DCAF16-Based Covalent Handle for the Rational Design of Monovalent Degraders

合理设计 计算机科学 化学 生化工程 纳米技术 材料科学 工程类
作者
Melissa Lim,Thang Do Cong,Lauren M. Orr,Ethan S. Toriki,Andrew C. Kile,James W. Papatzimas,Elijah Lee,Yihan Lin,Daniel K. Nomura
出处
期刊:ACS central science [American Chemical Society]
卷期号:10 (7): 1318-1331 被引量:86
标识
DOI:10.1021/acscentsci.4c00286
摘要

Targeted protein degradation with monovalent molecular glue degraders is a powerful therapeutic modality for eliminating disease causing proteins. However, rational design of molecular glue degraders remains challenging. In this study, we sought to identify a transplantable and linker-less covalent handle that could be appended onto the exit vector of various protein-targeting ligands to induce the degradation of their respective targets. Using the BET family inhibitor JQ1 as a testbed, we synthesized and screened a series of covalent JQ1 analogs and identified a vinylsulfonyl piperazine handle that led to the potent and selective degradation of BRD4 in cells. Through chemoproteomic profiling, we identified DCAF16 as the E3 ligase responsible for BRD4 degradation-an E3 ligase substrate receptor that has been previously covalently targeted for molecular glue-based degradation of BRD4. Interestingly, we demonstrated that this covalent handle can be transplanted across a diverse array of protein-targeting ligands spanning many different protein classes to induce the degradation of CDK4, the androgen receptor, BTK, SMARCA2/4, and BCR-ABL/c-ABL. Our study reveals a DCAF16-based covalent degradative and linker-less chemical handle that can be attached to protein-targeting ligands to induce the degradation of several different classes of protein targets.
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