1. Synthesis and X-ray crystal structure of [Ag(phendio)2]ClO4 (phendio = 1,10-phenanthroline-5,6-dione) and its effects on fungal and mammalian cells
- Author
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Michael Devereux, Malachy McCann, Kevin Kavanagh, Paul McCormack, Barry Coyle, Martin Clynes, Paula Kinsella, Robert O'Connor, Vickie McKee, and Sinead McKay
- Subjects
Cell division ,Protein Conformation ,Phenanthroline ,Antineoplastic Agents ,Crystal structure ,Crystallography, X-Ray ,Cell morphology ,General Biochemistry, Genetics and Molecular Biology ,Fungal Proteins ,Biomaterials ,Metal ,chemistry.chemical_compound ,Cell Line, Tumor ,Candida albicans ,Animals ,Humans ,DNA, Fungal ,Cytokinesis ,Perchlorates ,biology ,X-Rays ,Metals and Alloys ,biology.organism_classification ,Microscopy, Electron ,Crystallography ,Models, Chemical ,chemistry ,Metals ,visual_art ,Yield (chemistry) ,visual_art.visual_art_medium ,General Agricultural and Biological Sciences ,Copper ,DNA ,Phenanthrolines - Abstract
The Cu(II) and Ag(I) complexes, [Cu(phendio)3](ClO4)2 x 4H2O and [Ag(phendio)2]ClO4 (phendio = 1,10-phenanthroline-5,6-dione), are prepared in good yield by reacting phendio with the appropriate metal perchlorate salt. The X-ray crystal structure of the Ag(I) complex shows it to have a pseudo tetrahedral structure. 'Metal-free' phendio and the Cu(II) and Ag(I) phendio complexes strongly inhibit the growth of the fungal pathogen Candida albicans, and are more active than their 1,10-phenanthroline analogues. The simple Ag(I) salts, AgCH3CO2, AgNO3 and AgClO4 x H2O display superior anti-fungal properties compared to analogous simple Cu(II) and Mn(II) salts, suggesting that the nature of the metal ion strongly influences activity. Exposing C. albicans to 'metal-free' phendio, simple Ag(I) salts and [Ag(phendio)2]ClO4 causes extensive, non-specific DNA cleavage. 'Metal-free' phendio and [Ag(phendio)2]ClO4 induce gross distortions in fungal cell morphology and there is evidence for disruption of cell division. Both drugs also exhibit high anti-cancer activity when tested against cultured mammalian cells.
- Published
- 2004
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