Abstract
Noroviruses are the major cause of human epidemic nonbacterial gastroenteritis. Viral replication requires a 3C cysteine protease that cleaves a 200 kDa viral polyprotein into its constituent functional proteins. Here we describe the X-ray structure of the Southampton norovirus 3C protease (SV3CP) bound to an active site-directed peptide inhibitor (MAPI) which has been refined at 1.7 Å resolution. The inhibitor, acetyl-Glu-Phe-Gln-Leu-Gln-X, which is based on the most rapidly cleaved recognition sequence in the 200 kDa polyprotein substrate, reacts covalently through its propenyl ethyl ester group (X) with the active site nucleophile, Cys 139. The structure permits, for the first time, the identification of substrate recognition and binding groups in a noroviral 3C protease and thus provides important new information for the development of antiviral prophylactics.
Publication types
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Research Support, Non-U.S. Gov't
MeSH terms
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3C Viral Proteases
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Amino Acid Sequence
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Antiviral Agents / chemistry
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Antiviral Agents / pharmacology*
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Caliciviridae Infections / drug therapy
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Caliciviridae Infections / enzymology
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Catalytic Domain / drug effects
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Crystallography, X-Ray
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Cysteine Endopeptidases / chemistry*
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Cysteine Endopeptidases / metabolism
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Humans
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Models, Molecular
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Molecular Sequence Data
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Norovirus / chemistry
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Norovirus / drug effects
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Norovirus / enzymology*
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Peptides / chemistry
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Peptides / pharmacology*
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Protease Inhibitors / chemistry
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Protease Inhibitors / pharmacology*
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Protein Structure, Tertiary
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Sequence Alignment
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Substrate Specificity
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Viral Proteins / antagonists & inhibitors*
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Viral Proteins / chemistry*
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Viral Proteins / metabolism
Substances
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Antiviral Agents
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Peptides
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Protease Inhibitors
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Viral Proteins
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Cysteine Endopeptidases
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3C Viral Proteases