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A Screening Strategy for Metal Antitumor Agents as Exemplified byGold(III) Complexes

机译:以金属抗肿瘤药为例的筛选策略金(III)络合物

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摘要

The use of a screening strategy based on human tumor cell lines, which are also tumorigenic in immune-deprived mice, is described. Activity against the human tumor cells in vitro and in vivo, is complemented with studies on the mechanism of action. This aporoach is demonstrated using 2-[(dimethylamino)-methyl]phenyl (damp) gold(III) compounds of the type [Au X2(damp)], where X = chloride, thiocyanate, acetate, or the bidentate ligands oxalate and malonate. All compounds were shown to be selectively active against a human bladder tumor cell line (HT1376) in vitro, and active in an in vitro panel of ovarian tumor cell lines. The acetato complex was shown to be active in experimental animal models of both the HT1376 bladder tumor, and the CH1 ovarian tumor. Although the [AuX2(damp)] compounds share structural features in common with cisplatin, and exhibit interesting in vivo activity against human tumor cells, the data indicate that they have a very different biochemical mechanism from platinum-based drugs and represent a potentially new class of metal-based antitumor agents.
机译:描述了基于人肿瘤细胞系的筛选策略的使用,所述人肿瘤细胞系在免疫丧失的小鼠中也是致瘤的。在体外和体内对人肿瘤细胞的活性与作用机理的研究相辅相成。使用[Au X2(damp)]类型的2-[((二甲基氨基)-甲基]苯基(潮湿)金(III)化合物证明了这种孔隙,其中X =氯化物,硫氰酸盐,乙酸盐或双齿配体草酸盐和丙二酸盐。已显示所有化合物在体外对人膀胱肿瘤细胞系(HT1376)均具有选择性活性,并且在卵巢肿瘤细胞系的体外组中具有活性。乙酰复合物在HT1376膀胱肿瘤和CH1卵巢肿瘤的实验动物模型中均具有活性。尽管[AuX2(damp)]化合物具有与顺铂相同的结构特征,并且对人肿瘤细胞显示出有趣的体内活性,但数据表明它们与基于铂的药物具有非常不同的生化机制,并且代表了潜在的新类别金属基抗肿瘤药。

著录项

  • 期刊名称 Metal-Based Drugs
  • 作者

    Simon P. Fricker;

  • 作者单位
  • 年(卷),期 1999(6),4-5
  • 年度 1999
  • 页码 291–300
  • 总页数 10
  • 原文格式 PDF
  • 正文语种
  • 中图分类 药学;
  • 关键词

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