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Fragment-based lead generation: identification of seed fragments by a highly efficient fragment screening technology

机译:基于片段的线索生成:通过高效片段筛选技术识别种子片段

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摘要

For the detection of the precise and unambiguous binding of fragments to a specific binding site on the target protein, we have developed a novel reporter displacement binding assay technology. The application of this technology for the fragment screening as well as the fragment evolution process with a specific modelling based design strategy is demonstrated for inhibitors of the protein kinase p38alpha. In a fragment screening approach seed fragments were identified which were then used to build compounds from the deep-pocket towards the hinge binding area of the protein kinase p38alpha based on a modelling approach. BIRB796 was used as a blueprint for the alignment of the fragments. The fragment evolution of these deep-pocket binding fragments towards the fully optimized inhibitor BIRB796 included the modulation of the residence time as well as the affinity. The goal of our study was to evaluate the robustness and efficiency of our novel fragment screening technology at high fragment concentrations, compare the screening data with biochemical activity data and to demonstrate the evolution of the hit fragments with fast kinetics, into slow kinetic inhibitors in an in silico approach.
机译:为了检测片段与靶蛋白上特定结合位点的精确且明确的结合,我们开发了一种新颖的报道基因置换结合测定技术。证明了该技术在片段筛选以及片段进化过程中基于特定建模的设计策略的应用,证明了该蛋白激酶p38alpha的抑制剂。在片段筛选方法中,基于建模方法,确定了种子片段,然后将其用于从深口袋向蛋白激酶p38alpha的铰链结合区构建化合物。 BIRB796用作片段比对的蓝图。这些深口袋结合片段向完全优化的抑制剂BIRB796的片段进化包括停留时间和亲和力的调节。我们研究的目的是评估在高片段浓度下我们新颖的片段筛选技术的稳健性和效率,将筛选数据与生化活性数据进行比较,并证明具有快速动力学特性的命中片段演变为慢速动力学抑制剂。计算机方法。

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