Impact of copper and iron binding properties on the anticancer activity of 8-hydroxyquinoline derived Mannich bases.

Authors

Veronika F.S. Pape, Hungarian Academy of Sciences; Semmelweis University
Nóra V. May, Hungarian Academy of Sciences
G. Tamás Gál, Hungarian Academy of Sciences
István Szatmári, University of Szeged
Flóra Szeri, Thomas Jefferson University; Hungarian Academy of SciencesFollow
Ferenc Fülöp, University of Szeged
Gergely Szakács, Hungarian Academy of Sciences; Medical University of Vienna
Éva A. Enyedy, University of Szeged

Document Type

Article

Publication Date

12-4-2018

Comments

This article has been peer reviewed. It is the author’s final published version in Dalton Transactions, Volume 47, Issue 47, December 2018, Pages 17032-17045.

The published version is available at https://doi.org/10.1039/c8dt03088j. Copyright © Pape et al.

Abstract

The anticancer activity of 8-hydroxyquinolines relies on complex formation with redox active copper and iron ions. Here we employ UV-visible spectrophotometry and EPR spectroscopy to compare proton dissociation and complex formation processes of the reference compound 8-hydroxyquinoline (Q-1) and three related Mannich bases to reveal possible correlations with biological activity. The studied derivatives harbor a CH2-N moiety at position 7 linked to morpholine (Q-2), piperidine (Q-3), and chlorine and fluorobenzylamino (Q-4) substituents. Solid phase structures of Q-3, Q-4·HCl·H2O, [(Cu(HQ-2)2)2]·(CH3OH)2·Cl4·(H2O)2, [Cu(Q-3)2]·Cl2 and [Cu(HQ-4)2(CH3OH)]·ZnCl4·CH3OH were characterized by single-crystal X-ray diffraction analysis. In addition, the redox properties of the copper and iron complexes were studied by cyclic voltammetry, and the direct reaction with physiologically relevant reductants (glutathione and ascorbic acid) was monitored. In vitro cytotoxicity studies conducted with the human uterine sarcoma MES-SA/Dx5 cell line reveal the significant cytotoxicity of Q-2, Q-3, and Q-4 in the sub- to low micromolar range (IC50 values 0.2-3.3 μM). Correlation analysis of the anticancer activity and the metal binding properties of the compound series indicates that, at physiological pH, weaker copper(ii) and iron(iii) binding results in elevated toxicity (e.g.Q4: pCu = 13.0, pFe = 6.8, IC50 = 0.2 μM vs.Q1: pCu = 15.1, pFe = 13.0 IC50 = 2.5 μM). Although the studied 8-hydroxyquinolines preferentially bind copper(ii) over iron(iii), the cyclic voltammetry data revealed that the more cytotoxic ligands preferentially stabilize the lower oxidation state of the metal ions. A linear relationship between the pKa (OH) and IC50 values of the studied 8-hydroxyquinolines was found. In summary, we identify Q-4 as a potent and selective anticancer candidate with significant toxicity in drug resistant cells.

Recommended Citation

Pape, Veronika F.S.; May, Nóra V.; Gál, G. Tamás; Szatmári, István; Szeri, Flóra; Fülöp, Ferenc; Szakács, Gergely; and Enyedy, Éva A., "Impact of copper and iron binding properties on the anticancer activity of 8-hydroxyquinoline derived Mannich bases." (2018). Department of Dermatology and Cutaneous Biology Faculty Papers. Paper 106.
https://jdc.jefferson.edu/dcbfp/106

Creative Commons License

This work is licensed under a Creative Commons Attribution-Noncommercial 3.0 License

PubMed ID

30460942

Language

English