Virus-Specific Cofactor Requirement and Chimeric Hepatitis C Virus/GB Virus B Nonstructural Protein 3

doi:10.1128/JVI.74.9.4291-4301.2000

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Journal of Virology, May 2000, p. 4291-4301, Vol. 74, No. 9
0022-538X/00/$04.00+0
Copyright © 2000, American Society for Microbiology. All rights reserved.

Virus-Specific Cofactor Requirement and Chimeric Hepatitis C Virus/GB Virus B Nonstructural Protein 3

Nancy Butkiewicz,¹ Nanhua Yao,² Weidong Zhong,¹ Jacquelyn Wright-Minogue,¹ Paul Ingravallo,¹ Rumin Zhang,² James Durkin,² David N. Standring,¹ Bahige M. Baroudy,¹ David V. Sangar,³ Stanley M. Lemon,³ Johnson Y. N. Lau,¹ and Zhi Hong¹^,^*

Departments of Antiviral Therapy¹ and Structural Chemistry,² Schering-Plough Research Institute, Kenilworth, New Jersey 07033-0539, and Department of Microbiology and Immunology, The University of Texas Medical Branch at Galveston, Galveston, Texas 77555-1019³

Received 22 November 1999/Accepted 22 January 2000

GB virus B (GBV-B) is closely related to hepatitis C virus (HCV) and causes acute hepatitis in tamarins (Saguinus species),making it an attractive surrogate virus for in vivo testing ofanti-HCV inhibitors in a small monkey model. It has been reportedthat the nonstructural protein 3 (NS3) serine protease of GBV-Bshares similar substrate specificity with its counterpart in HCV.Authentic proteolytic processing of the HCV polyprotein junctions(NS4A/4B, NS4B/5A, and NS5A/5B) can be accomplished by the GBV-BNS3 protease in an HCV NS4A cofactor-independent fashion. We furthercharacterized the protease activity of a full-length GBV-B NS3protein and its cofactor requirement using in vitro-translatedGBV-B substrates. Cleavages at the NS4A/4B and NS5A/5B junctionswere readily detectable only in the presence of a cofactor peptidederived from the central region of GBV-B NS4A. Interestingly,the GBV-B substrates could also be cleaved by the HCV NS3 proteasein an HCV NS4A cofactor-dependent manner, supporting the notionthat HCV and GBV-B share similar NS3 protease specificity whileretaining a virus-specific cofactor requirement. This findingof a strict virus-specific cofactor requirement is consistentwith the lack of sequence homology in the NS4A cofactor regionsof HCV and GBV-B. The minimum cofactor region that supported GBV-Bprotease activity was mapped to a central region of GBV-B NS4A(between amino acids Phe22 and Val36) which overlapped with thecofactor region of HCV. Alanine substitution analysis demonstratedthat two amino acids, Val27 and Trp31, were essential for thecofactor activity, a finding reminiscent of the two critical residuesin the HCV NS4A cofactor, Ile25 and Ile29. A model for the GBV-BNS3 protease domain and NS4A cofactor complex revealed that GBV-Bmight have developed a similar structural strategy in the activationand regulation of its NS3 protease activity. Finally, a chimericHCV/GBV-B bifunctional NS3, consisting of an N-terminal HCV proteasedomain and a C-terminal GBV-B RNA helicase domain, was engineered.Both enzymatic activities were retained by the chimeric protein,which could lead to the development of a chimeric GBV-B virusthat depends on HCV proteasefunction.

^* Corresponding author. Mailing address: Antiviral Therapy, K-15-4/4945, Schering-Plough Research Institute, 2015 GallopingHill Rd., Kenilworth, NJ 07033-0539. Phone: (908) 740-3152. Fax:(908) 740-3918. E-mail: zhi.hong{at}spcorp.com.

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