Heterometallic bridged Pt(II)‐Zn(II) complexes: Influence of the substituent in 4′‐position in inert terpy ligand on antigenotoxicity, potential antitumor activity and mechanism of interactions of the complexes with biomolecules

Author:

Serezlić Majda Kolenović1ORCID,Hasić Rušid1ORCID,Ašanin Darko2ORCID,Šmit Biljana2ORCID,Matić Sanja Lj.2ORCID,Serafinović Marina Ćendić3ORCID,Nikodijević Danijela3ORCID,Jovankić Jovana3ORCID,Grgurić‐Šipka Sanja4,Soldatović Tanja V.1ORCID

Affiliation:

1. Department of Natural‐Mathematical Sciences State University of Novi Pazar Novi Pazar Serbia

2. Institute for Information Technologies University of Kragujevac Kragujevac Serbia

3. Faculty of Science University of Kragujevac Kragujevac Serbia

4. Faculty of Chemistry University of Belgrade Belgrade Serbia

Abstract

The synthesis and characterization of novel hetrometallic complexes [{cis‐PtCl(NH3)2(μ‐4,4′‐bipyridyl)ZnCl(terpy‐Cl)}](ClO4)2 (C1a), [{trans‐PtCl(NH3)2(μ‐4,4′‐bipyridyl)ZnCl(terpy)}](ClO4)2 (C2a), [{cis‐PtCl(NH3)2(μ‐pyrazine)ZnCl(terpy‐Cl)}](ClO4)2 (C3a) and [{trans‐PtCl(NH3)2(μ‐pyrazine)ZnCl(terpy‐Cl)}](ClO4)2 (C4a) (where terpy‐Cl = 4′‐chloro‐2,2′:6′,2′′‐terpyridine) was done. Acid–base titrations were performed by UV–Vis spectrophotometric method to evaluate the pKa values of corresponding aqua complexes. Interactions between complexes and important biomolecules, guanosine‐5′‐monophosphate (5′‐GMP) and glutathione (GSH) were examined by 1H NMR spectroscopy. The chloride substituent at the 4′ position on the middle pyridine ring of terpyridine ligand significantly affects the coordination of biomolecules, as well as overall stability of complexes. The complexes were evaluated in vitro for the antioxidant prevention of DNA damages. All tested novel complexes demonstrated a significant reduction in DNA damage against oxidative modifications of DNA caused by the hydroxyl and peroxyl radicals. Also, cytotoxicity evaluation showed that significant cytotoxicity occurs only after long‐term effect of C1a, C2a and C3a, complexes in HCT‐116 cells. Molecular docking studies predict results in agreement with experimental research.

Publisher

Wiley

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