Prospective Characterization of Full-Length Hepatitis C Virus NS5A Quasispecies during Induction and Combination Antiviral Therapy

doi:10.1128/JVI.74.19.9028-9038.2000

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Journal of Virology, October 2000, p. 9028-9038, Vol. 74, No. 19
0022-538X/00/$04.00+0
Copyright © 2000, American Society for Microbiology. All rights reserved.

Prospective Characterization of Full-Length Hepatitis C Virus NS5A Quasispecies during Induction and Combination Antiviral Therapy

J.-B. Nousbaum,¹^, S. J. Polyak,¹^,^* S. C. Ray,² D. G. Sullivan,¹ A. M. Larson,³ R. L. Carithers Jr.,³ and D. R. Gretch¹^,³

Departments of Laboratory Medicine¹ and Medicine,³ University of Washington, Seattle, Washington, and Department of Medicine, Johns Hopkins University School of Medicine, Baltimore, Maryland²

Received 23 March 2000/Accepted 13 July 2000

The hepatitis C virus (HCV) nonstructural 5A (NS5A) protein has been controversially implicated in the inherent resistanceof HCV to interferon (IFN) antiviral therapy in clinical studies.In this study, the relationship between NS5A mutations and selectionpressures before and during antiviral therapy and virologic responseto therapy were investigated. Full-length NS5A clones were sequencedfrom 20 HCV genotype 1-infected patients in a prospective, randomizedclinical trial of IFN induction (daily) therapy and IFN plus ribavirincombination therapy. Pretreatment NS5A nucleotide and amino acidphylogenies did not correlate with clinical IFN responses anddomains involved in NS5A functions in vitro were all well conservedbefore and during treatment. A consensus IFN sensitivity-determiningregion (ISDR_237-276) sequence associated with IFN resistancewas not found, although the presence of Ala₂₄₅ within the ISDRwas associated with nonresponse to treatment in genotype 1a-infectedpatients (P < 0.01). There were more mutations in the 26 aminoacids downstream of the ISDR required for PKR binding in pretreatmentisolates from responders versus nonresponders in both HCV-1a-and HCV-1b-infected patients (P < 0.05). In HCV-1a patients, moreamino acid changes were observed in isolates from IFN-sensitivepatients (P < 0.001), and the mutations appeared to be concentratedin two variable regions in the C terminus of NS5A, that correspondedto the previously described V3 region and a new variable region,310 to 330. Selection of pretreatment minor V3 quasispecies wasobserved within the first 2 to 6 weeks of therapy in respondersbut not nonresponders, whereas the ISDR and PKR binding domainsdid not change in either patient response group. These data suggestthat host-mediated selective pressures act primarily on the Cterminus of NS5A and that NS5A can perturb or evade the IFN-inducedantiviral response using sequences outside of the putative ISDR.Mechanistic studies are needed to address the role of the C terminusof NS5A in HCV replication and antiviralresistance.

^* Corresponding author. Mailing address: University of Washington, Box 359690, 325 9th Ave., Seattle, WA 98104-2499. Phone:(206) 341-5224. Fax: (206) 341-5203. E-mail: polyak{at}u.washington.edu.

Present address: Department of Hepato-Gastroenterology, University of Brest, Brest,France.

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