Discovery of benzoheterocyclic-substituted amide derivatives as apoptosis signal-regulating kinase 1 (ASK1) inhibitors

Lin Tang; Minxiong Li; Changlin Bai; Xuejin Feng; Haiyang Hu; Yufen Yao; Baiqing Li; Hongwei Li; Guohong Qin; Ning Xi; Genpin Lv; Lei Zhang

doi:10.1039/d3md00663h

Discovery of benzoheterocyclic-substituted amide derivatives as apoptosis signal-regulating kinase 1 (ASK1) inhibitors

RSC Med Chem. 2024 Jan 30;15(3):856-873. doi: 10.1039/d3md00663h. eCollection 2024 Mar 20.

Authors

Lin Tang^{1

2

3}, Minxiong Li², Changlin Bai², Xuejin Feng², Haiyang Hu², Yufen Yao⁴, Baiqing Li⁵, Hongwei Li⁶, Guohong Qin⁶, Ning Xi⁷, Genpin Lv³, Lei Zhang¹

Affiliations

¹ MOE International Joint Research Laboratory on Synthetic Biology and Medicines, School of Biology and Biological Engineering, South China University of Technology Guangzhou 510006 P.R. China lzhangce@scut.edu.cn.
² Sunshine Lake Pharmaceutical Co., Ltd. Dongguan 523871 P.R. China.
³ Shaoguan HEC Technology R & D Co., Ltd Shaoguan 512000 P.R. China dyglee@163.com.
⁴ Guangdong Provincial Key Laboratory of New Drug Design and Evaluation, School of Pharmaceutical Sciences, Sun Yat-Sen University 510006 Guangzhou P.R. China.
⁵ Guangzhou National Laboratory Guangzhou 510005 P.R. China.
⁶ Guangdong Yuchuang Electronics Co., Ltd. Shaoguan 512721 P.R. China.
⁷ Institute of Drug Discovery Technology, Ningbo University Ningbo 315211 P.R. China xining@nbu.edu.cn.

PMID: 38516590
PMCID: PMC10953477 (available on 2025-01-30)
DOI: 10.1039/d3md00663h

Abstract

Three series of benzoheterocyclic-substituted amide derivatives were designed and synthesized as potent ASK1 inhibitors in this work. After undergoing continuous structural optimization, compound 17a was discovered to be a novel inhibitor of ASK1 with good potency (kinase, IC₅₀ = 26 nM), noteworthy liver microsomal stability (human, T_1/2 = 340.4 min), good pharmacokinetic parameters (rat, T_1/2 p.o. = 2.11 h, AUC_last p.o. = 10 900 h ng mL^-1) and high oral bioavailability (rat, F = 97.9%), while also being inactive towards hERG (IC₅₀ > 10 μM).