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Abstract
The rhenium(I) complex fac -[Re(CO) 3 (2,9-dimethyl-1,10-phenanthroline)(OH 2 )]
+ ( 1 ) was previously shown to exhibit potent
in vitro anticancer
activity in a manner distinct from conventional platinum-based drugs
( J. Am. Chem. Soc. 2017 , 139 , 14302–14314). In this study, we report further efforts
to
explore its aqueous speciation and antitumor activity. The cellular
uptake of 1 was measured in A2780 and cisplatin-resistant
A2780CP70 ovarian cancer cells by inductively coupled plasma mass
spectrometry, revealing similar uptake efficiency in both cell lines.
High accumulation in the mitochondria was observed, contradicting
prior fluorescence microscopy studies. The luminescence of 1 is highly dependent
on pH and coordination environment, making fluorescence
microscopy somewhat unreliable for determining compound localization.
The in vivo anticancer activity of 1 was evaluated in
mice bearing patient-derived ovarian cancer tumor xenografts. These
studies conclusively show that 1 is capable of inhibiting
tumor growth, providing further credibility for the use of these compounds
as anticancer agents.