Jean Quancard, Anders Bach, Chiara Borsari, Russell Craft, Christian Gnamm, Stéphanie M. Guéret, Ingo V. Hartung, Hannes F. Koolman, Stefan Laufer, Susan Lepri, Josef Messinger, Kurt Ritter, Gianluca Sbardella, Andrea Unzue Lopez, Marina K. Willwacher, Brian Cox, Robert J. Young
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引用次数: 0
Abstract
The Hit to Lead (H2L) process is an integral part of contemporary drug discovery, encompassing the optimisation of validated Hit structures into Lead molecules. High quality leads build confidence, through activity and property profiles as well as preliminary biological data, which might include validating pharmacologic hypotheses along the way, indicating that further investment in the structure(s) and target would be worthwhile. Leads have line of sight to a development candidate and bring an understanding of what priorities Lead Optimisation should address. In this set of best practices, we detail the essential criteria that characterise a good lead, which include establishing SAR from analogues and assessing preliminary DMPK indicators, selectivity and early safety parameters. We highlight the importance of identifying liabilities of the lead series and demonstrating that each can be individually modulated whilst maintaining on target potency. We make the case for having physicochemical properties as critical optimisation parameters and how ligand efficiency metrics can enable this. Then we go over general tactics that can be used to convert hits into a lead series. These include essential steps that, when performed early, increase the chance of success such as deconstructive SAR, pharmacophore and bioactive conformation determination and scaffold optimisation. Finally, we suggest decision-making criteria to substantiate confidence in further investment or, as importantly, making a recommendation to cease further work on a series.
Hit to Lead (H2L)过程是当代药物发现的一个组成部分,包括优化验证Hit结构到铅分子。高质量的线索可以建立信心,通过活动和属性概况以及初步的生物学数据,其中可能包括在此过程中验证药理学假设,表明对结构和目标的进一步投资是值得的。潜在客户可以看到开发候选人,并了解潜在客户优化应该解决的优先事项。在这组最佳实践中,我们详细介绍了表征良好引线的基本标准,包括从类似物中建立SAR,评估初步DMPK指标,选择性和早期安全性参数。我们强调识别导联系列的责任的重要性,并证明每个导联系列都可以单独调节,同时保持目标效力。我们提出了将物理化学性质作为关键优化参数的案例,以及配体效率指标如何实现这一点。然后我们将讨论将热门游戏转化为领先系列游戏的一般策略。这些包括必要的步骤,如果及早进行,可以增加成功的机会,例如解构SAR,药效团和生物活性构象确定以及支架优化。最后,我们建议制定决策标准,以证实对进一步投资的信心,或者同样重要的是,建议停止对一系列的进一步工作。
期刊介绍:
Quality research. Outstanding publications. With an impact factor of 3.124 (2019), ChemMedChem is a top journal for research at the interface of chemistry, biology and medicine. It is published on behalf of Chemistry Europe, an association of 16 European chemical societies.
ChemMedChem publishes primary as well as critical secondary and tertiary information from authors across and for the world. Its mission is to integrate the wide and flourishing field of medicinal and pharmaceutical sciences, ranging from drug design and discovery to drug development and delivery, from molecular modeling to combinatorial chemistry, from target validation to lead generation and ADMET studies. ChemMedChem typically covers topics on small molecules, therapeutic macromolecules, peptides, peptidomimetics, and aptamers, protein-drug conjugates, nucleic acid therapies, and beginning 2017, nanomedicine, particularly 1) targeted nanodelivery, 2) theranostic nanoparticles, and 3) nanodrugs.
Contents
ChemMedChem publishes an attractive mixture of:
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