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Literature DB >> 31196889

Combinatorial Therapy of Zinc Metallochaperones with Mutant p53 Reactivation and Diminished Copper Binding.

Saif Zaman¹, Xin Yu^2,3, Anthony F Bencivenga⁴, Adam R Blanden⁵, Yue Liu^2,3, Tracy Withers^2,3, Bing Na^2,3, Alan J Blayney⁵, John Gilleran⁴, David A Boothman^6,7, Stewart N Loh⁵, S David Kimball^4,8,9, Darren R Carpizo^10,3,9.

Abstract

Chemotherapy and radiation are more effective in wild-type (WT) p53 tumors due to p53 activation. This is one rationale for developing drugs that reactivate mutant p53 to synergize with chemotherapy and radiation. Zinc metallochaperones (ZMC) are a new class of mutant p53 reactivators that restore WT structure and function to zinc-deficient p53 mutants. We hypothesized that the thiosemicarbazone, ZMC1, would synergize with chemotherapy and radiation. Surprisingly, this was not found. We explored the mechanism of this and found the reactive oxygen species (ROS) activity of ZMC1 negates the signal on p53 that is generated with chemotherapy and radiation. We hypothesized that a zinc scaffold generating less ROS would synergize with chemotherapy and radiation. The ROS effect of ZMC1 is generated by its chelation of redox active copper. ZMC1 copper binding (K Cu) studies reveal its affinity for copper is approximately 108 greater than Zn2+ We identified an alternative zinc scaffold (nitrilotriacetic acid) and synthesized derivatives to improve cell permeability. These compounds bind zinc in the same range as ZMC1 but bound copper much less avidly (106- to 107-fold lower) and induced less ROS. These compounds were synergistic with chemotherapy and radiation by inducing p53 signaling events on mutant p53. We explored other combinations with ZMC1 based on its mechanism of action and demonstrate that ZMC1 is synergistic with MDM2 antagonists, BCL2 antagonists, and molecules that deplete cellular reducing agents. We have identified an optimal Cu2+:Zn2+ binding ratio to facilitate development of ZMCs as chemotherapy and radiation sensitizers. Although ZMC1 is not synergistic with chemotherapy and radiation, it is synergistic with a number of other targeted agents. ©2019 American Association for Cancer Research.

Entities: CellLine Chemical Disease Gene Mutation Species

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Year: 2019 PMID： 31196889 PMCID： PMC6677634 DOI： 10.1158/1535-7163.MCT-18-1080

Source DB: PubMed Journal: Mol Cancer Ther ISSN： 1535-7163 Impact factor: 6.261

31 in total

1. Zinc supplementation augments in vivo antitumor effect of chemotherapy by restoring p53 function.

Authors: Ofer Margalit; Amos J Simon; Eduard Yakubov; Rosa Puca; Ady Yosepovich; Camila Avivi; Jasmine Jacob-Hirsch; Ilana Gelernter; Alon Harmelin; Iris Barshack; Gideon Rechavi; Gabriella D'Orazi; David Givol; Ninette Amariglio
Journal: Int J Cancer Date: 2011-11-30 Impact factor: 7.396

Review 2. Regulation of p53 in response to DNA damage.

Authors: N D Lakin; S P Jackson
Journal: Oncogene Date: 1999-12-13 Impact factor: 9.867

3. PRIMA-1(MET) synergizes with cisplatin to induce tumor cell apoptosis.

Authors: Vladimir J N Bykov; Nicole Zache; Helene Stridh; Jacob Westman; Jan Bergman; Galina Selivanova; Klas G Wiman
Journal: Oncogene Date: 2005-05-12 Impact factor: 9.867

4. MDM2 inhibition sensitizes neuroblastoma to chemotherapy-induced apoptotic cell death.

Authors: Eveline Barbieri; Parth Mehta; Zaowen Chen; Linna Zhang; Andrew Slack; Stacey Berg; Jason M Shohet
Journal: Mol Cancer Ther Date: 2006-09 Impact factor: 6.261

5. Zinc Metallochaperones Reactivate Mutant p53 Using an ON/OFF Switch Mechanism: A New Paradigm in Cancer Therapeutics.

Authors: Xin Yu; Samuel Kogan; Ying Chen; Ashley T Tsang; Tracy Withers; Hongxia Lin; John Gilleran; Brian Buckley; Dirk Moore; Joseph Bertino; Chang Chan; S David Kimball; Stewart N Loh; Darren R Carpizo
Journal: Clin Cancer Res Date: 2018-06-18 Impact factor: 12.531

6. Thiosemicarbazones Functioning as Zinc Metallochaperones to Reactivate Mutant p53.

Authors: Xin Yu; Adam Blanden; Ashley T Tsang; Saif Zaman; Yue Liu; John Gilleran; Anthony F Bencivenga; S David Kimball; Stewart N Loh; Darren R Carpizo
Journal: Mol Pharmacol Date: 2017-03-20 Impact factor: 4.436

7. Molar absorption coefficients and stability constants of Zincon metal complexes for determination of metal ions and bioinorganic applications.

Authors: Anna Kocyła; Adam Pomorski; Artur Krężel
Journal: J Inorg Biochem Date: 2017-08-24 Impact factor: 4.155

8. p53 status and the efficacy of cancer therapy in vivo.

Authors: S W Lowe; S Bodis; A McClatchey; L Remington; H E Ruley; D E Fisher; D E Housman; T Jacks
Journal: Science Date: 1994-11-04 Impact factor: 47.728

9. Small molecule restoration of wildtype structure and function of mutant p53 using a novel zinc-metallochaperone based mechanism.

Authors: Xin Yu; Adam R Blanden; Sumana Narayanan; Lalithapriya Jayakumar; David Lubin; David Augeri; S David Kimball; Stewart N Loh; Darren R Carpizo
Journal: Oncotarget Date: 2014-10-15

6. Zinc shapes the folding landscape of p53 and establishes a pathway for reactivating structurally diverse cancer mutants.

Authors: Adam R Blanden; Xin Yu; Darren R Carpizo; Stewart N Loh; Alan J Blayney; Christopher Demas; Jeung-Hoi Ha; Yue Liu; Tracy Withers
Journal: Elife Date: 2020-12-02 Impact factor: 8.713

6 in total

Combinatorial Therapy of Zinc Metallochaperones with Mutant p53 Reactivation and Diminished Copper Binding.

1. Zinc supplementation augments in vivo antitumor effect of chemotherapy by restoring p53 function.

Review 2. Regulation of p53 in response to DNA damage.

3. PRIMA-1(MET) synergizes with cisplatin to induce tumor cell apoptosis.

4. MDM2 inhibition sensitizes neuroblastoma to chemotherapy-induced apoptotic cell death.

5. Zinc Metallochaperones Reactivate Mutant p53 Using an ON/OFF Switch Mechanism: A New Paradigm in Cancer Therapeutics.

6. Thiosemicarbazones Functioning as Zinc Metallochaperones to Reactivate Mutant p53.

7. Molar absorption coefficients and stability constants of Zincon metal complexes for determination of metal ions and bioinorganic applications.

8. p53 status and the efficacy of cancer therapy in vivo.

9. Small molecule restoration of wildtype structure and function of mutant p53 using a novel zinc-metallochaperone based mechanism.

10. Serine starvation induces stress and p53-dependent metabolic remodelling in cancer cells.

Review 1. A role for bioinorganic chemistry in the reactivation of mutant p53 in cancer.

2. Benzothiazolyl and Benzoxazolyl Hydrazones Function as Zinc Metallochaperones to Reactivate Mutant p53.

Review 3. Follow the Mutations: Toward Class-Specific, Small-Molecule Reactivation of p53.

4. Bifunctional ligand design for modulating mutant p53 aggregation in cancer.

Review 5. p53 and Zinc: A Malleable Relationship.

6. Zinc shapes the folding landscape of p53 and establishes a pathway for reactivating structurally diverse cancer mutants.