| Literature DB >> 26775068 |
Nicola Margiotta1, Salvatore Savino2, Cristina Marzano3, Concetta Pacifico2, James D Hoeschele4, Valentina Gandin3, Giovanni Natile5.
Abstract
Kiteplatin, the neglected drug analogous of cisplatin but containing cis-1,4-DACH in place of the two ammines, has been recently reevaluated for its activity against cisplatin- and oxaliplatin-resistant tumors, in particular colo-rectal cancer. With the aim of further improving the pharmacological activity of this drug, Pt(IV) prodrugs were derived by addition of two, differently substituted, benzoate groups in axial positions (X-ray structure). The cytotoxic activity of both compounds resulted markedly potentiated reaching nanomolar concentration against a wide panel of human cancer cells. The ability of benzoate ligands to enhance the activity of kiteplatin most likely originates from their lipophilicity promoting a higher drug accumulation in cancer cells; however, it is to be noted that the increase in pharmacological effect is far greater than the increase in cellular uptake. Overcoming cisplatin- and oxaliplatin-resistance by kiteplatin derivatives appears to relate to the inability of membrane extrusion pumps to remove active Pt species from tumor cells.Entities:
Keywords: Benzoate ligands; Cell growth inhibition; Cellular accumulation; Kiteplatin; Pt(IV) complexes; X-ray crystal structure
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Year: 2015 PMID: 26775068 DOI: 10.1016/j.jinorgbio.2015.11.028
Source DB: PubMed Journal: J Inorg Biochem ISSN: 0162-0134 Impact factor: 4.155