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[新型亚硝基脲化合物的化疗特性]

[Chemotherapeutic characterization of new nitrosourea compounds].

作者信息

Zeller W J, Berger M R, Eisenbrand G, Petru E

机构信息

Institut für Toxikologie und Chemotherapie, Deutsches Krebsforschungszentrum, Heidelberg.

出版信息

Arch Geschwulstforsch. 1988;58(3):137-49.

PMID:3415433
Abstract

The development of new nitrosoureas is described using selected examples. Results obtained with water-soluble analogs and with compounds linked to biomolecules as for instance amino acids, oligopeptides and steroids, are presented. The pronounced antineoplastic effect of some water-soluble analogs is paralleled by an increased rate of DNA-interstrand cross-links and by an increased suppression of hematopoietic stem cells. The suppression of bone marrow stem cells is followed by their rapid regeneration. Water-soluble nitrosoureas induce significant less inhibition of glutathione reductase as compared with established compounds. With regard to long-term toxicity and carcinogenicity water-soluble are superior to established compounds as for instance BCNU. Linking of the nitrosourea moiety to amino acids and oligopeptides led to some analogs with outstanding therapeutic ratio. Out of a group of steroid-linked nitrosoureas, CNC-L-alanine-estradiol-17-ester (CNC-ala-17-E2) is chosen to demonstrate the possibility of reducing bone marrow toxicity despite unchanged or increased therapeutic activity by attachment of the nitrosourea moiety to a steroid. Results of a comparative interspecies in vitro evaluation of CNC-ala-17-E2 in transplanted MXT mammary carcinoma of the mouse, MNU-induced autochthonous rat mammary carcinoma and primary human mammary carcinomas are presented and the question is discussed to what extent in vitro activity of such receptor agents using the tumor stem cell assay reflects their in vivo activity.

摘要

本文通过选取的实例描述了新型亚硝基脲的研发情况。展示了水溶性类似物以及与生物分子(如氨基酸、寡肽和类固醇)相连的化合物所取得的结果。一些水溶性类似物显著的抗肿瘤作用伴随着DNA链间交联速率的增加以及对造血干细胞抑制作用的增强。骨髓干细胞受到抑制后会迅速再生。与已有的化合物相比,水溶性亚硝基脲对谷胱甘肽还原酶的抑制作用明显较小。在长期毒性和致癌性方面,水溶性亚硝基脲优于如卡莫司汀(BCNU)等已有的化合物。将亚硝基脲部分与氨基酸和寡肽相连得到了一些治疗指数优异的类似物。从一组与类固醇相连的亚硝基脲中,选择了CNC-L-丙氨酸-雌二醇-17-酯(CNC-ala-17-E2)来证明通过将亚硝基脲部分连接到类固醇上,在治疗活性不变或增加的情况下降低骨髓毒性的可能性。展示了在小鼠移植的MXT乳腺癌、N-甲基-N'-亚硝基脲(MNU)诱导的大鼠原位乳腺癌和原发性人类乳腺癌中对CNC-ala-17-E2进行种间体外比较评估的结果,并讨论了使用肿瘤干细胞测定法的此类受体药物的体外活性在多大程度上反映其体内活性的问题。

相似文献

1
[Chemotherapeutic characterization of new nitrosourea compounds].[新型亚硝基脲化合物的化疗特性]
Arch Geschwulstforsch. 1988;58(3):137-49.
2
[In vitro study of estradiol-linked nitrosourea in breast cancers in the mouse, rat and human: interspecies comparison].[雌二醇连接亚硝基脲对小鼠、大鼠和人类乳腺癌的体外研究:种间比较]
Wien Klin Wochenschr. 1989 Feb 17;101(4):130-4.
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Cytostatic activity of an estradiol-linked nitrosourea in MXT mammary carcinoma and L 5222 leukemia.一种雌二醇连接的亚硝基脲对MXT乳腺癌和L 5222白血病的细胞生长抑制活性。
Arzneimittelforschung. 1989 Dec;39(12):1577-9.
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Development of more selective anti-cancer nitrosoureas.更具选择性的抗癌亚硝基脲的研发。
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Eur J Cancer Clin Oncol. 1988 Jun;24(6):1027-32. doi: 10.1016/0277-5379(88)90153-8.
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Preclinical studies of steroid-linked nitrosoureas in murine pancreatic adenocarcinoma PANO2.类固醇连接的亚硝基脲在小鼠胰腺腺癌PANO2中的临床前研究。
J BUON. 2008 Apr-Jun;13(2):235-9.
7
Nitrosoureas: a review of experimental antitumor activity.亚硝基脲类:实验性抗肿瘤活性综述
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