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哌啶配体对双功能单核铂配合物中反式几何结构的活化作用。抗肿瘤作用的机制研究。

Activation of trans geometry in bifunctional mononuclear platinum complexes by a piperidine ligand. Mechanistic studies on antitumor action.

作者信息

Kasparkova Jana, Novakova Olga, Marini Victoria, Najajreh Yousef, Gibson Dan, Perez Jose-Manuel, Brabec Viktor

机构信息

Institute of Biophysics, Academy of Sciences of the Czech Republic, CZ-61265 Brno, Czech Republic.

出版信息

J Biol Chem. 2003 Nov 28;278(48):47516-25. doi: 10.1074/jbc.M304720200. Epub 2003 Sep 10.

DOI:10.1074/jbc.M304720200
PMID:12970368
Abstract

A paradigm for the structure-pharmacological activity relationship of bifunctional platinum antitumor drugs is that the trans isomer of antitumor cisplatin (transplatin) is clinically ineffective. To this end, however, several new complexes of the trans structure have been identified that exhibit cytotoxicity in tumor cells that is even better than that of the analogous cis isomers. We reported recently (Kasparkova, J., Marini, V., Najajreh, Y., Gibson, D., and Brabec, V. (2003) Biochemistry 42, 6321-6332) that the replacement of one ammine ligand by the heterocyclic ligand, such as piperidine, piperazine, or 4-picoline in the molecule of transplatin resulted in a radical enhancement of its cytotoxicity. We examined oligodeoxyribonucleotide duplexes bearing a site-specific cross-link of the transplatin analogue containing the piperidine ligand by biochemical methods. The results indicate that in contrast to transplatin, trans-(PtCl2(NH3)(piperidine)) forms stable 1,3-intrastrand cross-links in double-helical DNA that distort DNA and are not readily removed from DNA by nucleotide excision repair system. Hence, the intrastrand cross-links of trans-(PtCl2(NH3)(piperidine)) could persist for a sufficiently long time, potentiating its toxicity toward tumor cells. trans-(PtCl2(NH3)(piperidine)) also forms in DNA minor interstrand cross-links that are similar to those of transplatin so that these adducts appear less likely candidates for genotoxic lesion responsible for antitumor effects of trans-(PtCl2(NH3)(piperidine)). Hence, the role of structurally unique intrastrand cross-links in the anti-tumor effects of transplatin analogues in which one ammine group is replaced by a heterocyclic ligand may predominate.

摘要

双功能铂类抗肿瘤药物结构-药理活性关系的一个范例是,抗肿瘤顺铂(反铂)的反式异构体在临床上无活性。然而,在此基础上,已鉴定出几种新的反式结构配合物,它们在肿瘤细胞中表现出的细胞毒性甚至优于类似的顺式异构体。我们最近报道(卡斯帕科娃,J.,马里尼,V.,纳贾雷,Y.,吉布森,D.,和布拉贝克,V.(2003年)《生物化学》42卷,6321 - 6332页),在反铂分子中用杂环配体(如哌啶、哌嗪或4-甲基吡啶)取代一个氨配体,会使其细胞毒性显著增强。我们通过生化方法研究了带有含哌啶配体的反铂类似物位点特异性交联的寡脱氧核糖核苷酸双链体。结果表明,与反铂不同,反式-(PtCl2(NH3)(哌啶))在双螺旋DNA中形成稳定的1,3-链内交联,使DNA扭曲,且不易被核苷酸切除修复系统从DNA中去除。因此,反式-(PtCl2(NH3)(哌啶))的链内交联可能会持续足够长的时间,增强其对肿瘤细胞的毒性。反式-(PtCl2(NH3)(哌啶))在DNA小沟中也形成链间交联,与反铂的类似,因此这些加合物似乎不太可能是导致反式-(PtCl2(NH3)(哌啶))抗肿瘤作用的基因毒性损伤的候选物。因此,在一个氨基团被杂环配体取代的反铂类似物的抗肿瘤作用中,结构独特的链内交联的作用可能占主导地位。

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