Inhibitor of the non-structural protein 2 protease shows promising efficacy in mouse models of chikungunya

被引:0
作者
Metibemu, Damilohun S. [1 ]
Adeyinka, Olawale S. [1 ]
Falode, John [1 ]
Hampton, Tamia [1 ]
Crown, Olamide [1 ]
Ojobor, J. Chinenye [1 ]
Narayanan, Aarthi [2 ]
Julander, Justin [3 ,4 ]
Ogungbe, Ifedayo Victor [1 ]
机构
[1] Univ Alabama, Coll Sci, Chem & Biotechnol Sci & Engn Program, Huntsville, AL 35899 USA
[2] George Mason Univ, Coll Sci, Dept Biol, Fairfax, VA 22030 USA
[3] Utah State Univ, Inst Antiviral Res, Logan, UT 84322 USA
[4] Utah State Univ, Dept Anim Dairy & Vet Sci, Logan, UT 84322 USA
基金
美国国家卫生研究院;
关键词
Chikungunya; Non-structural protein; nsP2; protease; Vinyl sulfone; CHIKV; Covalent inhibitors; IN-VITRO;
D O I
10.1016/j.ejmech.2024.116808
中图分类号
R914 [药物化学];
学科分类号
100701 ;
摘要
Chikungunya virus (CHIKV) is responsible for the most endemic alphavirus infections called Chikungunya. The endemicity of Chikungunya has increased over the past two decades, and it is a pathogen with pandemic potential. There is currently no approved direct-acting antiviral to treat the disease. As part of our antiviral drug discovery program focused on alphaviruses and the non-structural protein 2 protease, we discovered that J12 and J13 can inhibit CHIKV nsP2 protease and block the replication of CHIKV in cell cultures. Both compounds are metabolically stable to human liver microsomal and S9 enzymes. J13 has excellent oral bioavailability in pharmacokinetics studies in mice and ameliorated Chikungunya symptoms in preliminary efficacy studies in mice. J13 exhibited an excellent safety profile in in vitro safety pharmacology and off-target screening assays, making J13 and its analogs good candidates for drug development against Chikungunya.
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页数:9
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