Structure-Based Lead Optimization of Enterovirus D68 2A Protease Inhibitors

被引:3
作者
Tan, Bin [1 ]
Liu, Chang [2 ,3 ]
Li, Kan [1 ]
Jadhav, Prakash [1 ]
Lambrinidis, George [4 ]
Zhu, Lan [5 ,6 ]
Olson, Linda [5 ,6 ]
Tan, Haozhou [1 ]
Wen, Yu [1 ]
Kolocouris, Antonios [4 ]
Liu, Wei [5 ,6 ]
Wang, Jun [1 ]
机构
[1] State Univ New Jersey, Ernest Mario Sch Pharm, Dept Med Chem, Piscataway, NJ 08854 USA
[2] Arizona State Univ, Biodesign Inst, Sch Mol Sci, Tempe, AZ 85287 USA
[3] Arizona State Univ, Biodesign Inst, Biodesign Ctr Appl Struct Discovery, Tempe, AZ 85287 USA
[4] Natl & Kapodistrian Univ Athens, Div Pharmaceut Chem, Lab Med Chem, Dept Pharm,Sch Hlth Sci, Athens 15771, Greece
[5] Med Coll Wisconsin, Canc Ctr, Milwaukee, WI 53226 USA
[6] Med Coll Wisconsin, Dept Pharmacol & Toxicol, Milwaukee, WI 53226 USA
基金
美国国家卫生研究院;
关键词
ACUTE FLACCID MYELITIS; PARTICLE MESH EWALD; FORCE-FIELD; RESPIRATORY ILLNESS; RESISTANCE; OUTBREAK; DESIGN;
D O I
10.1021/acs.jmedchem.3c00995
中图分类号
R914 [药物化学];
学科分类号
100701 ;
摘要
Enterovirus D68 (EV-D68) virus is a nonpolio enterovirus that typically causes respiratory illness and, in severe cases, can lead to paralysis and death in children. There is currently no vaccine or antiviral for EV-D68. We previously discovered the viral 2A protease (2A(pro)) as a viable antiviral drug target and identified telaprevir as a 2A(pro) inhibitor. 2A(pro) is a viral cysteine protease that cleaves the viral VP1-2A polyprotein junction. In this study, we report the X-ray crystal structures of EV-D68 2A(pro), wild-type, and the C107A mutant and the structure-based lead optimization of telaprevir. Guided by the X-ray crystal structure, we predicted the binding pose of telaprevir in 2A(pro) using molecular dynamics simulations. We then utilized this model to inform structure-based optimization of the telaprevir's reactive warhead and P1-P4 substitutions. These efforts led to the discovery of 2A(pro) inhibitors with improved antiviral activity than telaprevir. These compounds represent promising lead compounds for further development as EV-D68 antivirals.
引用
收藏
页码:14544 / 14563
页数:20
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