Tumor suppressor protein p53 expressed in yeast can remain diffuse, form a prion, or form unstable liquid-like droplets

Park, Sei-Kyoung; Park, Sangeun; Pentek, Christine; Liebman, Susan W.

doi:10.1016/j.isci.2020.102000

Cited by 24 publications

(26 citation statements)

References 86 publications

(79 reference statements)

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“…Overexpression of these same chaperones in cells not coexpressing p53 has no such effect (Sopko et al 2006;Johnson et al 2015). High-level p53 expression is toxic to yeast and is thought to involve p53 binding to endogenous yeast genes and thereby perturbing essential gene expression (Inga and Resnick 2001;Leão et al 2013;Park et al 2021). We noticed that the chaperones with the strongest effect on non-selective growth (i.e., those that induced the most p53 "toxicity") had the work, these results support the idea that p53 toxicity in yeast requires nuclear localization.…”

Section: Overexpression Of Specific Chaperones Inhibits P53(v272m) Functionsupporting

confidence: 72%

“…Indeed, experiments in mammalian cells with a different TS p53 mutant, C135V, suggested that at high temperature binding of cytosolic Hsp70 chaperones to the mutant p53 renders the NLS inaccessible without directly occluding it (Akakura et al 2001). p53 expressed in yeast can adopt several forms with distinct localization patternsboth punctate and diffuse, and in the cytosol, vacuole, or nucleussome of which can be stably propagated in prion-like ways, suggesting conformational changes in p53 drive the changes in localization (Park et al 2021). Since most of the chaperones we overexpressed are normally found diffusely in the cytosol, we think that the distinct patterns of p53 mislocalization outside the nucleus upon overexpression of distinct chaperones (punctate, diffuse, vacuolar) may have more to do with the conformation of p53 resulting from chaperone interaction than with chaperone binding per se.…”

Section: )mentioning

confidence: 99%

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Selective functional inhibition of a tumor-derived p53 mutant by cytosolic chaperones identified using split-YFP in budding yeast

Denney

Weems

McMurray

2021

Preprint

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Life requires the oligomerization of individual proteins into higher-order assemblies. In order to form functional oligomers, monomers must adopt appropriate three-dimensional structures. Molecular chaperones transiently bind nascent or misfolded proteins to promote proper folding. Single missense mutations frequently cause disease by perturbing folding despite chaperone engagement. A misfolded mutant capable of oligomerizing with wild-type proteins can dominantly poison oligomer function. We previously found evidence that human-disease-linked mutations in Saccharomyces cerevisiae septin proteins slow folding and attract chaperones, resulting in a kinetic delay in oligomerization that prevents the mutant from interfering with wild-type function. Here we build upon our septin studies to develop a new approach to identifying chaperone interactions in living cells, and use it to expand our understanding of chaperone involvement, kinetic folding delays, and oligomerization in the recessive behavior of tumor-derived mutants of the tumor suppressor p53. We find evidence of increased binding of several cytosolic chaperones to a recessive, misfolding-prone mutant, p53(V272M). Similar to our septin results, chaperone overexpression inhibits the function of p53(V272M) with minimal effect on the wild type. Unlike mutant septins, p53(V272M) is not kinetically delayed under conditions in which it is functional. Instead, it interacts with wild-type p53 but this interaction is temperature sensitive. At high temperatures or upon chaperone overexpression, p53(V272M) is excluded from the nucleus and cannot function or perturb wild-type function. Chaperone inhibition liberates the mutant to enter the nucleus where it has a slight dominant-negative effect. These findings provide new insights into the effects of missense mutations.

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Section: Overexpression Of Specific Chaperones Inhibits P53(v272m) Functionsupporting

confidence: 72%

Section: )mentioning

confidence: 99%

Selective functional inhibition of a tumor-derived p53 mutant by cytosolic chaperones identified using split-YFP in budding yeast

Denney

Weems

McMurray

2021

Preprint

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“… 64 Interestingly, transient p53 overexpression in yeast induced the formation of p53 prion aggregates; however, liquid-like p53 condensates were generated in response to stress and disappeared after stress removal. 65 …”

Section: Discussionmentioning

confidence: 99%

Phase separation of p53 precedes aggregation and is affected by oncogenic mutations and ligands

et al. 2021

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“…However, as soon as mutant p53 expression was shut off, wild-type p53 fully recovered its transcriptional abilities [14]. These results thus show that mutant p53 did not print its [p53 MUT ] conformation on wild-type p53 in a prion-like manner in S. cerevisiae, although recent data also suggest that when fused to EYFP, p53 overexpression leads, in some rare yeast cells, to the formation of aggregates that are transmitted across generations [161]. Altogether, these data show that the dominant-negative effect of mutant p53 is dose-dependent and can be reduced or even neutralized by increasing the wild-type/mutant p53 ratio.…”

Section: P53 Aggregation: the Trapping Evidencementioning

confidence: 76%

p53, A Victim of the Prion Fashion

Friocourt

Roux

Voisset

2021

Cancers

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Identified in the late 1970s as an oncogene, a driving force leading to tumor development, p53 turned out to be a key tumor suppressor gene. Now p53 is considered a master gene regulating the transcription of over 3000 target genes and controlling a remarkable number of cellular functions. The elevated prevalence of p53 mutations in human cancers has led to a recurring questioning about the roles of mutant p53 proteins and their functional consequences. Both mutants and isoforms of p53 have been attributed dominant-negative and gain of function properties among which is the ability to form amyloid aggregates and behave in a prion-like manner. This report challenges the ongoing “prion p53” hypothesis by reviewing evidence of p53 behavior in light of our current knowledge regarding amyloid proteins, prionoids and prions.

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Tumor suppressor protein p53 expressed in yeast can remain diffuse, form a prion, or form unstable liquid-like droplets

Cited by 24 publications

References 86 publications

Selective functional inhibition of a tumor-derived p53 mutant by cytosolic chaperones identified using split-YFP in budding yeast

Selective functional inhibition of a tumor-derived p53 mutant by cytosolic chaperones identified using split-YFP in budding yeast

Phase separation of p53 precedes aggregation and is affected by oncogenic mutations and ligands

p53, A Victim of the Prion Fashion

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