Is antitumor Pt(IV) complex containing two axial lonidamine ligands a true dual- or multi-action prodrug?

Author:

Kasparkova Jana1ORCID,Kostrhunova Hana1,Novohradsky Vojtech1,Ma Lili2,Zhu Guangyu2,Milaeva Elena R3,Shtill Alexender A4,Vinck Robin5,Gasser Gilles5,Brabec Viktor1ORCID,Nazarov Alexey A3ORCID

Affiliation:

1. Czech Academy of Sciences, Institute of Biophysics , Brno CZ-61265, Czech Republic

2. Department of Chemistry, City University of Hong Kong , Hong Kong SAR, P. R. China

3. Faculty of Chemistry, Lomonosov Moscow State University , 119991 Moscow, Russian Federation

4. Blokhin Cancer Center, Russian Academy of Medical Sciences , 115478 Moscow, Russian Federation

5. Chimie ParisTech, PSL University, CNRS, Institute of Chemistry for Life and Health Sciences , 75005 Paris, France

Abstract

Abstract This work studied the mechanism of action of a Pt(IV) complex 2 bearing two axial lonidamine ligands, which are selective inhibitors of aerobic glycolysis. The presence of two lonidamine ligands in 2 compared to the parent Pt(II) complex increased its antiproliferative activity, cellular accumulation, and changed its cell cycle profile and mechanism of cell death. In 3D cell culture, 2 showed exceptional antiproliferative activity with IC50 values as low as 1.6 μM in MCF7 cells. The study on the influence of the lonidamine ligands in the Pt complex on glycolysis showed only low potency of ligands to affect metabolic processes in cancer cells, making the investigated complex, not a dual- or multi-action prodrug. However, the Pt(IV) prodrug effectively delivers the cytotoxic Pt(II) complex into cancer cells.

Funder

Grantová Agentura České Republiky

Russian Foundation for Basic Research

European Research Council

Publisher

Oxford University Press (OUP)

Subject

Metals and Alloys,Biochemistry,Biomaterials,Biophysics,Chemistry (miscellaneous)

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