Kinetic and structural analyses of hepatitis C virus polyprotein processing.

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J Virol. 1994 August; 68(8): 5045-5055

Kinetic and structural analyses of hepatitis C virus polyprotein processing.

R Bartenschlager, L Ahlborn-Laake, J Mous and H Jacobsen

F. Hoffmann-La Roche Ltd., Basel, Switzerland.

ABSTRACT

Recombinant vaccinia viruses were used to study the processingof hepatitis C virus (HCV) nonstructural polyprotein precursor.HCV-specific proteins and cleavage products were identifiedby size and by immunoprecipitation with region-specific antisera.A polyprotein beginning with 20 amino acids derived from thecarboxy terminus of NS2 and ending with the NS5B stop codon(amino acids 1007 to 3011) was cleaved at the NS3/4A, NS4A/4B,NS4B/5A, and NS5A/5B sites, whereas a polyprotein in which theputative active site serine residue was replaced by an alanineremained unprocessed, demonstrating that the NS3-encoded serine-typeproteinase is essential for cleavage at these sites. Processingof the NS3'-5B polyprotein was complex and occurred rapidly.Discrete polypeptide species corresponding to various processingintermediates were detected. With the exception of NS4AB-5A/NS5A,no clear precursor-product relationships were detected. Usingdouble infection of cells with vaccinia virus recombinants expressingeither a proteolytically inactive NS3'-5B polyprotein or anactive NS3 proteinase, we found that cleavage at the NS4A/4B,NS4B/5A, and NS5A/5B sites could be mediated in trans. Absenceof trans cleavage at the NS3/4A junction together with the findingthat processing at this site was insensitive to dilution ofthe enzyme suggested that cleavage at this site is an intramolecularreaction. The trans-cleavage assay was also used to show that(i) the first 211 amino acids of NS3 were sufficient for processingat all trans sites and (ii) small deletions from the amino terminusof NS3 selectively affected cleavage at the NS4B/5A site, whereasmore extensive deletions also decreased processing efficienciesat the other sites. Using a series of amino-terminally truncatedsubstrate polyproteins in the trans-cleavage assay, we foundthat NS4A is essential for cleavage at the NS4B/5A site andthat processing at this site could be restored by NS4A providedin cis (i.e., together with the substrate) or in trans (i.e.,together with the proteinase). These results suggest that inaddition to the NS3 proteinase, NS4A sequences play an importantrole in HCV polyprotein processing.

J Virol. 1994 August; 68(8): 5045-5055

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