| Article ID | Journal | Published Year | Pages | File Type |
|---|---|---|---|---|
| 1317299 | Journal of Inorganic Biochemistry | 2014 | 8 Pages |
We report new anticancer prodrugs, platinum(IV) derivatives of oxaliplatin conjugated with valproic acid (VPA), a well-known drug having histone deacetylase inhibitory activity. Like most platinum(IV) derivatives, the cytotoxicity of the conjugates was lower in cell culture than that of oxaliplatin, but greater than those of its Pt(IV) derivative containing biologically inactive axial ligands in several cancer cell lines. Notably, these conjugates display activity in both cisplatin sensitive- and resistant tumor cells capable of both markedly enhanced accumulation in tumor cells and acting in a dual threat manner, concurrently targeting histone deacetylase and genomic DNA. These results demonstrate the dual targeting strategy to be a valuable route to pursue in the design of platinum agents which may be more effective in cancer types that are typically resistant to therapy by conventional cisplatin. Moreover, platinum(IV) derivatives containing VPA axial ligands seem to be promising dual-targeting candidates for additional preclinical studies.
Graphical abstractNew anticancer prodrugs, Pt(IV) derivatives of oxaliplatin with one or two axial valproato (2-propylpentanoate) ligand(s), were synthesized and characterized. These conjugates display activity in both cisplatin sensitive- and resistant tumor cells capable of both markedly enhanced accumulation in tumor cells and dual targeting of histone deacetylase and DNA simultaneously.Figure optionsDownload full-size imageDownload as PowerPoint slide
