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The Discovery of Kvl.5 Blockers as a Case Study for the Application of Virtual Screening Approaches

机译:Kvl.5阻滞剂的发现作为虚拟筛选方法应用的案例研究

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Different virtual screening techniques are available as alternatives to high throughput screening.These different techniques have been rarely used together on the same target.We had the opportunity to do so in order to discover novel blockers of the voltage-dependent potassium channel Kvl.5,a potential target for the treatment of atrial fibrillation.Our corporate database was searched,using a protein-based pharmacophore,derived from a homology model,as query.As a result,244 molecules were screened in vitro,19 of them (7.8%) were found to be active.Five of them,belonging to five different chemical classes,exhibited IC_(50) values under 10 muM.The performance of this structure-based virtual screening protocol has been compared with those of similarity and ligand-based pharmacophore searches.The analysis of the results supports the conventional wisdom of using as many virtual screening techniques as possible in order to maximize the chance of finding as many chemotypes as possible.
机译:可以使用不同的虚拟筛选技术替代高通量筛选。这些不同的技术很少在同一目标上一起使用。我们有机会这样做,以发现电压依赖性钾通道Kvl.5的新型阻断剂,我们使用基于同源模型的基于蛋白质的药效基团搜索了我们的公司数据库,结果在体外筛选了244个分子,其中19个分子(7.8%)被发现具有活性。其中五个,属于五种不同的化学类别,在10μM以下表现出的IC_(50)值。已将该基于结构的虚拟筛选方案的性能与相似性和基于配体的药效团进行了比较结果分析支持使用尽可能多的虚拟筛查技术以最大化发现尽可能多的化学型的机会的传统智慧。

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