Issue 8, 2023
From the journal:

RSC Medicinal Chemistry

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

Yonghui Sun, ORCID logo a   Zimo Yang, ORCID logo a   Zhimin Zhang,b   Zhen Li,a   Liubin Guo,b   Hao Pan,b   Xin Luo,a   Dongzhou Liu*b  and  Yu Rao ORCID logo *a  

* Corresponding authors

a MOE Key Laboratory of Protein Sciences, School of Pharmaceutical Sciences, MOE Key Laboratory of Bioorganic Phosphorus Chemistry & Chemical Biology, Tsinghua University, Beijing 100084, China
E-mail: yrao@tsinghua.edu.cn

b Global Drug Development Center, Huadong Medicine Co., Ltd, No. 866 Mogan Mountain Road, Hangzhou 310011, China
E-mail: jefferydliu@eastchinapharm.com

Abstract

Ibrutinib is a first-line drug for the treatment of B-cell malignancies. BTKC481S 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.

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

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Article information

DOI
https://doi.org/10.1039/D3MD00216K
Article type
Research Article
Submitted
10 May 2023
Accepted
14 Jun 2023
First published
21 Jun 2023

RSC Med. Chem., 2023,14, 1562-1566

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

Y. Sun, Z. Yang, Z. Zhang, Z. Li, L. Guo, H. Pan, X. Luo, D. Liu and Y. Rao, RSC Med. Chem., 2023, 14, 1562 DOI: 10.1039/D3MD00216K

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