Synthese, in vivo- und in vitro-Untersuchungen zur tumorhemmenden Wirkung von cis-Dichloro-dipeptidester-platin(II)-Komplexen / Synthesis, in vivo and in vitro Studies on the Antineoplastic Effect of cis-Dichloro-dipeptide Ester Platinum(II) Complexes

Abstract

Cis-Dichlorodipeptide esterplatinum complexesCl₂Pt(MetGlyOEt),Cl₂Pt(EthionylGlyOEt), Cl₂Pt(GlyGlyOEt)2 and Cl₂Pt(GlySerOEt)₂ are prepared from the α-amino acid complexes by peptide synthesis using platinum as an amino protecting group. cis-Cl₂Pt(GlyGlyOEt)2 and cis-Cl₂Pt(GlySerOEt)2 have been prepared also directly from K₂PtCl₄ and the dipeptidesters. cis-Cl₂Pt(GlyGlyOEt)₂ (2 a) and cis-Cl₂Pt(NH₃)₂ (5) lead to a prefered inhibition of the DNA-synthesis of sarcoma 180, Yoshida-sarcoma and Walker-256-carcinosarcoma in vitro; RNA- and protein biosynthesis are influenced to a much lower degree. 2a and 5 cause filamentous growth in Escherichia coli B. The DNA polymerase deficient strain of E. coli, p 3478 pol A-, is more inhibited by 2 a and 5 than the non deficient strain W 3110 pol A⁺. Tumor growth of di-2-chloro-ethylmethylamine (HN₂) resistant sarcoma 180 and of Yoshida sarcoma is weakly inhibited, whereas Walker-256-carcinosarcoma is markedly inhibited; however 2a and 5 show similar inhibition of the same tumor.