Sensitivity to Cisplatin and Platinum-Containing Compounds of Schizosaccharomyces pombe Rad Mutants

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Vol. 54, Issue 1, 213-219, July 1998

Sensitivity to Cisplatin and Platinum-Containing Compounds of Schizosaccharomyces pombe Rad Mutants

Paola Perego, Franco Zunino, Nives Carenini, Fernando Giuliani, Silvano Spinelli, and Stephen B. Howell

Department of Experimental Oncology B, Istituto Nazionale per lo Studio e la Cura dei Tumori, 20133 Milan, Italy (P.P., F.Z., N.C.), Boehringer Mannheim Italia, Monza, Italy (F.G., S.S.) and Department of Medicine and the Cancer Center, University of California, San Diego, La Jolla, CA 92094 (S.B.H.).

The role of genes that affect response to radiation in determining sensitivity to platinum-containing compounds was studiedusing a panel of 23 strains of the yeast Schizosaccharomyces pombe.The radiation-hypersensitive mutants all had the same geneticbackground and most of them contained mutations that disabledeither cell cycle checkpoints or DNA repair. The tested platinumcompounds included cisplatin and two complexes containing diaminocyclohexane(oxaliplatin and tetraplatin), two ammine/cyclohexylamine complexeswith different orientation of the leaving groups (JM216 and JM335)and a multinuclear platinum complex (BBR 3464). The cytotoxiceffect of the selected platinum complexes was evaluated by usinga microtiter growth inhibition assay with a 48 hr exposure todrug. The mutants fell into three groups with respect to sensitivityto cisplatin: four mutants (rad2, -7, -11, -15) exhibited minimalchange in sensitivity; fifteen mutants (rad4-6, -8-10, -12-14,-16-17, -19-21, and -22) were 5.1-21.7-fold hypersensitive; onlyrad1 and -3 mutants, defective in checkpoints, and rad18, defectivein repair, displayed a marked hypersensitivity. None of the mutantsdemonstrated appreciable change in sensitivity to JM216 presumablyas a consequence of a lack of resistance of the wild-type strain,whereas a moderate increase in sensitivity to JM335 was observedfor most of the mutants, and hypersensitivity to BBR3464 was observedonly in rad1 and -3. No relevant changes in sensitivity to tetraplatinwere observed. Most of the mutants, with the exception of rad2,-7, and -15, were hypersensitive to oxaliplatin. These findingsdemonstrate that specific mutations have disparate effects onthe profile of sensitivity to different members of the same classof cytotoxic agents, which provides genetic evidence that differentmechanisms are involved in differential cytotoxicity induced byPt compounds. The results also demonstrate the utility of sucha panel of mutants, constructed on the same genetic background,for detecting specific cellular response; presumably, this reflectsthe recognition or processing of specific DNA adducts. In conclusion,because the rad1 and rad3 gene products are determinants of cellularresponse to a large number of platinum-containing compounds, thepresent results support a critical role of genes involved in cellcycle control in cellular sensitivity to these agents.

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