Hsp70 molecular chaperones are required to support p53 tumor suppressor activity under stress conditions

Walerych, Dawid; Olszewski, Maciej B.; Gutkowska, Małgorzata; Helwak, Aleksandra; Żylicz, Maciej; Żylicz, Alicja

doi:10.1038/onc.2009.281

Cited by 77 publications

(79 citation statements)

References 47 publications

(51 reference statements)

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“…Further, in vivo studies using firefly luciferase as a model substrate have documented the role of Hsp90 in protecting the proteins during stress and its role in refolding of non-native structures and degradation of terminally misfolded proteins during recovery from stress (Schneider et al, 1996). Hsp90-HOP, together with Hsp70-Hsp40 functions as a folding machine, also called foldosome that participates in the refolding of stress-denatured proteins during the recovery phase and prevents aggregation of misfolded proteins (Hutchison et al, 1994;McClellan et al, 2007;Powers et al, 2008;Schumacher et al, 1996;Walerych et al, 2009;Wegele et al, 2006). The Hsp90 reservoir, besides buffering proteostasis against environmental stress, is also involved in safeguarding protein functions in context of genetic variation.…”

Section: Ii41122 the Hsp90 Chaperone Systemmentioning

confidence: 99%

“…It could be due to the direct effect of 17-AAG on the folding machinery of cells. Hsp90 has been shown to co-operate with Hsp70-Hsp40 via the co-chaperones such as HOP in refolding stress-denatured proteins and in preventing misfolded proteins to form aggregates (Hutchison et al, 1994;McClellan et al, 2007;Powers et al, 2008;Schumacher et al, 1996;Walerych et al, 2009;Wegele et al, 2006). Additionally, Hsp90 inhibition has been shown to induce transcription of HSPs by HSF1 mediated activation (Sittler et al, 2001).…”

Section: Vi2 Assessment Of Folding Capacity Of Cells Using Fluc-basmentioning

confidence: 99%

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Firefly luciferase mutants as sensors of proteome stress

et al. 2011

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Section: Ii41122 the Hsp90 Chaperone Systemmentioning

confidence: 99%

Section: Vi2 Assessment Of Folding Capacity Of Cells Using Fluc-basmentioning

confidence: 99%

Firefly luciferase mutants as sensors of proteome stress

et al. 2011

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“…Several clinical trials have been based on strategies to reintroduce wildtype P53 copies into cancerous tissues (27)(28)(29). In addition, there have been several clinical attempts to use molecular chaperones that can rescue wildtype P53 (30)(31)(32)(33). Because of the oncogenic role of mutant P53 (3,26), reactivation of transcriptionally inactive mutant P53 is a promising approach to cancer therapy (30).…”

Section: P53mentioning

confidence: 99%

The curcumin analog HO-3867 selectively kills cancer cells by converting mutant p53 protein to transcriptionally active wildtype p53

Madan

Parker

Bauer

et al. 2018

Journal of Biological Chemistry

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“…In our previous reports we have established that Hsp90 rescues the WT p53 tumor suppressor protein activity at physiological temperature in a single chaperone reaction. We demonstrated that WT p53 binding to the specific DNA promoter sequence in vitro at physiological temperature is Hsp90-and ATP-dependent and that the p53 transcriptional activity in cells requires Hsp90 (25,26). WT p53 was shown to bind to Hsp90 in native or nearly native conformation (27).…”

mentioning

confidence: 99%

ATP Binding to Hsp90 Is Sufficient for Effective Chaperoning of p53 Protein

Walerych

Gutkowska

Klejman

et al. 2010

Journal of Biological Chemistry

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Hsp90 is a ubiquitous, ATP-dependent chaperone, essential for eukaryotes. It possesses a broad spectrum of substrates, among which is the p53 transcription factor, encoded by a tumor-suppressor gene. Here, we elucidate the role of the adenine nucleotide in the Hsp90 chaperone cycle, by taking advantage of a unique in vitro assay measuring Hsp90-dependent p53 binding to the promoter sequence. E42A and D88N Hsp90␤ variants bind but do not hydrolyze ATP, whereas E42A has increased and D88N decreased ATP affinity, compared with WT Hsp90␤. Nevertheless, both of these mutants interact with WT p53 with a similar affinity. Surprisingly, in the case of WT, but also E42A Hsp90␤, the presence of ATP stimulates dissociation of Hsp90-p53 complexes and results in p53 binding to the promoter sequence. D88N Hsp90␤ is not efficient in both of these reactions. Using a trap version of the chaperonin GroEL, which irreversibly captures unfolded proteins, we show that Hsp90 chaperone action on WT p53 results in a partial unfolding of the substrate. The ATP-dependent dissociation of p53-Hsp90 complex allows further folding of p53 protein to an active conformation, able to bind to the promoter sequence. Furthermore, in support of these results, the overproduction of WT or E42A Hsp90␤ stimulates transcription from the WAF1 gene promoter in H1299 cells. Altogether, our research indicates that ATP binding to Hsp90␤ is a sufficient step for effective WT p53 client protein chaperoning.Hsp90 is an abundant protein in cells of all known organisms, with the exception of the Archea kingdom. Although in bacteria its presence is not required for survival (1), yeast and higher eukaryotes are fully dependent on its activity (2, 3). In multicellular organisms Hsp90 plays a key role in the activation and stabilization of various protein substrates. Among these are kinases (Raf1, Akt, and Src), telomerase, Rab GDP dissociation inhibitors, glucocorticoid hormone receptors (GR), 3 and transcription factors such as the p53 tumor suppressor protein (4 -6). These Hsp90 substrates belong to different protein families and do not share common sequence or structural motifs. Hence, modes of interaction and chaperoning may possess both common features and specific differences.Hsp90 is functional as a dimer, each monomer consisting of three domains connected with flexible linkers of different length and sequence depending on organism and isoform. The main substrate binding region is proposed to be localized in the middle domain (7), however structural (8) and biochemical studies (9 -11) suggest that at least two distinct surfaces of interaction should exist on Hsp90 chaperone while binding its protein substrate. Repositioning of the domains of the Hsp90 may be translated into conformational rearrangements of a protein substrate, changing its tertiary structure and exposing buried residues, thus enabling interaction with other proteins and ligands, such as hormones or nucleic acids.Despite the initial controversy on the ATP dependence of Hsp90 (12), it was unambig...

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Hsp70 molecular chaperones are required to support p53 tumor suppressor activity under stress conditions

Cited by 77 publications

References 47 publications

Firefly luciferase mutants as sensors of proteome stress

Firefly luciferase mutants as sensors of proteome stress

The curcumin analog HO-3867 selectively kills cancer cells by converting mutant p53 protein to transcriptionally active wildtype p53

ATP Binding to Hsp90 Is Sufficient for Effective Chaperoning of p53 Protein

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