AI Article Synopsis

  • Cisplatin has been a key anti-cancer drug for over 30 years, and research continues to find ways to minimize its toxicity and resistance.
  • Recent studies propose new dinuclear platinum complexes that use bridging bisphosphonates, which may enhance cancer treatment directly at tumor sites in the bone.
  • The paper describes the synthesis and characterization of four new platinum complexes, evaluated for their effectiveness against various human tumor cell lines, including those resistant to cisplatin.

Article Abstract

For over 30 years cisplatin has been one of the most active antitumour agents in clinical use, nevertheless research for overcoming cisplatin toxicity and resistance or for improving its efficacy has never ceased. In this context we have recently proposed dinuclear Pt complexes with bridging geminal bisphosphonates as novel Pt-prodrugs with potential activity at the bone surface after embedment in inorganic matrices and implantation at the tumour site. In the present paper we report the synthesis and full characterization of four new platinum complexes having a dinuclear structure with a bisphosphonate (2-ammonium-1-hydroxyethane-1,1-diyl-bisphosphonate or 3-ammonium-1-hydroxypropane-1,1-diyl-bisphosphonate, AHBP-H and PAM-H, respectively) acting as a bridging ligand between two platinum moieties (cis-[Pt(NH(3))(2)](2+), directly related to cisplatin, and [Pt(cis-1,4-DACH)](2+), known to be able to overcome the cisplatin resistance). Moreover, as a preliminary investigation, the in vitro cytotoxicity of the new complexes has been evaluated on a panel of 13 human tumour cell lines including cisplatin- and multidrug-resistant sublines.

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Source
http://dx.doi.org/10.1039/b919721dDOI Listing

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