Biophysical analysis of DNA modified by 1,2-diaminocyclohexane platinum(II) complexes
Modification of DNA and double-stranded deoxyoligonucleotides with antitumour 1, 2-diamino-cyclohexanedinitroplatinum(II) (Pt-dach) complexes was investigated with the aid of physico-chemical methods and chemical probes of nucleic acid conformation. The three Pt-dach complexes were used which differ...
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Veröffentlicht in: | Nucleic acids research 1992-01, Vol.20 (2), p.267-272 |
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Sprache: | eng |
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Zusammenfassung: | Modification of DNA and double-stranded deoxyoligonucleotides with antitumour 1, 2-diamino-cyclohexanedinitroplatinum(II) (Pt-dach) complexes was investigated with the aid of physico-chemical methods and chemical probes of nucleic acid conformation. The three Pt-dach complexes were used which differed in isomeric forms of the dach non-leaving D5gand-Pt(1R, 2R-dach), Pt(1S, 2S-dach) and Pt(1R, 2S-dach) complexes. The latter complex has lower antitumour activity than the other two Pt-dach complexes. Pt(1R, 2S-dach) complex exhibits the slowest [kinetics of its binding to DNA and of the conversion of monofunctional binding to bifunctional lesions. The anomalously slow electrophoretic mobility of multimers of the platinated and ligated oligomers suggests that bifunctional binding of Pt-dach complexes to a d(GG) site within double-stranded oligonucleotides induces bending of the oligomer. In addition, chemical probing of double-helical dexoyoligonucleoides modified by the Pt-dach complexes at the d(GG) sites reveals that Pt(1R, 2S-dach) complex induces more extensive conformatoonal changes in the oligomer than Pt(1R, 2R-dach) and Pt(1S, 2S-dach) complexes. It is proposed that different effects of the Pt-dach complexes on DNA observed in this work arise mainly from a steric crowding of the axially oriented cyclohexane ring in the DNA adduct of Pt(1R, 2S-dach) complex. |
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ISSN: | 0305-1048 1362-4962 |
DOI: | 10.1093/nar/20.2.267 |