Issue 10, 2019

Kinetic analysis of the accumulation of a half-sandwich organo-osmium pro-drug in cancer cells

Abstract

The organo-osmium half-sandwich complex [(η6-p-cymene)Os(Ph-azopyridine-NMe2)I]+ (FY26) exhibits potent antiproliferative activity towards cancer cells and is active in vivo. The complex is relatively inert, but rapidly activated in cells by displacement of coordinated iodide. Here, we study time-dependent accumulation of FY26 in A2780 human ovarian cancer cells at various temperatures in comparison with the chlorido metabolite [(η6-p-cymene)Os(Ph-azopyridine-NMe2)Cl]+ (FY25). Mathematical models described the time evolution of FY26 and FY25 intracellular and extracellular concentrations taking into account both cellular transport (influx and efflux) and the intracellular conversion of FY26 to FY25. Uptake of iodide complex FY26 at 37 °C was 17× faster than that of chloride complex FY25, and efflux 1.4× faster. Osmium accumulation decreased markedly after 24 h of exposure. Modelling revealed that this phenomenon could be explained by complex-induced reduction of osmium uptake, rather than by a model involving enhanced osmium efflux. The intracellular osmium concentration threshold above which reduction in drug uptake was triggered was estimated as 20.8 μM (95% confidence interval [16.5, 30]). These studies provide important new insight into the dynamics of transport of this organometallic anticancer drug candidate.

Graphical abstract: Kinetic analysis of the accumulation of a half-sandwich organo-osmium pro-drug in cancer cells

Supplementary files

Article information

Article type
Paper
Submitted
04 ⵢⵓⵍ 2019
Accepted
23 ⵢⵓⵍ 2019
First published
17 ⵛⵓⵜ 2019
This article is Open Access
Creative Commons BY license

Metallomics, 2019,11, 1648-1656

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