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The use of mammalian two-hybrid technologies for high-throughput drug screening

机译:哺乳动物双杂交技术在高通量药物筛选中的应用

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Developing agents that target protein-protein interactions (PPIs) is an emerging field in drug discovery. Although this target class has hitherto remained underexplored, it holds exceptional promise related to the large amount of potential PPI targets compared to single protein targets and it offers important opportunities to increase the specificity of therapeutic molecules. While several PPI modulating therapeutics have recently been reported and a number of these are in clinical trial, progress in the field has been hampered by the lack of efficient screening systems. Recently, a number of cellular approaches have been developed that complement classical in vitro screening methods and which exhibit a number of important assets related to the physiological context they provide. Here we discuss the utility of two-hybrid technologies towards high-throughput screening for PPI inhibitors, in particular those that operate in a mammalian cellular background. We review a number of cases where mammalian two-hybrids have been successfully applied to identify small molecule disruptors of PPIs and zoom in further on the MAPPIT (Mammalian Protein-Protein Interaction Trap) technology platform. The value of this approach for drug discovery is illustrated by recent data from MAPPIT-based screening projects.
机译:靶向蛋白质-蛋白质相互作用(PPI)的显影剂是药物发现中的新兴领域。尽管迄今尚未对该靶标类别进行探索,但与单蛋白靶标相比,它具有与大量潜在PPI靶标有关的特殊前景,并且为提高治疗分子的特异性提供了重要机会。尽管最近已经报道了几种调节PPI的疗法,其中许多正在临床试验中,但是由于缺乏有效的筛选系统,该领域的进展受到了阻碍。近来,已经开发了许多细胞方法,这些方法补充了经典的体外筛选方法,并且展现出许多与其提供的生理环境有关的重要资产。在这里,我们讨论了两种杂交技术对PPI抑制剂(特别是在哺乳动物细胞背景下运行的PPI抑制剂)的高通量筛选的实用性。我们回顾了哺乳动物两杂交已成功应用于鉴定PPI的小分子干扰物并进一步放大MAPPIT(哺乳动物蛋白质-蛋白质相互作用陷阱)技术平台的许多情况。来自基于MAPPIT的筛查项目的最新数据说明了这种方法对药物发现的价值。

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