吡咯烷类β-分泌酶抑制剂的发现：通过构象设计保持配体结合效率来推进先导化合物优化。

Discovery of pyrrolidine-based β-secretase inhibitors: lead advancement through conformational design for maintenance of ligand binding efficiency.

机构信息

Department of Medicinal Chemistry, Merck Research Laboratories, Merck & Co., PO Box 4, West Point, PA 19486, USA.

出版信息

Bioorg Med Chem Lett. 2012 Jan 1;22(1):240-4. doi: 10.1016/j.bmcl.2011.11.024. Epub 2011 Nov 12.

DOI:10.1016/j.bmcl.2011.11.024

Abstract

We have developed a novel series of pyrrolidine derived BACE-1 inhibitors. The potency of the weak initial lead structure was enhanced using library-based SAR methods. The series was then further advanced by rational design while maintaining a minimal ligand binding efficiency threshold. Ultimately, the co-crystal structure was obtained revealing that these inhibitors interacted with the enzyme in a unique fashion. In all, the potency of the series was enhanced by 4 orders of magnitude from the HTS lead with concomitant increases in physical properties needed for series advancement. The progression of these developments in a systematic fashion is described.

摘要

我们开发了一系列新型吡咯烷衍生的 BACE-1 抑制剂。采用基于文库的 SAR 方法提高了弱初始先导结构的活性。然后，通过合理设计进一步推进该系列，同时保持最小的配体结合效率阈值。最终，获得了共晶结构，揭示了这些抑制剂以独特的方式与酶相互作用。总之，该系列的活性比 HTS 先导化合物提高了 4 个数量级，同时也提高了系列推进所需的物理性质。系统地描述了这些进展。

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吡咯烷类β-分泌酶抑制剂的发现：通过构象设计保持配体结合效率来推进先导化合物优化。

Discovery of pyrrolidine-based β-secretase inhibitors: lead advancement through conformational design for maintenance of ligand binding efficiency.

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