UNLABELLED: Intravenous silibinin (SIL) is an approved therapeutic that has recently been applied to patients with chronic hepatitis C, successfully clearing hepatitis C virus (HCV) infection in some patients even in monotherapy. Previous studies suggested multiple antiviral mechanisms of SIL; however, the dominant mode of action has not been determined. We first analyzed the impact of SIL on replication of subgenomic replicons from different HCV genotypes in vitro and found a strong inhibition of RNA replication for genotype 1a and genotype 1b. In contrast, RNA replication and infection of genotype 2a were minimally affected by SIL. To identify the viral target of SIL we analyzed resistance to SIL in vitro and in vivo. Selection for drug resistance in cell culture identified a mutation in HCV nonstructural protein (NS) 4B conferring partial resistance to SIL. This was corroborated by sequence analyses of HCV from a liver transplant recipient experiencing viral breakthrough under SIL monotherapy. Again, we identified distinct mutations affecting highly conserved amino acid residues within NS4B, which mediated phenotypic SIL resistance also in vitro. Analyses of chimeric viral genomes suggest that SIL might target an interaction between NS4B and NS3/4A. Ultrastructural studies revealed changes in the morphology of viral membrane alterations upon SIL treatment of a susceptible genotype 1b isolate, but not of a resistant NS4B mutant or genotype 2a, indicating that SIL might interfere with the formation of HCV replication sites. CONCLUSION: Mutations conferring partial resistance to SIL treatment in vivo and in cell culture argue for a mechanism involving NS4B. This novel mode of action renders SIL an attractive candidate for combination therapies with other directly acting antiviral drugs, particularly in difficult-to-treat patient cohorts.
UNLABELLED: Intravenous silibinin (SIL) is an approved therapeutic that has recently been applied to patients with chronic hepatitis C, successfully clearing hepatitis C virus (HCV) infection in some patients even in monotherapy. Previous studies suggested multiple antiviral mechanisms of SIL; however, the dominant mode of action has not been determined. We first analyzed the impact of SIL on replication of subgenomic replicons from different HCV genotypes in vitro and found a strong inhibition of RNA replication for genotype 1a and genotype 1b. In contrast, RNA replication and infection of genotype 2a were minimally affected by SIL. To identify the viral target of SIL we analyzed resistance to SIL in vitro and in vivo. Selection for drug resistance in cell culture identified a mutation in HCV nonstructural protein (NS) 4B conferring partial resistance to SIL. This was corroborated by sequence analyses of HCV from a liver transplant recipient experiencing viral breakthrough under SIL monotherapy. Again, we identified distinct mutations affecting highly conserved amino acid residues within NS4B, which mediated phenotypic SIL resistance also in vitro. Analyses of chimeric viral genomes suggest that SIL might target an interaction between NS4B and NS3/4A. Ultrastructural studies revealed changes in the morphology of viral membrane alterations upon SIL treatment of a susceptible genotype 1b isolate, but not of a resistant NS4B mutant or genotype 2a, indicating that SIL might interfere with the formation of HCV replication sites. CONCLUSION: Mutations conferring partial resistance to SIL treatment in vivo and in cell culture argue for a mechanism involving NS4B. This novel mode of action renders SIL an attractive candidate for combination therapies with other directly acting antiviral drugs, particularly in difficult-to-treat patient cohorts.
Authors: Karoline Rutter; Thomas-Matthias Scherzer; Sandra Beinhardt; Heidrun Kerschner; Albert F Stättermayer; Harald Hofer; Theresia Popow-Kraupp; Petra Steindl-Munda; Peter Ferenci Journal: Antivir Ther Date: 2011
Authors: Rafael Bárcena; Ana Moreno; Miguel Angel Rodríguez-Gandía; Agustín Albillos; Carlos Arocena; Carlos Blesa; Fernando García-Hoz; Javier Graus; Javier Nuño; Pedro López-Hervás; Luis Gajate; Adolfo Martínez; Teresa Bermejo; María Luisa Mateos; Santos Del Campo Journal: J Hepatol Date: 2012-10-13 Impact factor: 25.083
Authors: M Biermer; B Schlosser; B Fülöp; F van Bömmel; A Brodzinski; R Heyne; K Keller; C Sarrazin; T Berg Journal: J Viral Hepat Date: 2011-12-29 Impact factor: 3.728
Authors: Roy L Hawke; Sarah J Schrieber; Tedi A Soule; Zhiming Wen; Philip C Smith; K Rajender Reddy; Abdus S Wahed; Steven H Belle; Nezam H Afdhal; Victor J Navarro; Josh Berman; Qi-Ying Liu; Edward Doo; Michael W Fried Journal: J Clin Pharmacol Date: 2009-10-19 Impact factor: 3.126
Authors: S DebRoy; N Hiraga; M Imamura; C N Hayes; S Akamatsu; L Canini; A S Perelson; R T Pohl; S Persiani; S L Uprichard; C Tateno; H Dahari; K Chayama Journal: J Viral Hepat Date: 2016-06-08 Impact factor: 3.728
Authors: Stephen J Polyak; Nicholas H Oberlies; Eve-Isabelle Pécheur; Harel Dahari; Peter Ferenci; Jean-Michel Pawlotsky Journal: Antivir Ther Date: 2012-09-25
Authors: Oliver Grünvogel; Katharina Esser-Nobis; Anna Reustle; Philipp Schult; Birthe Müller; Philippe Metz; Martin Trippler; Marc P Windisch; Michael Frese; Marco Binder; Oliver Fackler; Ralf Bartenschlager; Alessia Ruggieri; Volker Lohmann Journal: J Virol Date: 2015-08-12 Impact factor: 5.103
Authors: Julia Dietz; Daniel Rupp; Simone Susser; Johannes Vermehren; Kai-Henrik Peiffer; Natalie Filmann; Dimitra Bon; Thomas Kuntzen; Stefan Mauss; Georgios Grammatikos; Dany Perner; Caterina Berkowski; Eva Herrmann; Stefan Zeuzem; Ralf Bartenschlager; Christoph Sarrazin Journal: PLoS One Date: 2016-06-09 Impact factor: 3.240
Authors: Jason D Graci; Stephen P Jung; John Pichardo; Frederick Lahser; Xiao Tong; Zhengxian Gu; Joseph M Colacino Journal: Antimicrob Agents Chemother Date: 2016-11-21 Impact factor: 5.191