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      Newly synthesized hepatitis C virus replicon RNA is protected from nuclease activity by a protease-sensitive factor(s).

      Journal of Biology
      Cell Line, Endopeptidases, metabolism, Hepacivirus, genetics, physiology, Humans, Polyethylene Glycols, pharmacology, RNA, Viral, Replicon, Ribonucleases, Viral Nonstructural Proteins, Virus Replication

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          Abstract

          Biochemical characterization of hepatitis C virus (HCV) replication using purified, membrane-associated replication complexes is hampered by the presence of endogenous nuclease activity that copurifies with the replication complex. In this study, pulse-chase analyses were used to demonstrate that newly synthesized replicon RNA was protected from nuclease activity by a factor(s) that was sensitive to 0.5% NP-40 or protease treatment. Nuclease susceptibility was not related to disruption of lipid membranes, since NP-40 did not significantly affect the buoyant density of HCV replication complexes or protease susceptibility of HCV NS3 and NS5A proteins. These results suggest that a protease-sensitive factor(s) protects newly synthesized RNA from nuclease degradation. Copyright 2004 American Society for Microbiology

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          Author and article information

          Journal
          15331754
          514995
          10.1128/JVI.78.18.10202-10205.2004

          Chemistry
          Cell Line,Endopeptidases,metabolism,Hepacivirus,genetics,physiology,Humans,Polyethylene Glycols,pharmacology,RNA, Viral,Replicon,Ribonucleases,Viral Nonstructural Proteins,Virus Replication

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