Relation of Metal-Binding Property and Selective Toxicity of 8-Hydroxyquinoline Derived Mannich Bases Targeting Multidrug Resistant Cancer Cells

Author:

Pape Veronika F.S.ORCID,Gaál Anikó,Szatmári IstvánORCID,Kucsma Nóra,Szoboszlai Norbert,Streli Christina,Fülöp FerencORCID,Enyedy Éva A.ORCID,Szakács Gergely

Abstract

Resistance to chemotherapeutic agents is a major obstacle in cancer treatment. A recently proposed strategy is to target the collateral sensitivity of multidrug resistant (MDR) cancer. Paradoxically, the toxicity of certain metal chelating agents is increased, rather than decreased, by the function of P-glycoprotein (Pgp), which is known to confer resistance by effluxing chemotherapeutic compounds from cancer cells. We have recently characterized and compared the solution’s chemical properties including ligand protonation and the metal binding properties of a set of structurally related 8-hydroxyquinoline derived Mannich bases. Here we characterize the impact of the solution stability and redox activity of their iron(III) and copper(II) complexes on MDR-selective toxicity. Our results show that the MDR-selective anticancer activity of the studied 8-hydroxyquinoline derived Mannich bases is associated with the iron deprivation of MDR cells and the preferential formation of redox-active copper(II) complexes, which undergo intracellular redox-cycling to induce oxidative stress.

Funder

Magyar Tudományos Akadémia

European Research Council

Nemzeti Kutatási és Technológiai Hivatal

Nemzeti Kutatási Fejlesztési és Innovációs Hivatal

Publisher

MDPI AG

Subject

Cancer Research,Oncology

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