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金类抗癌药物的生物学评价策略。

Strategies for the biological evaluation of gold anticancer agents.

机构信息

Genzyme Corp., Framingham, MA 01701, USA.

出版信息

Anticancer Agents Med Chem. 2011 Dec;11(10):940-52. doi: 10.2174/187152011797927634.

Abstract

Since the introduction of the monomeric orally bioavailable anti-arthritic gold compound auranofin in 1985, and the success of the platinum-based anti-cancer drugs, there has been a great deal of interest in the use of gold compounds for cancer therapy. However this early promise has not materialized into an approved drug in spite of extensive and innovative efforts in gold chemistry. Therefore, in the light of this lack of success, the strategies for the biological evaluation of potential gold-based anti-cancer drugs are discussed. It is proposed that the biological testing strategy should be multi-faceted incorporating an understanding of the molecular properties of the compounds under investigation related to their behaviour in a biological environment, an evaluation of their comparative in vitro potency against tumor cells, ascertaining the biochemical mechanism of action and target identification to aid in medicinal chemistry design, evaluation of in vivo activity in relevant tumor models, and an understanding of their toxicological and pharmacokinetic properties. This strategy will be exemplified with work on Au(III) cyclometallated complexes in which an integrated approach to the search for new metal-based anticancer drugs was adopted, incorporating in vitro screening, in vivo human tumor xenograft models, and mechanistic studies. The importance of mechanistic studies which have led to the identification of new molecular targets for gold drugs, and in vivo evaluation are emphasized.

摘要

自 1985 年单体口服生物可利用抗关节炎金化合物金诺芬问世,以及铂类抗癌药物取得成功以来,人们对金化合物在癌症治疗中的应用产生了浓厚的兴趣。然而,尽管在金化学方面进行了广泛而创新的努力,这种早期的承诺并没有转化为一种批准的药物。因此,鉴于这种缺乏成功,我们讨论了用于评估潜在基于金的抗癌药物的生物学策略。有人提出,生物测试策略应该是多方面的,包括了解与化合物在生物环境中的行为相关的分子特性,评估它们对肿瘤细胞的体外相对效力,确定生化作用机制和靶标鉴定以辅助药物化学设计,在相关肿瘤模型中评估体内活性,并了解其毒性和药代动力学特性。这项策略将通过 Au(III) 配位金属复合物的工作得到例证,其中采用了一种综合方法来寻找新的金属抗癌药物,包括体外筛选、体内人肿瘤异种移植模型和机制研究。强调了机制研究的重要性,这些研究导致了对金药物的新分子靶标的识别和体内评估。

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