BREAST CANCER-INHIBITING PROPERTIES OF LEAVING GROUP DERIVATIVES OF [1,2-BIS(2,6-DIFLUORO-3-HYDROXYPHENYL)ETHYLENEDIAMINE]PLATINUM(II)

GUST, R and SCHONENBERGER, H (1993) BREAST CANCER-INHIBITING PROPERTIES OF LEAVING GROUP DERIVATIVES OF [1,2-BIS(2,6-DIFLUORO-3-HYDROXYPHENYL)ETHYLENEDIAMINE]PLATINUM(II). EUROPEAN JOURNAL OF MEDICINAL CHEMISTRY, 28 (2). pp. 117-127. ISSN 0223-5234,

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Abstract

Meso-configurated [1,2-bis(2,6-difluoro-3-hydroxyphenyl)ethylenediamine]platinum(II) complexes (meso4-PtX2) with SO42-, NO3-, PhSO3- cyclobutane-1,1-dicarboxylate (CBDC) and isocitrate as the leaving groups (X) and the two diastereomeric dichloroplatinum(II) derivatives were synthesized. The influence of the leaving groups of meso-4-PtX2 on several murine tumors: P388 leukemia, MXT-M3.2 breast cancer (hormone-sensitive) and MXT-Ovex breast cancer (hormone-insensitive) was studied. The compounds with leaving groups, which are more easily exchangeable by water molecules (SO42-, NO3-, PhSO3, produced stronger tumor inhibition and also more pronounced side effects than those with moderately stable (Cl-) or stable (CBDC, isocitrate) bond leaving groups. Against the P388 leukemia, none of the tested complexes were cytotoxic to the same extent as cisplatin. The MXT-Ovex breast cancer, however, was strongly inhibited by meso-4-PtSO4 which was even more active than cisplatin. The hormone-sensitive MXT-M3.2 breast cancer underwent 78% inhibition by the most interesting compound of the meso-4-PtX2 leaving-group series (ie meso-4-PtCl2) at the non-toxic dosage of 5 mumol/kg. With the well-tolerated, more active diastereomer. D.L.-4-PtCl2, 99% inhibition of tumor growth could be achieved at a dose of 10 mumol/kg.

Item Type: Article
Uncontrolled Keywords: DEPENDENT MAMMARY-CARCINOMA; <1,2-BIS(FLUOROPHENYL)ETHYLENEDIAMINE>PLATINUM(II) COMPLEXES; TUMOR; [1,2-BIS(2,6-DIFLUORO-3-HYDROXYPHENYL)ETHYLENEDIAMINE]PLATINUM(II) COMPLEXES; SO4-2-, NO3-(-), PHSO3-(-), CL-(-), CYCLOBUTANE-1,1-DICARBOXYLATE (CBDC)-LEAVING AND ISOCITRATE-LEAVING GROUPS; SYNTHESIS; TUMOR-INHIBITING PROPERTIES; P388 MOUSE LEUKEMIA; MXT MOUSE MAMMARY TUMOR; HORMONE-SENSITIVE AND HORMONE-INSENSITIVE
Depositing User: Dr. Gernot Deinzer
Last Modified: 19 Oct 2022 08:43
URI: https://pred.uni-regensburg.de/id/eprint/54182

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