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Interferon and ribavirin therapy does not select for resistance mutations in hepatitis C virus polymerase

Ribavirin has a minor and transient effect on hepatitis C virus (HCV) replication and has been suggested to select a novel mutation, F415Y, in the RNA‐dependent RNA polymerase of subtype 1a viruses. Twenty‐nine patients with chronic hepatitis C (subtyped by INNO LiPA as 1a, 17; 1b, 11; 1a/1b, 1) who...

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Published in:Journal of viral hepatitis 2008-08, Vol.15 (8), p.571-577
Main Authors: Ward, C. L., Dev, A., Rigby, S., Symonds, W. T., Patel, K., Zekry, A., Pawlotsky, J.-M., McHutchison, J. G.
Format: Article
Language:English
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Summary:Ribavirin has a minor and transient effect on hepatitis C virus (HCV) replication and has been suggested to select a novel mutation, F415Y, in the RNA‐dependent RNA polymerase of subtype 1a viruses. Twenty‐nine patients with chronic hepatitis C (subtyped by INNO LiPA as 1a, 17; 1b, 11; 1a/1b, 1) who were nonresponders to interferon‐based therapies were identified retrospectively and screened at Baseline, week 24 of treatment, and 24 weeks post‐treatment. Selection of resistance mutations, including at amino acid position 415 of the polymerase, was investigated. Using clonal sequencing and pyrosequencing of the NS5B gene, we screened for the F415Y resistance mutation among patients who received combination therapy with ribavirin and interferon α. Of the 15 subtype 1a patients treated with interferon plus ribavirin, only one had the F415Y change at week 24, and an F/Y mixture was still present 24 weeks after therapy. Four additional patients in this group had the F415Y change 24 weeks post‐therapy. The NS5B genes were sequenced in order to identify amino acid changes associated with ribavirin therapy, but no evidence was found that ribavirin selects for particular amino acids in the RNA‐dependent RNA polymerase. Ribavirin, a weak inhibitor of HCV replication, does not select for resistance mutations in the sequence of the HCV RNA polymerase.
ISSN:1352-0504
1365-2893
DOI:10.1111/j.1365-2893.2008.00980.x