Please use this identifier to cite or link to this item: https://hdl.handle.net/2440/4777
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dc.contributor.authorSmith, Katharine A.en
dc.contributor.authorDeacon, Glen B.en
dc.contributor.authorJackson, W. Royen
dc.contributor.authorTiekink, Edward Richard Tomen
dc.contributor.authorRainone, Silvinaen
dc.contributor.authorWebster, Lorraine K.en
dc.date.issued1998en
dc.identifier.citationMetal-Based Drugs. 5(5):295-304en
dc.identifier.issn0793-0291en
dc.identifier.urihttp://hdl.handle.net/2440/4777-
dc.description.abstractNew arylbismuth(lll) oxinates, PhBi(MeOx)₂, (p-MeC₆H₄)Bi(Ox)₂, (p-MeC₆H₄)Bi(MeOx)₂, (p-ClC₆H4)Bi(Ox)₂, and (p-ClC₆H₄)Bi(MeOx)₂ (Ox− = quinolin-8-olate and MeOx−=2-methylquinolin-8-olate) have been prepared by reaction of the appropriate diarylbismuth chlorides with Na(Ox) or Na(MeOx) in the presence of 15-crown-5. An X-ray crystallographic study has shown PhBi(MeOx)₂ to be a five coordinate monomer with distorted square pyramidal stereochemistry. Chelating MeOx ligands have a cisoid arrangement in the square plane and the phenyl group is apical. The lattice is stabilised by significant π-π interactions between centrosymmetric molecules. A range of these complexes has been shown to have high in vitro biological activity (comparable with or better than cisplatin) against L1210 leukaemia, the corresponding cisplatin resistant line, and a human ovarian cell line, SKOV-3. However, initial in vivo testing against a solid mouse plasmacytoma (PC6) and P388 leukaemia has not revealed significant activity.en
dc.description.statementofresponsibilityKatharine A. Smith, Glen B. Deacon, W. Roy Jackson, Edward R. T. Tiekink, Silvina Rainone, and Lorraine K. Websteren
dc.language.isoenen
dc.titlePreparation and anti-tumour activity of some arylbismuth(III) oxine complexesen
dc.typeJournal articleen
dc.contributor.schoolSchool of Chemistry and Physicsen
dc.identifier.doi10.1155/MBD.1998.295en
Appears in Collections:Chemistry publications

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