Palladium(II) compounds with potential antitumour properties and their platinum analogues: A comparative study of the reaction of some orotic acid derivatives with DNA in vitro

被引:106
作者
Butour, JL
Wimmer, S
Wimmer, F
Castan, P
机构
[1] UNIV TOULOUSE 3, CHIM INORGAN LAB, F-31062 TOULOUSE, FRANCE
[2] CNRS, INST PHARMACOL & BIOL STRUCT, F-31077 TOULOUSE, FRANCE
[3] UNIV BRUNEI DARUSSALAM, DEPT CHEM, BANDAR SERI BEGAWAN, BRUNEI
关键词
antitumour activity; platinum compounds; palladium compounds; orotic acid metal compounds; DNA-metal complexes;
D O I
10.1016/S0009-2797(97)00022-7
中图分类号
Q5 [生物化学]; Q7 [分子生物学];
学科分类号
071010 ; 081704 ;
摘要
Ethidium bromide was used to study perturbations induced in salmon sperm DNA complexed with a series of platinum and palladium compounds obtained from chloro and erotic acid derivatives as leaving ligands. The antitumoral activity of these compounds against Sarcoma 180 cells grafted intraperitoneally into mice is correlated with their capacity to interact with DNA in vitro and to perturb its secondary structure. Nevertheless, among these compounds, [Pt(Dach)(3-methyl-orot)] and [Pt(Dach)(5-fluoro-orot)] do not interact with DNA in vitro and are inactive against Sarcoma 180 cells. This lack of activity originates from the fact that strong chelating properties of the ligand prevent hydrolysis of the compounds which are unable to give rise to aquo species which are the reactive ones. On the other hand, the interaction with DNA is not the only prerequisite in order that a compound be active towards tumour cells. In fact, cis-[Pd(NH3)(2)Cl-2] and cis-[Pd(Dach)Cl-2] are not antitumoral. It is well known that the former undergoes an inactive trans-conformation and that the two compounds hydrolyse very fast assuming that they interact in vivo with a lot of molecules particularly proteins preventing them to reach the DNA, their pharmalogical target. By contrast, [Pd(Dach)(3-methyl-orot)] (T/C = 267%) and [Pd(Dach)(5-fluoro-orot)](T/C = 270%) display significant antitumour activity. (C) 1997 Elsevier Science Ireland Ltd.
引用
收藏
页码:165 / 178
页数:14
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