Design, synthesis, and evaluation of BTK-targeting PROTACs with optimized bioavailability in vitro and in vivo

Yonghui Sun; Zimo Yang; Zhimin Zhang; Zhen Li; Liubin Guo; Hao Pan; Xin Luo; Dongzhou Liu; Yu Rao

doi:10.1039/d3md00216k

Design, synthesis, and evaluation of BTK-targeting PROTACs with optimized bioavailability in vitro and in vivo

RSC Med Chem. 2023 Jun 21;14(8):1562-1566. doi: 10.1039/d3md00216k. eCollection 2023 Aug 16.

Authors

Yonghui Sun¹, Zimo Yang¹, Zhimin Zhang², Zhen Li¹, Liubin Guo², Hao Pan², Xin Luo¹, Dongzhou Liu², Yu Rao¹

Affiliations

¹ MOE Key Laboratory of Protein Sciences, School of Pharmaceutical Sciences, MOE Key Laboratory of Bioorganic Phosphorus Chemistry & Chemical Biology, Tsinghua University Beijing 100084 China yrao@tsinghua.edu.cn.
² Global Drug Development Center, Huadong Medicine Co., Ltd No. 866 Mogan Mountain Road Hangzhou 310011 China jefferydliu@eastchinapharm.com.

PMID: 37593574
PMCID: PMC10429852 (available on 2024-06-21)
DOI: 10.1039/d3md00216k

Abstract

Ibrutinib is a first-line drug for the treatment of B-cell malignancies. BTK^C481S mutation has led to drug resistance during clinical application. Herein, a novel BTK-targeting PROTAC molecule with better solubility and bioavailability was developed. Compound 15-271 has better solubility than ibrutinib and some reported BTK PROTACs. 15-271 has better liver microsomal stability than its analogues in multiple species. More importantly, 15-271 has a longer half-life and better bioavailability in vivo. The development strategy of compound 15-271 can be a general procedure for the optimization of other PROTACs.