| Article ID | Journal | Published Year | Pages | File Type |
|---|---|---|---|---|
| 1317049 | Journal of Inorganic Biochemistry | 2011 | 10 Pages |
Bisphosphonates (BPs), the synthetic analogues of pyrophosphate, are widely used in the treatment of metabolic bone diseases. BPs exhibit a preferential accumulation in malignant pleural mesothelioma (MPM) and, furthermore, nitrogen-containing BPs (n-BPs) show significant inhibition of MPM cell proliferation. We synthesised dinuclear platinum(II) complexes containing a n-BP moiety as bridging ligand and am(m)ines as terminal ligands (Pt–n-BP)s, with the aim of obtaining bifunctional mesothelioma-targeted drugs. We compared the antiproliferative effect of the single drugs (i.e. Pt-model and n-BPs) with that of the preformed Pt–n-BP complexes by means of the combination index (CI) in order to assess the synergistic/additive/antagonistic effect of the two constituents in the resulting conjugates. The combination of the two individual drugs was almost additive, while the preformed Pt–n-BP produced an antagonistic effect. Furthermore, (Pt–n-BP)s neither inhibited the mevalonate pathway (as n-BPs normally do) nor increased the Pt uptake. The minimal biological results of these conjugates could be traced back to a slow and inappropriate hydrolysis, that does not split the adduct into active components.
Graphical AbstractWe synthesised platinum(II) complexes containing a n-bisphosphonate (BP) moiety (Pt-n-BP) as bifunctional mesothelioma-targeted drugs.Figure optionsDownload full-size imageDownload as PowerPoint slide
