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Advantages of Crystallographic Fragment Screening: Functional and Mechanistic Insights from a Powerful Platform for Efficient Drug Discovery

机译:晶体碎片筛查的优势:来自有效药物发现的强大平台的功能和机理见解

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摘要

X-ray crystallography has been an under-appreciated screening tool for fragment-based drug discovery due to the perception of low throughput and technical difficulty. Investigators in industry and academia have overcome these challenges by taking advantage of key factors that contribute to a successful crystallographic screening campaign. Efficient cocktail design and soaking methodologies have evolved to maximize throughput while minimizing false positivesegatives. In addition, technical improvements at synchrotron beamlines have dramatically increased data collection rates thus enabling screening on a timescale comparable to other techniques. The combination of available resources and efficient experimental design has resulted in many successful crystallographic screening campaigns. The three-dimensional crystal structure of the bound fragment complexed to its target, a direct result of the screening effort, enables structure-based drug design while revealing insights regarding protein dynamics and function not readily obtained through other experimental approaches. Furthermore, this “chemical interrogation” of the target protein crystals can lead to the identification of useful reagents for improving diffraction resolution or compound solubility.
机译:由于对低通量和技术难度的感知,X射线晶体学已成为基于片段药物发现的一种未被充分认识的筛选工具。工业界和学术界的研究人员通过利用有助于成功进行晶体筛查活动的关键因素,克服了这些挑战。高效的鸡尾酒设计和浸泡方法已得到发展,可以最大程度地提高通量,同时最大程度地减少假阳性/阴性。此外,同步加速器光束线的技术改进大大提高了数据收集率,因此可以在与其他技术相当的时间范围内进行筛选。可用资源和有效的实验设计的结合已导致许多成功的晶体学筛选活动。结合到其靶标上的结合片段的三维晶体结构是筛选工作的直接结果,它使得能够进行基于结构的药物设计,同时揭示了关于蛋白质动力学和功能的见解,而这些见解是其他实验方法无法轻易获得的。此外,靶蛋白晶体的这种“化学询问”可以导致鉴定用于改善衍射分辨率或化合物溶解度的有用试剂。

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