高效合成免疫调节药物类似物可实现结构降解关系的探索。
Efficient Synthesis of Immunomodulatory Drug Analogues Enables Exploration of Structure-Degradation Relationships.
机构信息
Department of Molecular, Cellular and Developmental Biology, Yale University, 219 Prospect Street, New Haven, CT, 06520-8103, USA.
Arvinas LLC, 5 Science Park, 395 Winchester Avenue, New Haven, CT, 06511, USA.
出版信息
ChemMedChem. 2018 Aug 10;13(15):1508-1512. doi: 10.1002/cmdc.201800271. Epub 2018 Jul 4.
Abstract
The immunomodulatory drugs (IMiDs) thalidomide, pomalidomide, and lenalidomide have been approved for the treatment of multiple myeloma for many years. Recently, their use as E3 ligase recruiting elements for small-molecule-induced protein degradation has led to a resurgence in interest in IMiD synthesis and functionalization. Traditional IMiD synthesis follows a stepwise route with multiple purification steps. Herein we describe a novel one-pot synthesis without purification that provides rapid access to a multitude of IMiD analogues. Binding studies with the IMiD target protein cereblon (CRBN) reveals a narrow structure-activity relationship with only a few compounds showing sub-micromolar binding affinity in the range of pomalidomide and lenalidomide. However, anti-proliferative activity as well as Aiolos degradation could be identified for two IMiD analogues. This study provides useful insight into the structure-degradation relationships for molecules of this type as well as a rapid and robust method for IMiD synthesis.
摘要
免疫调节药物(IMiDs)沙利度胺、泊马度胺和来那度胺已被批准用于治疗多发性骨髓瘤多年。最近,它们作为 E3 连接酶招募小分子诱导蛋白降解的元件,重新引起了对 IMiD 合成和功能化的兴趣。传统的 IMiD 合成采用分步路线,需要经过多个纯化步骤。在此,我们描述了一种无需纯化的新型一锅合成方法,可快速获得多种 IMiD 类似物。与 IMiD 靶蛋白 cereblon(CRBN)的结合研究表明,结构-活性关系很窄,只有少数化合物在泊马度胺和来那度胺的范围内显示出亚微摩尔的结合亲和力。然而,两种 IMiD 类似物都能表现出抗增殖活性和 Aiolos 降解。这项研究为这类分子的结构-降解关系提供了有用的见解,以及一种快速而稳健的 IMiD 合成方法。
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