Restoration of the Tumor Suppressor Function of Y220C-Mutant p53 by Rezatapopt, a Small-Molecule Reactivator

Anna M. Puzio-Kuter; Lizhong Xu; Mary Kate McBrayer; Romyr Dominique; Hongju H. Li; Bruce J. Fahr; Alyssa M. Brown; Amy E. Wiebesiek; Brandon M. Russo; Chris L. Mulligan; Hong Yang; Josh Battaglia; Kimberly A. Robell; Dafydd H. Thomas; Kuo Sen Huang; Alexander Solovyov; Benjamin D. Greenbaum; Jonathan D. Oliner; Thomas W. Davis; Melissa L. Dumble; Melissa L. Johnson; Shunbin Xiong; Peirong Yang; Guillermina Lozano; Marc M. Fellous; Binh T. Vu; Alison M. Schram; Arnold J. Levine; Masha V. Poyurovsky

doi:10.1158/2159-8290.CD-24-1421

Restoration of the Tumor Suppressor Function of Y220C-Mutant p53 by Rezatapopt, a Small-Molecule Reactivator

Anna M. Puzio-Kuter
, Lizhong Xu
, Mary Kate McBrayer
, Romyr Dominique
, Hongju H. Li
, Bruce J. Fahr
, Alyssa M. Brown
, Amy E. Wiebesiek
, Brandon M. Russo
, Chris L. Mulligan
, Hong Yang
, Josh Battaglia
, Kimberly A. Robell
, Dafydd H. Thomas
, Kuo Sen Huang
, Alexander Solovyov
, Benjamin D. Greenbaum
, Jonathan D. Oliner
, Thomas W. Davis
, Melissa L. Dumble

Melissa L. Johnson, Shunbin Xiong, Peirong Yang, Guillermina Lozano, Marc M. Fellous, Binh T. Vu, Alison M. Schram, Arnold J. Levine, Masha V. Poyurovsky

Research output: Contribution to journal › Article › peer-review

18 Scopus citations

Abstract

Restoration of the tumor suppressor function of tumor-associated p53 mutants, including the Y220C substitution, has posed a significant challenge for therapeutic discovery. In this study, we describe rezatapopt (PC14586), part of a series of compounds designed to reactivate the p53 Y220C mutant. These compounds restore p53 tumor suppressor function by correcting its conformation and enabling it to bind DNA and activate downstream target genes, thus inducing antiproliferative changes in tumor cells. Our findings are supported by biochemical and structural analysis, in vitro and in vivo transcriptomics, and functional data, revealing the recovery of multiple aspects of the wild-type p53 program. These compounds demonstrate potent antitumor activity in preclinical models as single agents and in combination with immunotherapy. Currently, rezatapopt is being evaluated in a registrational phase II clinical trial for patients with advanced solid tumors harboring the TP53 Y220C mutation.

Original language	English
Pages (from-to)	1159-1179
Number of pages	21
Journal	Cancer Discovery
Volume	15
Issue number	6
DOIs	https://doi.org/10.1158/2159-8290.CD-24-1421
State	Published - 1 Jun 2025
Externally published	Yes

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Puzio-Kuter, A. M., Xu, L., McBrayer, M. K., Dominique, R., Li, H. H., Fahr, B. J., Brown, A. M., Wiebesiek, A. E., Russo, B. M., Mulligan, C. L., Yang, H., Battaglia, J., Robell, K. A., Thomas, D. H., Huang, K. S., Solovyov, A., Greenbaum, B. D., Oliner, J. D., Davis, T. W., ... Poyurovsky, M. V. (2025). Restoration of the Tumor Suppressor Function of Y220C-Mutant p53 by Rezatapopt, a Small-Molecule Reactivator. Cancer Discovery, 15(6), 1159-1179. https://doi.org/10.1158/2159-8290.CD-24-1421

@article{ca0e22170da74bca8b25674ab3e42f1e,

title = "Restoration of the Tumor Suppressor Function of Y220C-Mutant p53 by Rezatapopt, a Small-Molecule Reactivator",

abstract = "Restoration of the tumor suppressor function of tumor-associated p53 mutants, including the Y220C substitution, has posed a significant challenge for therapeutic discovery. In this study, we describe rezatapopt (PC14586), part of a series of compounds designed to reactivate the p53 Y220C mutant. These compounds restore p53 tumor suppressor function by correcting its conformation and enabling it to bind DNA and activate downstream target genes, thus inducing antiproliferative changes in tumor cells. Our findings are supported by biochemical and structural analysis, in vitro and in vivo transcriptomics, and functional data, revealing the recovery of multiple aspects of the wild-type p53 program. These compounds demonstrate potent antitumor activity in preclinical models as single agents and in combination with immunotherapy. Currently, rezatapopt is being evaluated in a registrational phase II clinical trial for patients with advanced solid tumors harboring the TP53 Y220C mutation.",

author = "Puzio-Kuter, \{Anna M.\} and Lizhong Xu and McBrayer, \{Mary Kate\} and Romyr Dominique and Li, \{Hongju H.\} and Fahr, \{Bruce J.\} and Brown, \{Alyssa M.\} and Wiebesiek, \{Amy E.\} and Russo, \{Brandon M.\} and Mulligan, \{Chris L.\} and Hong Yang and Josh Battaglia and Robell, \{Kimberly A.\} and Thomas, \{Dafydd H.\} and Huang, \{Kuo Sen\} and Alexander Solovyov and Greenbaum, \{Benjamin D.\} and Oliner, \{Jonathan D.\} and Davis, \{Thomas W.\} and Dumble, \{Melissa L.\} and Johnson, \{Melissa L.\} and Shunbin Xiong and Peirong Yang and Guillermina Lozano and Fellous, \{Marc M.\} and Vu, \{Binh T.\} and Schram, \{Alison M.\} and Levine, \{Arnold J.\} and Poyurovsky, \{Masha V.\}",

note = "Publisher Copyright: {\textcopyright} 2025 The Authors; Published by the American Association for Cancer Research.",

year = "2025",

month = jun,

day = "1",

doi = "10.1158/2159-8290.CD-24-1421",

language = "English",

volume = "15",

pages = "1159--1179",

journal = "Cancer Discovery",

issn = "2159-8274",

publisher = "American Association for Cancer Research Inc.",

number = "6",

}

Puzio-Kuter, AM, Xu, L, McBrayer, MK, Dominique, R, Li, HH, Fahr, BJ, Brown, AM, Wiebesiek, AE, Russo, BM, Mulligan, CL, Yang, H, Battaglia, J, Robell, KA, Thomas, DH, Huang, KS, Solovyov, A, Greenbaum, BD, Oliner, JD, Davis, TW, Dumble, ML, Johnson, ML, Xiong, S, Yang, P, Lozano, G, Fellous, MM, Vu, BT, Schram, AM, Levine, AJ & Poyurovsky, MV 2025, 'Restoration of the Tumor Suppressor Function of Y220C-Mutant p53 by Rezatapopt, a Small-Molecule Reactivator', Cancer Discovery, vol. 15, no. 6, pp. 1159-1179. https://doi.org/10.1158/2159-8290.CD-24-1421

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T1 - Restoration of the Tumor Suppressor Function of Y220C-Mutant p53 by Rezatapopt, a Small-Molecule Reactivator

AU - Puzio-Kuter, Anna M.

AU - Xu, Lizhong

AU - McBrayer, Mary Kate

AU - Dominique, Romyr

AU - Li, Hongju H.

AU - Fahr, Bruce J.

AU - Brown, Alyssa M.

AU - Wiebesiek, Amy E.

AU - Russo, Brandon M.

AU - Mulligan, Chris L.

AU - Yang, Hong

AU - Battaglia, Josh

AU - Robell, Kimberly A.

AU - Thomas, Dafydd H.

AU - Huang, Kuo Sen

AU - Solovyov, Alexander

AU - Greenbaum, Benjamin D.

AU - Oliner, Jonathan D.

AU - Davis, Thomas W.

AU - Dumble, Melissa L.

AU - Johnson, Melissa L.

AU - Xiong, Shunbin

AU - Yang, Peirong

AU - Lozano, Guillermina

AU - Fellous, Marc M.

AU - Vu, Binh T.

AU - Schram, Alison M.

AU - Levine, Arnold J.

AU - Poyurovsky, Masha V.

PY - 2025/6/1

Y1 - 2025/6/1

N2 - Restoration of the tumor suppressor function of tumor-associated p53 mutants, including the Y220C substitution, has posed a significant challenge for therapeutic discovery. In this study, we describe rezatapopt (PC14586), part of a series of compounds designed to reactivate the p53 Y220C mutant. These compounds restore p53 tumor suppressor function by correcting its conformation and enabling it to bind DNA and activate downstream target genes, thus inducing antiproliferative changes in tumor cells. Our findings are supported by biochemical and structural analysis, in vitro and in vivo transcriptomics, and functional data, revealing the recovery of multiple aspects of the wild-type p53 program. These compounds demonstrate potent antitumor activity in preclinical models as single agents and in combination with immunotherapy. Currently, rezatapopt is being evaluated in a registrational phase II clinical trial for patients with advanced solid tumors harboring the TP53 Y220C mutation.

AB - Restoration of the tumor suppressor function of tumor-associated p53 mutants, including the Y220C substitution, has posed a significant challenge for therapeutic discovery. In this study, we describe rezatapopt (PC14586), part of a series of compounds designed to reactivate the p53 Y220C mutant. These compounds restore p53 tumor suppressor function by correcting its conformation and enabling it to bind DNA and activate downstream target genes, thus inducing antiproliferative changes in tumor cells. Our findings are supported by biochemical and structural analysis, in vitro and in vivo transcriptomics, and functional data, revealing the recovery of multiple aspects of the wild-type p53 program. These compounds demonstrate potent antitumor activity in preclinical models as single agents and in combination with immunotherapy. Currently, rezatapopt is being evaluated in a registrational phase II clinical trial for patients with advanced solid tumors harboring the TP53 Y220C mutation.

UR - https://www.scopus.com/pages/publications/105008355225

U2 - 10.1158/2159-8290.CD-24-1421

DO - 10.1158/2159-8290.CD-24-1421

M3 - Article

C2 - 39945593

AN - SCOPUS:105008355225

SN - 2159-8274

VL - 15

SP - 1159

EP - 1179

JO - Cancer Discovery

JF - Cancer Discovery

IS - 6

ER -

Restoration of the Tumor Suppressor Function of Y220C-Mutant p53 by Rezatapopt, a Small-Molecule Reactivator

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