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Interaction of 2-aminopyrimidine with dichloro-1-alkyl-2-(naphthylazo) imidazolepalladium(II) complexes : Kinetic and mechanistic studies

机译:2-氨基嘧啶与二氯-1-烷基-2-(萘偶氮咪唑)咪唑钯(II)配合物的相互作用:动力学和机理研究

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摘要

BackgroundThe anticancer properties of cisplatin and palladium(II) complexes stem from the ability of the cis-MCl2 fragment to bind to DNA bases. However, cisplatin also interacts with non-cancer cells, mainly through bonding molecules containing -SH groups, resulting in nephrotoxicity. This has aroused interest in the design of palladium(II) complexes of improved activity and lower toxicity. The reaction of DNA bases with palladium(II) complexes with chelating N,N/donors of the cis-MCl2 configuration constitutes a model system that may help explore the mechanism of cisplatin's anticancer activity. Heterocyclic compounds are found widely in nature and are essential to many biochemical processes. Amongst these naturally occurring compounds, the most thoroughly studied is that of pyrimidine. This was one of the factors that encouraged this study into the kinetics and mechanism of the interaction of 2-aminopyrimidine (2-NH2-Pym) with dichloro-{1-alkyl-2-(α-naphthylazo)imidazole}palladium(II) [Pd(α-NaiR)Cl2, >1] and dichloro-{1-alkyl-2-(β-naphthylazo)imidazole}palladium(II) [Pd(β-NaiR)Cl2, >2] complexes where the alkyl R = Me (>a), Et (>b), or Bz (>c).
机译:背景顺铂和钯(II)配合物的抗癌特性源于顺式MCl2片段与DNA碱基结合的能力。但是,顺铂也主要通过包含-SH基团的键合分子与非癌细胞相互作用,从而产生肾毒性。这引起了人们对设计具有更高活性和更低毒性的钯(II)配合物的兴趣。 DNA碱基与钯(II)配合物与顺式-MCl2构型的螯合N,N / 供体的反应构成了一个模型系统,可以帮助探索顺铂的抗癌活性机理。杂环化合物广泛存在于自然界中,并且对于许多生化过程都是必不可少的。在这些天然存在的化合物中,最深入研究的是嘧啶。这是鼓励该研究2-氨基嘧啶(2-NH2-Pym)与二氯-{1-烷基-2-(α-萘基偶氮)咪唑}钯(II)相互作用的动力学和机理的因素之一。 [Pd(α-NaiR)Cl2,> 1] 和二氯-{1-烷基-2-(β-萘基偶氮)咪唑}钯(II)[Pd(β-NaiR)Cl2, > 2] 复杂,其中烷基R = Me(> a ),Et(> b )或Bz(> c )。

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