Broad-Spectrum Antivirals against 3C or 3C-Like Proteases of Picornaviruses, Noroviruses, and Coronaviruses

被引:255
|
作者
Kim, Yunjeong [1 ]
Lovell, Scott [2 ]
Tiew, Kok-Chuan [3 ]
Mandadapu, Sivakoteswara Rao [3 ]
Alliston, Kevin R. [3 ]
Battaile, Kevin P. [4 ]
Groutas, William C. [3 ]
Chang, Kyeong-Ok [1 ]
机构
[1] Kansas State Univ, Coll Vet Med, Dept Diagnost Med & Pathobiol, Manhattan, KS 66506 USA
[2] Univ Kansas, Del Shankel Struct Biol Ctr, Prot Struct Lab, Lawrence, KS 66045 USA
[3] Wichita State Univ, Dept Chem, Wichita, KS 67208 USA
[4] IMCA CAT Hauptman Woodward Med Res Inst, Argonne, IL USA
关键词
STRUCTURE-BASED DESIGN; BIOLOGICAL EVALUATION; CRYSTAL-STRUCTURE; BINDING SITE; ACTIVE-SITE; INHIBITORS; PROTEINASE; EXPRESSION; REVEALS; ASSAY;
D O I
10.1128/JVI.01348-12
中图分类号
Q93 [微生物学];
学科分类号
071005 ; 100705 ;
摘要
Phylogenetic analysis has demonstrated that some positive-sense RNA viruses can be classified into the picornavirus-like supercluster, which includes picornaviruses, caliciviruses, and coronaviruses. These viruses possess 3C or 3C-like proteases (3Cpro or 3CLpro, respectively), which contain a typical chymotrypsin-like fold and a catalytic triad (or dyad) with a Cys residue as a nucleophile. The conserved key sites of 3Cpro or 3CLpro may serve as attractive targets for the design of broad-spectrum antivirals for multiple viruses in the supercluster. We previously reported the structure-based design and synthesis of potent protease inhibitors of Norwalk virus (NV), a member of the Caliciviridae family. We report herein the broad-spectrum antiviral activities of three compounds possessing a common dipeptidyl residue with different warheads, i.e., an aldehyde (GC373), a bisulfite adduct (GC376), and an alpha-ketoamide (GC375), against viruses that belong to the supercluster. All compounds were highly effective against the majority of tested viruses, with half-maximal inhibitory concentrations in the high nanomolar or low micromolar range in enzyme-and/ or cell-based assays and with high therapeutic indices. We also report the high-resolution X-ray cocrystal structures of NV 3CLpro-, poliovirus 3Cpro-, and transmissible gastroenteritis virus 3CLpro-GC376 inhibitor complexes, which show the compound covalently bound to a nucleophilic Cys residue in the catalytic site of the corresponding protease. We conclude that these compounds have the potential to be developed as antiviral therapeutics aimed at a single virus or multiple viruses in the picornavirus-like supercluster by targeting 3Cpro or 3CLpro.
引用
收藏
页码:11754 / 11762
页数:9
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