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通过改变环取代基降低乳腺肿瘤抑制药物[1,2-双(2,6-二氯-4-羟基苯基)-乙二胺]二氯铂(II)的雌激素副作用。

Reduction of the estrogenic side effects of the mammary tumor-inhibiting drug [1,2-bis(2,6-dichloro-4-hydroxyphenyl)- ethylenediamine]dichloroplatinum(II) by variation of ring substituents.

作者信息

Gust R, Karl J, Faderl M, Schönenberger H

机构信息

Institut für Pharmazie, Lehrstuhl Pharmazeutische Chemie II der Universität Regensburg, Germany.

出版信息

Arch Pharm (Weinheim). 1995 May;328(5):457-63. doi: 10.1002/ardp.19953280511.

Abstract

[1,2-Bis(4-methoxy/4-hydroxyphenyl)ethylenediamine]dichloroplatinum-(II) complexes with Cl-, CH3-, or OCH3-substituents in the ortho-positions of the aromatic rings (meso-1-PtCl2, D,L-1-PtCl2, meso-2-PtCl2, D,L-2-PtCl2, meso-3-PtCl2, meso-4-PtCl2, meso-5-PtCl2) were tested on the MDA-MB 231 breast cancer cell line, the lymphocytic leukemia P388, and the estrogen receptor-positive and -negative MXT mammary carcinoma of the mouse (MXT,ER(+)-MC, MXT,ER(-)-MC). The comparison of the effects of methoxy-substituted complexes (meso-1-PtCl2, D,L-1-PtCl2, meso-3-PtCl2) with those of the respective hydroxy-substituted ones (meso-2-PtCl2, D,L-2-PtCl2, meso-4-PtCl2) shows that a reduction of estrogenic effects as well as a total loss of the mammary tumor-inhibiting activity takes place on methylation of the 4-OH group. The exchange of the 2,6-standing chlorine atoms by methyl groups in meso-2-PtCl2 led to the non-estrogenic, but on the MXT,ER(+)-MC highly effective derivative meso-4-PtCl2 which proved to be also cytotoxic on ER(-)-tumors such as MXT,ER(-)-MC, and the P388 leukemia.

摘要

在芳香环邻位带有Cl-、CH3-或OCH3取代基的[1,2-双(4-甲氧基/4-羟基苯基)乙二胺]二氯铂-(II)配合物(内消旋-1-PtCl2、D,L-1-PtCl2、内消旋-2-PtCl2、D,L-2-PtCl2、内消旋-3-PtCl2、内消旋-4-PtCl2、内消旋-5-PtCl2)在MDA-MB 231乳腺癌细胞系、淋巴细胞白血病P388以及小鼠雌激素受体阳性和阴性的MXT乳腺癌(MXT、ER(+)-MC、MXT、ER(-)-MC)上进行了测试。甲氧基取代的配合物(内消旋-1-PtCl2、D,L-1-PtCl2、内消旋-3-PtCl2)与相应的羟基取代的配合物(内消旋-2-PtCl2、D,L-2-PtCl2、内消旋-4-PtCl2)效果比较表明,4-OH基团甲基化会导致雌激素效应降低以及乳腺肿瘤抑制活性完全丧失。内消旋-2-PtCl2中2,6位的氯原子被甲基取代后,得到了非雌激素性的但对MXT、ER(+)-MC高效的衍生物内消旋-4-PtCl2,该衍生物对ER(-)肿瘤如MXT、ER(-)-MC以及P388白血病也具有细胞毒性。

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