Comparative solution equilibrium studies of antitumor ruthenium(η 6 -p-cymene) and rhodium(η 5 -C 5 Me 5 ) complexes of 8-hydroxyquinolines

Comparative solution equilibrium studies of antitumor ruthenium(η 6 -p-cymene) and rhodium(η 5 -C 5 Me 5 ) complexes of 8-hydroxyquinolines

Complex formation processes of [Ru(η -p-cymene)(H O) ] and [Rh(η -C Me )(H O) ] organometallic cations with 8-hydroxyquinoline (HQ) ligands were studied in aqueous solution by the combined use of H NMR spectroscopy, UV-visible spectrophotometry and pH-potentiometry. Solution stability, chloride ion...

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Veröffentlicht in:Dalton transactions : an international journal of inorganic chemistry 2017-03, Vol.46 (13), p.4382-4396
Hauptverfasser: Dömötör, Orsolya, Pape, Veronika F S, May, Nóra V, Szakács, Gergely, Enyedy, Éva A
Format: Artikel
Sprache:eng
Schlagworte:
Antineoplastic Agents - chemical synthesis
Antineoplastic Agents - chemistry
Antineoplastic Agents - pharmacology
Biotechnology
Cancer
Cell Line, Tumor
Cell Survival - drug effects
Chlorides - chemistry
Coordination Complexes - chemical synthesis
Coordination Complexes - chemistry
Coordination Complexes - pharmacology
Cyclopentanes - chemistry
Drug Discovery
Formations
Humans
Ligands
Mathematical models
Metalorganic compounds
Monoterpenes - chemistry
Organometallic Compounds
Oxyquinoline - chemistry
Piperidines - chemistry
Rhodium - chemistry
Ruthenium - chemistry
Stability
Sulfonic Acids - chemistry
Toxicity
Water - chemistry
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Zusammenfassung:Complex formation processes of [Ru(η -p-cymene)(H O) ] and [Rh(η -C Me )(H O) ] organometallic cations with 8-hydroxyquinoline (HQ) ligands were studied in aqueous solution by the combined use of H NMR spectroscopy, UV-visible spectrophotometry and pH-potentiometry. Solution stability, chloride ion affinity and lipophilicity of the complexes were characterized together with the in vitro cytotoxicity against a pair of cancer cell lines, responsive and resistant to classic chemotherapy. The solid phase structure of the [Rh(η -C Me )(8-quinolinolato)(Cl)] complex was characterized by single-crystal X-ray diffraction analysis. In addition to the unsubstituted HQ its 7-(1-piperidinylmethyl) (PHQ) and 5-sulfonate (HQS) derivatives were involved. PHQ has a significant preference for targeting multidrug resistant cancer cell lines, while HQS served as a water soluble model compound. The equilibrium studies revealed the formation of mono[M(L)(H O)] complexes with prominently high solution stability, which predominate at physiological pH even in the micromolar concentration range, and the formation of mixed hydroxido [M(L)(OH)] complexes was characterized by relatively high pK values (8.5-10.3). In comparison to the Rh(η -C Me ) species the complexation process with Ru(η -p-cymene) is much slower, and both the pK values and the H O/Cl co-ligand exchange constants are lower by 1-1.5 orders of magnitude. The stability order obtained for these organometallic complexes is as follows: HQS > HQ > PHQ. The cytotoxicity of the ligands and their Ru(η -p-cymene) and Rh(η -C Me ) complexes was investigated against MES-SA (human uterine sarcoma) cell line and its multidrug resistant counterpart (MES-SA/Dx5). HQ and its complexes show similar cytotoxicity in both cell lines. In contrast, PHQ and its Rh(η -C Me ) complex are more potent against MES-SA/Dx5 cells, while this selectivity could not be observed for the Ru(η -p-cymene) complex.
ISSN:1477-9226
1477-9234
DOI:10.1039/c7dt00439g