Functionalization of Ruthenium(II)(η6 -p-cymene)(3-hydroxy-2-pyridone) Complexes with (Thio)Morpholine: Synthesis and Bioanalytical Studies.
Muhammad HanifSamuel M MeierZenita AdhireksanHelena HenkeSanela MarticSanam MovassaghiMahmoud LabibWolfgang KandiollerStephen M F JamiesonMichaela HejlMichael A JakupecHeinz-Bernhard KraatzCurt A DaveyBernhard K KepplerChristian G HartingerPublished in: ChemPlusChem (2017)
Hydroxypyr(id)ones constitute an emerging platform for the design of drug molecules, owing to their favorable biocompatibility and toxicity profiles. Herein, [RuII (η6 -p-cymene)] complexes with 3-hydroxy-2-pyridinone functionalized with morpholine and thiomorpholine, as a means often used in medicinal chemistry to alter the physicochemical properties of drug compounds, are reported. The compounds underwent hydrolysis of the Ru-Cl bond and the aqua species were stable for up to 48 h in aqueous solution, as observed by 1 H NMR spectroscopy and ESI-MS. The compounds formed adducts with amino acids and proteins through cleavage of the pyridinone ligand. Binding experiments to the nucleosome core particle by means of X-ray crystallography revealed similar reactivity and exclusive binding to histidine moieties of the histone proteins. Preliminary cyclin-dependent kinase 2 (CDK2)/cyclin A kinase inhibitory studies revealed promising activity similar to that of structurally related organometallic compounds.
Keyphrases
- cell cycle
- ms ms
- aqueous solution
- single cell
- dna methylation
- amino acid
- multiple sclerosis
- protein kinase
- tyrosine kinase
- high throughput
- oxidative stress
- emergency department
- high resolution
- drug induced
- gene expression
- magnetic resonance imaging
- quantum dots
- adverse drug
- cell death
- computed tomography
- transcription factor
- electronic health record
- dual energy
- electron microscopy