdm-2 plus wild-type p53 resulted in a 50% reduction in the number of transformed foci (relative to the level for ras plus mdm-2); however, more than half (9 of 17) of the cell lines derived from these foci expressed low levels of a murine p53 protein with the characteristics of a wild-type p53. These results are in contrast to previous studies which demonstrated that even minimal levels of wild-type p53 are not tolerated in cells transformed by ras plus myc, E1A, or mutant p53. The mdm-2 oncogene can overcome the previously demonstrated growth-suppressive properties of p53.

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