Naturally occurring dominant resistance mutations to hepatitis C virus protease and polymerase inhibitors in treatment-naïve patients

Thomas Kuntzen; Jörg Timm; Andrew Berical; Niall J. Lennon; Aaron M. Berlin; Sarah Young; Bongshin Lee; David Heckerman; Jonathan M. Carlson; Laura L. Reyor; Marianna Kleyman; Cory McMahon; Christopher Birch; Julian Schulze zur Wiesch; Timothy Ledlie; Michael Koehrsen; Chinnappa D. Kodira; Andrew Roberts; Georg M. Lauer; Hugo R. Rosen; Florian Bihl; Andreas Cerny; Ulrich Spengler; Zhimin Liu; Arthur Y. Kim; Yanming Xing; Arne Schneidewind; M.A. Madey; Jaquelyn Fleckenstein; Vicki M. Park; James E. Galagan; Chad Nusbaum; Bruce D. Walker; Gerond Lake‐Bakaar; Eric S. Daar; Ira M. Jacobson; Edward D. Gomperts; Brian R. Edlin; Sharyne Donfield; Raymond T. Chung; Andrew H. Talal; Tony N. Marion; Bruce W. Birren; Matthew R. Henn; Todd M. Allen

doi:10.1002/hep.22549

Naturally occurring dominant resistance mutations to hepatitis C virus protease and polymerase inhibitors in treatment-naïve patients

Thomas Kuntzen(Harvard University), Jörg Timm(Essen University Hospital), Andrew Berical(Harvard University), Niall J. Lennon(Broad Institute), Aaron M. Berlin(Broad Institute), Sarah Young(Broad Institute), Bongshin Lee(Microsoft (United States)), David Heckerman(Microsoft (United States)), Jonathan M. Carlson(Microsoft (United States)), Laura L. Reyor(Harvard University), Marianna Kleyman(Harvard University), Cory McMahon(Harvard University), Christopher Birch(Harvard University), Julian Schulze zur Wiesch(Universität Hamburg), Timothy Ledlie(Essen University Hospital), Michael Koehrsen(Broad Institute), Chinnappa D. Kodira(Broad Institute), Andrew Roberts(Broad Institute), Georg M. Lauer(Harvard University), Hugo R. Rosen(University of Colorado Hospital), Florian Bihl(University Hospital of Geneva), Andreas Cerny(Swiss HIV Cohort Study), Ulrich Spengler(University Hospital Bonn), Zhimin Liu(University of Tennessee Health Science Center), Arthur Y. Kim(Harvard University), Yanming Xing(University of Tennessee Health Science Center), Arne Schneidewind(Harvard University), M.A. Madey(University of Tennessee Health Science Center), Jaquelyn Fleckenstein(University of Tennessee Health Science Center), Vicki M. Park(University of Tennessee Health Science Center), James E. Galagan(Broad Institute), Chad Nusbaum(Broad Institute), Bruce D. Walker(Howard Hughes Medical Institute), Gerond Lake‐Bakaar(Cornell University), Eric S. Daar(The Lundquist Institute), Ira M. Jacobson(Cornell University), Edward D. Gomperts(Children's Hospital of Los Angeles), Brian R. Edlin(Cornell University), Sharyne Donfield(Rho (United States)), Raymond T. Chung(Harvard University), Andrew H. Talal(Cornell University), Tony N. Marion(University of Tennessee Health Science Center), Bruce W. Birren(Broad Institute), Matthew R. Henn(Broad Institute), Todd M. Allen(Harvard University)

Hepatology

July 28, 2008

10.1002/hep.22549

Cited by 345Open Access

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Abstract

UNLABELLED: Resistance mutations to hepatitis C virus (HCV) nonstructural protein 3 (NS3) protease inhibitors in <1% of the viral quasispecies may still allow >1000-fold viral load reductions upon treatment, consistent with their reported reduced replicative fitness in vitro. Recently, however, an R155K protease mutation was reported as the dominant quasispecies in a treatment-naïve individual, raising concerns about possible full drug resistance. To investigate the prevalence of dominant resistance mutations against specifically targeted antiviral therapy for HCV (STAT-C) in the population, we analyzed HCV genome sequences from 507 treatment-naïve patients infected with HCV genotype 1 from the United States, Germany, and Switzerland. Phylogenetic sequence analysis and viral load data were used to identify the possible spread of replication-competent, drug-resistant viral strains in the population and to infer the consequences of these mutations upon viral replication in vivo. Mutations described to confer resistance to the protease inhibitors Telaprevir, BILN2061, ITMN-191, SCH6 and Boceprevir; the NS5B polymerase inhibitor AG-021541; and to the NS4A antagonist ACH-806 were observed mostly as sporadic, unrelated cases, at frequencies between 0.3% and 2.8% in the population, including two patients with possible multidrug resistance. Collectively, however, 8.6% of the patients infected with genotype 1a and 1.4% of those infected with genotype 1b carried at least one dominant resistance mutation. Viral loads were high in the majority of these patients, suggesting that drug-resistant viral strains might achieve replication levels comparable to nonresistant viruses in vivo. CONCLUSION: Naturally occurring dominant STAT-C resistance mutations are common in treatment-naïve patients infected with HCV genotype 1. Their influence on treatment outcome should further be characterized to evaluate possible benefits of drug resistance testing for individual tailoring of drug combinations when treatment options are limited due to previous nonresponse to peginterferon and ribavirin.

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