Developing new anti-cancer drugs: novel targets and methodological problems.

Forum (Genoa, Italy) Pub Date : 1999-07-01
V Spataro, C Sessa
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Abstract

The identification of molecular events relevant in the biology of cancer cells and the possibility of defining the molecular profile of cancer cell lines have radically changed the process of cancer-drug development. Cancer drug discovery relies now mainly on the National Cancer Institute cell line screening program; this screening system allows the selection of compounds with well-defined molecular mechanisms of action by screening them on cell lines characterised at the molecular level and by comparing their cytotoxicity through a computer-based analysis of the response profile. Biologically targeted drugs, which should hit specific molecular or biochemical targets, can be classified by a specific target, such as farnesyltransferase inhibitors, or by general mechanism of action. The clinical development of these new anti-cancer agents presents a significant challenge because clinical studies should comply with the molecular premises and be devised in order to provide the "proof of principle", that is the ability of the drug to interact with and activate or block the molecular target. After a summary of the main features and problems faced in the clinical development of biologically targeted anti-cancer therapies, the pre-clinical and clinical data available for some cell-cycle modulators, signal transduction inhibitors, drugs acting on the mitochondria and proteasome inhibitors will be reviewed.

开发新的抗癌药物:新的靶点和方法问题。
癌细胞生物学中相关分子事件的识别以及确定癌细胞系分子谱的可能性从根本上改变了抗癌药物的开发过程。癌症药物的发现现在主要依赖于国家癌症研究所的细胞系筛选项目;该筛选系统允许选择具有明确分子作用机制的化合物,方法是在分子水平上对具有特征的细胞系进行筛选,并通过基于计算机的反应谱分析比较它们的细胞毒性。生物靶向药物是指靶向特定的分子或生化靶标的药物,可根据特定靶标(如法尼基转移酶抑制剂)或一般作用机制进行分类。这些新型抗癌药物的临床开发面临着重大挑战,因为临床研究应遵循分子前提,并设计为提供“原理证明”,即药物与分子靶点相互作用并激活或阻断的能力。在总结生物靶向抗癌治疗临床发展的主要特点和面临的问题后,对一些细胞周期调节剂、信号转导抑制剂、作用于线粒体的药物和蛋白酶体抑制剂的临床前和临床资料进行了综述。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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