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Targeting G-quadruplex structures with Zn(<scp>ii</scp>) terpyridine derivatives: a SAR study

Authors :
Sonia Montanaro
Borja Díaz de Greñu
Natalia Busto
Tarita Biver
Begoña García
Blanca R. Manzano
Félix A. Jalón
M. Carmen Carrión
Source :
Dalton Transactions. 49:13372-13385
Publication Year :
2020
Publisher :
Royal Society of Chemistry (RSC), 2020.

Abstract

Based on the ability of terpyridines to react with G-quadruplex DNA (G4) structures along with the interest aroused by Zn as an essential metal centre in many biological processes, we have synthesized and characterized six Zn chloride or nitrate complexes containing terpyridine ligands with different 4&#39;-substituents. In addition, we have studied their interaction with G4 and their cytotoxicity. Our experimental results revealed that the leaving group exerts a strong influence on the cytotoxicity, since the complexes bearing chloride were more cytotoxic than their nitrate analogues and an effect of the terpyridine ligand was also observed. The thermal stabilization profiles showed that the greatest stabilization of hybrid G4, Tel22, was observed for the Zn complexes bearing the terpyridine ligand that contained one or two methylated 4-(imidazol-1-yl)phenyl substituents, 3Cl and 3(L)2, respectively, probably due to their extra positive charge. Stability and aquation studies for these complexes were carried out and no ligand release was detected. Complexes 3Cl and 3(L)2 were successfully internalized by SW480 cells and they seemed to be localized mainly in the nucleolus. The highest cytotoxicity, G4 selectivity and G4 affinity determined by fluorescence and ITC experiments, and subcellular localization quantified by ICP-MS measurements, rendered 3Cl a very interesting complex from a biological standpoint.

Details

ISSN :
14779234 and 14779226
Volume :
49
Database :
OpenAIRE
Journal :
Dalton Transactions
Accession number :
edsair.doi.dedup.....b8dcc24ae54c065e7c674885bc0b743e
Full Text :
https://doi.org/10.1039/d0dt02125c