Literature DB >> 9092638

Effect of geometric isomerism in dinuclear platinum antitumour complexes on the rate of formation and structure of intrastrand adducts with oligonucleotides.

K J Mellish1, Y Qu, N Scarsdale, N Farrell.   

Abstract

The dinuclear platinum complexes [[trans -PtCl (NH3)2]2[mu]-[NH2(CH2) n NH2]](NO3)2[1,1/t,t ( n = 4,6)] and [[cis-PtCl(NH3)2]2[mu];-[NH2(CH2) n NH2](NO3) 2[1,1/c,c ( n = 4,6)] exhibit antitumour activity comparable with cisplatin. 1,1/c,c complexes do not form 1,2 GG intrastrand adducts, the major adduct of cisplatin, with double-stranded DNA. This 1H NMR spectroscopy study shows that, in the absence of a complementary strand, 1,1/c,c ( n = 4,6) form a 1,2 GG (N7, N7) intrastrand adduct with r(GpG), d(GpG) and d(TGGT). Initial binding to r(GpG) (and also reaction with GMP) at 37 degrees C was slower for 1,1/c,c compared with 1,1/t,t, whereas the second binding step (adduct closure) was faster for 1,1/c,c. However, the 1H NMR spectra of the 1,1/c,c adducts at 37 degrees C show two H8 signals, one of which is broad and becomes sharper on increasing the temperature, indicating restricted rotation around the Pt-N7 bond. For the d(GpG)-1,1/c,c ( n = 4) adduct, 2D NMR spectroscopy assigned the broad H8 signal to the 3' G, which has syn base orientation and 60% S-type/40% N-type sugar conformation. The 5' G has anti base orientation and S-type sugar conformation. Apart from the restricted rotation around the 3' G, the structure is similar to that of 1,2 GG intrastrand adducts of 1,1/t,t. This steric hindrance may explain the inability of 1,1/c,c complexes to form 1,2 GG intrastrand adducts with sterically more demanding double-stranded DNA.

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Year:  1997        PMID: 9092638      PMCID: PMC146552          DOI: 10.1093/nar/25.6.1265

Source DB:  PubMed          Journal:  Nucleic Acids Res        ISSN: 0305-1048            Impact factor:   16.971


  36 in total

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2.  Crystal structure of double-stranded DNA containing the major adduct of the anticancer drug cisplatin.

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Journal:  Nature       Date:  1995-10-19       Impact factor: 49.962

3.  Sequence specificity of DNA-DNA interstrand cross-link formation by cisplatin and dinuclear platinum complexes.

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4.  Structure and isomerization of an intrastrand cisplatin-cross-linked octamer DNA duplex by NMR analysis.

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5.  Formation of DNA adducts by the anticancer drug carboplatin: different nucleotide sequence preferences in vitro and in cells.

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Review 6.  Nonclassical platinum antitumor agents: perspectives for design and development of new drugs complementary to cisplatin.

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7.  DNA-binding properties of novel cis- and trans platinum-based anticancer agents in 2 human ovarian carcinoma cell lines.

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8.  Solution structure of a cisplatin-induced DNA interstrand cross-link.

Authors:  H Huang; L Zhu; B R Reid; G P Drobny; P B Hopkins
Journal:  Science       Date:  1995-12-15       Impact factor: 47.728

9.  Intrastrand cross-links are not formed in the reaction between transplatin and native DNA: relation with the clinical inefficiency of transplatin.

Authors:  M Boudvillain; R Dalbiès; C Aussourd; M Leng
Journal:  Nucleic Acids Res       Date:  1995-07-11       Impact factor: 16.971

10.  Effects of geometric isomerism and ligand substitution in bifunctional dinuclear platinum complexes on binding properties and conformational changes in DNA.

Authors:  N Farrell; T G Appleton; Y Qu; J D Roberts; A P Fontes; K A Skov; P Wu; Y Zou
Journal:  Biochemistry       Date:  1995-11-28       Impact factor: 3.162

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  1 in total

1.  Effects of geometric isomerism in dinuclear antitumor platinum complexes on their interactions with N-acetyl-L-methionine.

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  1 in total

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