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Novel Ligands for a Purine Riboswitch Discovered by RNA-Ligand Docking

机译:RNA配体对接发现嘌呤核糖开关的新型配体

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摘要

The increasing number of RNA crystal structures enables a structure-based approach to the discovery of new RNA-binding ligands. To develop the poorly explored area of RNA-ligand docking, we have conducted a virtual screening exercise for a purine riboswitch to probe the strengths and weaknesses of RNA-ligand docking. Using a standard protein-ligand docking program with only minor modifications, four new ligands with binding affinities in the micromolar range were identified, including two compounds based on molecular scaffolds not resembling known ligands. RNA-ligand docking performed comparably to protein-ligand docking indicating that this approach is a promising option to explore the wealth of RNA structures for structure-based ligand design.
机译:RNA晶体结构的数量不断增加,使得能够采用基于结构的方法来发现新的RNA结合配体。为了开发RNA配体对接的探索区域,我们进行了一次嘌呤核糖开关的虚拟筛选练习,以探查RNA配体对接的优缺点。使用仅进行少量修改的标准蛋白质-配体对接程序,鉴定了四个新的配体,其结合亲和力在微摩尔范围内,包括基于分子支架的两种与已知配体不相似的化合物。 RNA-配体对接的性能与蛋白质-配体对接的性能相当,这表明该方法是探索大量RNA结构用于基于结构的配体设计的有前途的选择。

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