A Novel Trinuclear Platinum Complex Overcomes Cisplatin Resistance in an Osteosarcoma Cell System

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Vol. 55, Issue 3, 528-534, March 1999

A Novel Trinuclear Platinum Complex Overcomes Cisplatin Resistance in an Osteosarcoma Cell System

Paola Perego, Claudia Caserini, Laura Gatti, Nives Carenini, Simona Romanelli, Rosanna Supino, Donato Colangelo, Ilario Viano, Roberto Leone, Silvano Spinelli, Gabriella Pezzoni, Carla Manzotti, Nicholas Farrell, and Franco Zunino

Division of Experimental Oncology B, Istituto Nazionale per lo Studio e la Cura dei Tumori, Milan, Italy (P.P., C.C., L.G., N.C., S.R., R.S.); Department of Medical Sciences, Universita' degli Studi di Torino, Turin, Italy (D.C., I.V.); Department of Pharmacology, Universita' degli Studi di Verona, Verona, Italy (R.L.); Boehringer Mannheim Italia S.p.A., Monza, Italy (S.S., G.P., C.M.); and Department of Chemistry, Virginia Commonwealth University, Richmond, Virginia (N.F.)

Multinuclear platinum compounds have been designed to circumvent the cellular resistance to conventional platinum-based drugs.In an attempt to examine the cellular basis of the preclinicalantitumor efficacy of a novel multinuclear platinum compound (BBR3464) in the treatment of cisplatin-resistant tumors, we haveperformed a comparative study of cisplatin and BBR 3464 in a humanosteosarcoma cell line (U2-OS) and in an in vitro selected cisplatin-resistantsubline (U2-OS/Pt). A marked increase of cytotoxic potency ofBBR 3464 in comparison with cisplatin in U2-OS cells and a completelack of cross-resistance in U2-OS/Pt cells were found. A detailedanalysis of the cisplatin-resistant phenotype indicated that itwas associated with reduced cisplatin accumulation, reduced interstrandcross-link (ICL) formation and DNA platination, microsatelliteinstability, and reduced expression of the DNA mismatch repairprotein PMS2. Despite BBR 3464 charge and molecular size, in U2-OSand U2-OS/Pt cells, BBR 3464 accumulation and DNA-bound platinumwere much higher than those observed for cisplatin. In contrast,the frequency of ICLs after exposure to BBR 3464 was very low.The time course of ICL formation after drug removal revealed alow persistence of these types of DNA lesions induced by BBR 3464,in contrast to an increase of DNA lesions induced by cisplatin,suggesting that components of the DNA repair pathway handle thetwo types of DNA lesions differently. The cellular response ofHCT116 mismatch repair-deficient cells was consistent with a lackof influence of mismatch repair status on BBR 3464 cytotoxicity.Because BBR 3464 produces high levels of lesions different fromICLs, likely including intra-strand cross-links and monoadducts,the ability of the triplatinum complex to overcome cisplatin resistanceappears to be related to a different mechanism of DNA interaction(formation of different types of drug-induced DNA lesions) ascompared with conventional mononuclear complexes rather than theability to overcome specific cellularalterations.

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