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Design Principles for Fragment Libraries: Maximizing the Value of Learnings from Pharma Fragment-Based Drug Discovery (FBDD) Programs for Use in Academia

机译:碎片图书馆的设计原则:最大限度地提高在学术界使用的基于药物碎片的药物发现(FBDD)程序的学习价值

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摘要

Fragment-based drug discovery (FBDD) is well suited for discovering both drug leads and chemical probes of protein function; it can cover broad swaths of chemical space and allows the use of creative chemistry. FBDD is widely implemented for lead discovery in industry but is sometimes. used less systematically in academia. Design principles and implementation approaches for fragment libraries are continually evolving, and the lack of up-to-date guidance may prevent more effective application of FBDD in academia. This Perspective explores many of the theoretical, practical, and strategic considerations that occur within FBDD programs, including the optimal size, complexity, physicochemical profile, and shape profile of fragments in FBDD libraries, as well as compound storage, evaluation; and screening technologies. This:compilation of industry experience in FBDD will hopefully be useful for those pursuing FBDD in academia.
机译:基于片段的药物发现(FBDD)非常适合发现药物前导和蛋白质功能的化学探针。它可以覆盖广泛的化学空间,并允许使用创造性的化学。 FBDD已广泛用于在行业中发现潜在客户,但有时是。在学术界较少系统地使用。片段库的设计原理和实现方法不断发展,缺少最新指南可能会阻止FBDD在学术界更有效地应用。本观点探讨了FBDD程序中发生的许多理论,实践和战略考虑,包括FBDD库中片段的最佳大小,复杂性,理化特征和形状特征,以及化合物的存储,评估;和筛选技术。 FBDD行业经验的汇编对于希望在学术界追求FBDD的人们将是有用的。

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