Discovery of a Potent and Orally Bioavailable Xanthine Oxidase/Urate Transporter 1 Dual Inhibitor as a Potential Treatment for Hyperuricemia and Gout

被引:3
作者
Yang, Xinye [1 ]
Li, Yong [1 ]
Pan, Shengqiang [1 ]
Ma, Facheng [1 ]
Chen, Hong [1 ]
Deng, Jinhui [1 ]
Yue, Jie [2 ]
Gong, Qijie [2 ]
Zheng, Mi [1 ]
Zeng, Ying [1 ]
Li, Jing [1 ]
Zhang, Yingjun [1 ]
Wang, Xiaojun [1 ]
Zhang, Xiaojin [2 ]
机构
[1] HEC Res & Dev Ctr, HEC Pharm Grp, Dongguan 523871, Peoples R China
[2] China Pharmaceut Univ, Dept Chem, Lab Drug Design & Discovery, Nanjing 211198, Peoples R China
基金
中国国家自然科学基金;
关键词
ALLOPURINOL; URATE; FEBUXOSTAT; PHARMACOKINETICS; POPULATION; MONKEYS; DRUGS;
D O I
10.1021/acs.jmedchem.4c01480
中图分类号
R914 [药物化学];
学科分类号
100701 ;
摘要
The main uric acid-lowering agents in clinical use for hyperuricemia and gout are xanthine oxidase (XO) inhibitors or urate transporter 1 (URAT1) inhibitors. While these therapies can partially control the disease, they have various limitations. The development of XO/URAT1 dual inhibitors offers the potential to enhance therapeutic potency and reduce toxicity compared with single-target inhibitors. Through scaffold hopping from the XO inhibitor febuxostat (2) and the URAT1 inhibitor probenecid (3), followed by structure-activity relationship (SAR) studies, we identified compound 27 as a potent dual inhibitor of XO and URAT1. Compound 27 demonstrated significant dual inhibition in vitro (XO IC50 = 35 nM; URAT1 IC50 = 31 nM) and exhibited favorable pharmacology and pharmacokinetic (PK) profiles in multiple species including monkeys. Furthermore, toxicity studies in rats and monkeys revealed general safety profiles, supporting that compound 27 emerges as a promising novel drug candidate with potent XO/URAT1 dual inhibition for the treatment of gout.
引用
收藏
页码:14668 / 14691
页数:24
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