1000174-41-3Relevant academic research and scientific papers
Tuning the hydrophobicity of ruthenium(II)-arene (RAPTA) drugs to modify uptake, biomolecular interactions and efficacy
Scolaro, Claudine,Chaplin, Adrian B.,Hartinger, Christian G.,Bergamo, Alberta,Cocchietto, Moreno,Keppler, Bernhard K.,Sava, Gianni,Dyson, Paul J.
, p. 5065 - 5072 (2008/03/13)
The antitumour activity of the organometallic ruthenium(ii)-arene mixed phosphine complexes, [Ru(η6-p-cymene)Cl(PTA)(PPh 3)]BF4 1b and [Ru(η6-C6H 5CH2CH2OH)Cl(PTA)(PPh3)]BF 4 2b (PTA = 1,3,5-triaza-7-phosphaadamantane), have been evaluated in vitro and compared to their RAPTA analogues, [Ru(η6-p-cymene) Cl2(PTA)] 1a and [Ru(η6-C6H 5CH2CH2OH)Cl2(PTA)] 2a. The results show that the addition of the PPh3 ligand to 2a increases the cytotoxicity towards the TS/A adenocarcinoma cancer cells, which correlates with increased uptake, but also increases cytotoxicity to non-tumourigenic HBL-100 cells, thus decreasing selectivity. The decrease in selectivity has been correlated to increased DNA interactions relative to proteins, demonstrated by reactivity of the compounds with a 14-mer oligonucleotide and the model proteins ubiquitin and cytochrome-c. This journal is The Royal Society of Chemistry.
