首页> 外文期刊>Journal of Medicinal Chemistry >Fragment-Guided Discovery of Pyrazole Carboxylic Acid Inhibitors of the Kelch-like ECH-Associated Protein 1: Nuclear Factor Erythroid 2 Related Factor 2 (KEAP1:NRF2) Protein-Protein Interaction
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Fragment-Guided Discovery of Pyrazole Carboxylic Acid Inhibitors of the Kelch-like ECH-Associated Protein 1: Nuclear Factor Erythroid 2 Related Factor 2 (KEAP1:NRF2) Protein-Protein Interaction

机译:片段引导发现 Kelch 样 ECH 相关蛋白 1 的吡唑羧酸抑制剂:核因子红细胞 2 相关因子 2 (KEAP1:NRF2) 蛋白-蛋白质相互作用

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摘要

The NRF2-mediated cytoprotective response is central to cellular homoeostasis, and there is increasing interest in developing small-molecule activators of this pathway as therapeutics for diseases involving chronic oxidative stress. The protein KEAP1, which regulates NRF2, is a key point for pharmacological intervention, and we recently described the use of fragment-based drug discovery to develop a tool compound that directly disrupts the protein-protein interaction between NRF2 and KEAP1. We now present the identification of a second, chemically distinct series of KEAP1 inhibitors, which provided an alternative chemotype for lead optimization. Pharmacophoric information from our original fragment screen was used to identify new hit matter through database searching and to evolve this into a new lead with high target affinity and cell-based activity. We highlight how knowledge obtained from fragment-based approaches can be used to focus additional screening campaigns in order to de-risk projects through the rapid identification of novel chemical series.
机译:NRF2介导的细胞保护反应是细胞稳态的核心,人们越来越关注开发该途径的小分子激活剂作为涉及慢性氧化应激的疾病的治疗方法。调节NRF2的蛋白质KEAP1是药物干预的关键点,我们最近描述了使用基于片段的药物发现来开发一种直接破坏NRF2和KEAP1之间蛋白质-蛋白质相互作用的工具化合物。现在,我们提出了第二个化学上不同的KEAP1抑制剂系列的鉴定,它为先导化合物优化提供了另一种化学型。来自我们原始片段筛选的药效信息用于通过数据库搜索识别新的命中物质,并将其演变为具有高靶标亲和力和基于细胞活性的新先导化合物。我们重点介绍了如何利用从基于片段的方法中获得的知识来集中精力进行额外的筛选活动,以便通过快速识别新的化学系列来降低项目的风险。
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