Evolution of the Hepatitis C Virus Second Envelope Protein Hypervariable Region in Chronically Infected Patients Receiving Alpha Interferon Therapy

Pawlotsky, Jean‐Michel; Germanidis, Georgios; Frainais, Pierre-Olivier; Bouvier, M; Soulier, Alexandre; Pellerin, Muriel; Dhumeaux, Daniel

doi:10.1128/jvi.73.8.6490-6499.1999

Cited by 78 publications

(46 citation statements)

References 70 publications

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“…Nonresponders or partial responders and, more often, responder-relapsers to a first course of IFN-␣ may achieve a sustained virologic response after a second identical course of IFN-␣ therapy. 79,81,82 In such cases, we observed significant qualitative HCV quasispecies changes after the first course of IFN. 79 The selected HCV variants were not intrinsically resistant to IFN-␣, because they were definitively cleared after the second course of IFN.…”

Section: Causes Of Hcv Resistance To Ifnmentioning

confidence: 85%

“…79,81,82 In such cases, we observed significant qualitative HCV quasispecies changes after the first course of IFN. 79 The selected HCV variants were not intrinsically resistant to IFN-␣, because they were definitively cleared after the second course of IFN. They just became fit in the environment created by the administration and subsequent withdrawal of IFN during and after the first course of treatment.…”

Section: Causes Of Hcv Resistance To Ifnmentioning

confidence: 85%

“…In the vast majority of, if not all, patients who do not achieve a sustained virologic response, IFN administration and subsequent IFN withdrawal are associated with significant qualitative changes in the composition of HCV quasispecies. [76][77][78][79][80] Both the mechanisms of action of IFN-␣ and recent clinical and virologic observations suggest that the selected HCV quasispecies variants are not intrinsically resistant to IFN-␣ but just become fit in the environment created by IFN-induction of host responses. This is supported by the following arguments:…”

Section: Causes Of Hcv Resistance To Ifnmentioning

confidence: 99%

“…They became nonfit and could be cleared during the second course of IFN because the nature of the host-virus interaction was different several months after the first course and could be tipped toward sustained viral clearance by IFN at that time. 79 Viral factors, nevertheless, appear to play an important role in HCV resistance to IFN-based therapy, probably conferring HCV quasispecies and infected cell properties that allow them to survive in the context of IFN administration. High quasispecies genetic complexity (i.e., a large size of the quasispecies sequence repertoire) at the beginning of therapy is an independent predictor of treatment failure.…”

Section: Causes Of Hcv Resistance To Ifnmentioning

confidence: 99%

“…Failure to clear HCV RNA during therapy is associated with significant qualitative HCV quasispecies changes in most, if not all, cases. [76][77][78][79][80] Although viral escape could be one of the mechanisms involved in treatment failure, most of these changes appear to be the consequence of the inability of the host to clear infection. They result in the accumulation of mutations on HCV genome during ongoing replication and selection of the corresponding variants.…”

Section: Consequences Of Hcv Resistance To Ifnmentioning

confidence: 99%

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Hepatitis C Virus Resistance to Antiviral Therapy

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Section: Causes Of Hcv Resistance To Ifnmentioning

confidence: 85%

Section: Causes Of Hcv Resistance To Ifnmentioning

confidence: 85%

Section: Causes Of Hcv Resistance To Ifnmentioning

confidence: 99%

Section: Causes Of Hcv Resistance To Ifnmentioning

confidence: 99%

Section: Consequences Of Hcv Resistance To Ifnmentioning

confidence: 99%

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Hepatitis C virus (HCV) causes acute and chronic liver disease in humans, including chronic hepatitis, cirrhosis, and hepatocellular carcinoma. Studies of this virus have been hampered by the lack of a productive cell culture system; most information thus has been obtained from analysis of the HCV genome, heterologous expression systems, in vitro and in vivo models, and structural analyses. Structural analyses of HCV components provide an essential framework for understanding of the molecular mechanisms of HCV polyprotein processing, RNA replication, and virion assembly and may contribute to a better understanding of the pathogenesis of hepatitis C. Moreover, these analyses should allow the identification of novel targets for antiviral intervention and development of new strategies to prevent and combat viral hepatitis. This article reviews the current knowledge of HCV structural biology. H epatitis C virus (HCV) is a small, envelopedRNA virus belonging to the Flaviviridae family, genus Hepacivirus, that causes acute and chronic liver disease in humans, including chronic hepatitis, cirrhosis, and hepatocellular carcinoma. The HCV genome is a single-stranded RNA molecule of positive polarity. It contains a single open reading frame (ORF) encoding a polyprotein of about 3,000 amino acids (Fig. 1). The ORF is flanked by 5Ј and 3Ј untranslated regions (UTR) of 341 and approximately 230 nucleotides in length, respectively. Both 5Ј and 3Ј UTR bear highly conserved RNA structures essential for polyprotein translation and genome replication. The 5Ј UTR contains an internal ribosome entry site (IRES) that binds the 40S ribosomal subunit and initiates polyprotein translation in a cap-independent manner. The polyprotein precursor is cotranslationally and posttranslationally processed by both cellular and viral proteases at the level of the endoplasmic reticulum (ER) membrane to yield 10 mature proteins. 1 The structural proteins include the core (C), which forms the viral nucleocapsid, and the envelope glycoproteins E1 and E2. They are released by host-cell signal peptidases. The structural proteins are separated from the nonstructural proteins by the short membrane peptide p7, thought to be a viroporin. The nonstructural (NS) proteins NS2 to NS5B are involved in polyprotein processing and viral replication. The proteolytic processing of NS polyprotein part is complex and requires two distinct proteinases: the NS2-NS3 zinc-dependent metalloproteinase, and the NS3 serine proteinase located in the N-terminal region of NS3. The NS2-NS3 proteinase appears to be dedicated solely to cleavage at the NS2/NS3 site that occurs rapidly and by a conformation-dependent, autocatalytic mechanism. 2 The remaining NS proteins are released by the NS3 proteinase associated with its cofactor, NS4A. The C-terminal region of NS3 protein includes RNA helicase and NTPase activities. NS4B is an integral membrane protein of unknown function. NS5A is a polyphosphorylated protein of unknown function, and NS5B is the RNA-dependent RNA polymerase (Rd...

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Evolution of the Hepatitis C Virus Second Envelope Protein Hypervariable Region in Chronically Infected Patients Receiving Alpha Interferon Therapy

Cited by 78 publications

References 70 publications

Hepatitis C Virus Resistance to Antiviral Therapy

Hepatitis C Virus Resistance to Antiviral Therapy

Structure and Molecular Virology

Structural biology of hepatitis C virus

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