Warning: Undefined array key "mm" in /www/wwwroot/www.ai-bt.com/si.php on line 10 Deprecated: trim(): Passing null to parameter #1 ($string) of type string is deprecated in /www/wwwroot/www.ai-bt.com/si.php on line 10 Reaction of Zn7metallothionein with cis- and trans-[Pt(N-donor)2Cl2] anticancer complexes: trans-Pt(II) complexes retain their N-donor ligands.

Literature DB >> 17665893

Reaction of Zn7metallothionein with cis- and trans-[Pt(N-donor)2Cl2] anticancer complexes: trans-Pt(II) complexes retain their N-donor ligands.

Markus Knipp¹, Andrei V Karotki, Serge Chesnov, Giovanni Natile, Peter J Sadler, Viktor Brabec, Milan Vasák.

Abstract

Intrinsic and acquired resistance are major drawbacks of platinum-based cancer therapy. The protein superfamily of cysteine- and ZnII-rich proteins, metallothioneins (MT), efficiently inactivate these antitumor drugs because of the strong reactivity of platinum compounds with S-donor molecules. In this study the reactions of human Zn7MT-2 with twelve cis/trans-[Pt(N-donor)2Cl2] compounds and [Pt(dien)Cl]Cl, including new generation drugs, were investigated and the products characterized. A comparison of reaction kinetics revealed that trans-PtII compounds react faster with Zn7MT-2 than cis-PtII compounds. The characterization of the products showed that while all ligands in cis-PtII compounds were replaced by cysteine thiolates, trans-PtII compounds retained their N-donor ligands, thus remaining in a potentially active form. These results provide an increased understanding of the role of MT in the acquired resistance to platinum-based anticancer drugs.

Entities: Chemical Disease Species

Mesh：

Substances：

Year: 2007 PMID： 17665893 DOI： 10.1021/jm070271l

Source DB: PubMed Journal: J Med Chem ISSN： 0022-2623 Impact factor: 7.446

Keyword Cloud
Cited

18 in total

1. Exploring metallodrug-protein interactions by mass spectrometry: comparisons between platinum coordination complexes and an organometallic ruthenium compound.

Authors: Angela Casini; Chiara Gabbiani; Elena Michelucci; Giuseppe Pieraccini; Gloriano Moneti; Paul J Dyson; Luigi Messori
Journal: J Biol Inorg Chem Date: 2009-03-14 Impact factor: 3.358

2. Mass spectrometric strategies to improve the identification of Pt(II)-modification sites on peptides and proteins.

Authors: Huilin Li; Jonathon R Snelling; Mark P Barrow; James H Scrivens; Peter J Sadler; Peter B O'Connor
Journal: J Am Soc Mass Spectrom Date: 2014-05-21 Impact factor: 3.109

3. Use of top-down and bottom-up Fourier transform ion cyclotron resonance mass spectrometry for mapping calmodulin sites modified by platinum anticancer drugs.

Authors: Huilin Li; Tzu-Yung Lin; Steve L Van Orden; Yao Zhao; Mark P Barrow; Ana M Pizarro; Yulin Qi; Peter J Sadler; Peter B O'Connor
Journal: Anal Chem Date: 2011-11-18 Impact factor: 6.986

4. Reactivity of platinum-based antitumor drugs towards a Met- and His-rich 20mer peptide corresponding to the N-terminal domain of human copper transporter 1.

Authors: Zhengyi Wu; Qin Liu; Xiao Liang; Xiaoliang Yang; Ningyan Wang; Xinghao Wang; Hongzhe Sun; Yi Lu; Zijian Guo
Journal: J Biol Inorg Chem Date: 2009-08-08 Impact factor: 3.358

5. Proteins as possible targets for cytotoxic trans-platinum(II) complexes with aliphatic amine ligands: Further exceptions to the DNA paradigm.

Authors: Leticia Cubo; Michael Groessl; Paul J Dyson; Adoración G Quiroga; Carmen Navarro-Ranninger; Angela Casini
Journal: ChemMedChem Date: 2010-08-02 Impact factor: 3.466

Reaction of Zn7metallothionein with cis- and trans-[Pt(N-donor)2Cl2] anticancer complexes: trans-Pt(II) complexes retain their N-donor ligands.

1. Exploring metallodrug-protein interactions by mass spectrometry: comparisons between platinum coordination complexes and an organometallic ruthenium compound.

2. Mass spectrometric strategies to improve the identification of Pt(II)-modification sites on peptides and proteins.

3. Use of top-down and bottom-up Fourier transform ion cyclotron resonance mass spectrometry for mapping calmodulin sites modified by platinum anticancer drugs.

4. Reactivity of platinum-based antitumor drugs towards a Met- and His-rich 20mer peptide corresponding to the N-terminal domain of human copper transporter 1.

5. Proteins as possible targets for cytotoxic trans-platinum(II) complexes with aliphatic amine ligands: Further exceptions to the DNA paradigm.

6. Trans labilization of am(m)ine ligands from platinum(II) complexes by cancer cell extracts.

7. Zeptomole electrochemical detection of metallothioneins.

8. Peculiar mechanistic and structural features of the carboplatin-cytochrome c system revealed by ESI-MS analysis.

9. Reaction of human metallothionein-3 with cisplatin and transplatin.

10. Crystal structures of cisplatin bound to a human copper chaperone.