Cereblon调节药物的物理化学性质决定药代动力学和处置情况。
Physicochemistry of Cereblon Modulating Drugs Determines Pharmacokinetics and Disposition.
作者信息
Kong Nikki R, Liu Hu, Che Jianwei, Jones Lyn H
机构信息
Center for Protein Degradation, Dana-Farber Cancer Institute, 360 Longwood Avenue, Boston, Massachusetts 02215, United States.
出版信息
ACS Med Chem Lett. 2021 Oct 8;12(11):1861-1865. doi: 10.1021/acsmedchemlett.1c00475. eCollection 2021 Nov 11.
Abstract
Immunomodulatory drugs (IMiDs) thalidomide, lenalidomide, and pomalidomide engage cereblon and mediate a protein interface with neosubstrates such as zinc finger transcription factors promoting their polyubiquitination and degradation. The IMiDs have garnered considerable excitement in drug discovery, leading to exploration of targeted protein degradation strategies. Although the molecular modes-of-action of the IMiDs and related degraders have been the subject of intense research, their pharmacokinetics and disposition have been relatively understudied. Here, we assess the effects of physicochemistry of the IMiDs, the phthalimide EM-12, and the candidate drug CC-220 (iberdomide) on lipophilicity, solubility, metabolism, permeability, intracellular bioavailability, and cell-based potency. The insights yielded in this study will enable the rational property-based design and development of targeted protein degraders in the future.
摘要
免疫调节药物(IMiDs)沙利度胺、来那度胺和泊马度胺与脑啡肽结合,并介导与锌指转录因子等新底物的蛋白质相互作用,促进它们的多聚泛素化和降解。IMiDs在药物研发中引起了极大的关注,促使人们探索靶向蛋白质降解策略。尽管IMiDs及相关降解剂的分子作用模式一直是深入研究的课题,但其药代动力学和处置情况相对研究较少。在此,我们评估了IMiDs、邻苯二甲酰亚胺EM-12和候选药物CC-220(伊布度胺)的物理化学性质对亲脂性、溶解度、代谢、渗透性、细胞内生物利用度和基于细胞的效力的影响。本研究获得的见解将有助于未来基于性质的合理设计和开发靶向蛋白质降解剂。
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