The stereoselectivity of antitumor active [1,2-diamino-1-phenylpropane]dichloroplatinum(II) complexes

被引：17

作者：

Gust, R

Gelbcke, M

Angermaier, B

Bachmann, H

Krauser, R

Schonenberger, H

机构：

[1] FREE UNIV BRUSSELS,LAB CHIM PHARMACEUT ORGAN,INST PHARM,B-1050 BRUSSELS,BELGIUM

[2] UNIV REGENSBURG,LAB PHARMAZEUT CHEM 2,INST PHARM,D-93040 REGENSBURG,GERMANY

来源：

INORGANICA CHIMICA ACTA | 1997年 / 264卷 / 1-2期

关键词：

antitumor activity; platinum complexes; diamine complexes; stereoselectivity;

D O I：

10.1016/S0020-1693(97)05603-X

中图分类号：

O61 [无机化学];

学科分类号：

070301 ; 081704 ;

摘要：

The syntheses of enantiomeric threo- and erythro-1,2-diamino-1-phenylpropanes (Ph/Me) and of the racemic 1,2-diaminophenylethane (Ph/H) are described. These diamines and related N-2-methyl- and N-1,N-2-dimethyl-l,2-diamino-1-phenylpropanes were transformed into dichloroplatinum(II) complexes (Ph/H-PtCl2, Ph/Me-PtCl2, Ph/Me-Me-PtCl2, Ph/Me-Dime-PtCl2). For the H-1 NMR spectroscopical determination of their optical purity the diamines (Ph/Me) were converted with (R)-myrtenal into their diimines. In the test on the MCF-7 breast cancer cell line (R,R)-Ph/Me-PtCl2 produced the strongest effect of all new complexes, comparable with that of the standard cisplatin and of other Pt complexes. Its enantiomer (S,S)-Ph/Me-PtCl2 possessed a distinctly weaker inhibitory potency while the erythro-configurated counterparts were even less active [(R,R) > (S,S) > (S,R) = (R,S)]. All N-2-methylated and N-1,N-2-dimethylated complexes (Ph/Me-Me-PtCl2, Ph/Me-Dime-PtCl2) showed comparable activities equaling those of (R,S)- and (S,R)-Ph/Me-PtCl2. The molecular reasons for the differing potencies of the diastereomeric and enantiomeric Ph/Me-PtCl2 complexes are discussed in consideration of the complex conformation. (C) 1997 Elsevier Science S.A.

引用

页码：145 / 160

页数：16

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