Journal
ANTIVIRAL RESEARCH
Volume 111, Issue -, Pages 13-22Publisher
ELSEVIER
DOI: 10.1016/j.antiviral.2014.08.012
Keywords
Hepatitis C virus (HCV); Human Lactoferrin (hLF); Inhibitor; Viral replication; NS3; ATPase/Helicase
Categories
Funding
- Canadian Institutes of Health Research
- Natural Sciences and the Engineering Research Council of Canada
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Hepatitis C virus (HCV) is a major public-health problem with 130-170 million individuals chronically infected worldwide. In order to halt the epidemic, therapy against HCV will need to be both effective and widely available. Studies focusing on safe and affordable natural product active against HCV have revealed the antiviral activity of the human Lactoferrin (hLF) protein which binds and neutralizes the circulating virion. In the current study, investigation of hLF activity on the HCV subgenomic replicon system, which is independent from viral entry and shedding, revealed a distinct antireplicative activity of hLF against HCV. Hepatocellular uptake of hLF was confirmed and correlated with qualitative HCV staining reduction. Quantitative dose-response inhibition assays confirmed an hLF-mediated and dose-dependent HCV replication reduction reaching up to 60%. The in cellulo anti-HCV activity of hLF was additive to both Ribavirin and Interferon-alpha-21x Further investigation of hLF activity against the essential viral proteins involved in HCV genome replication revealed an inhibitory activity against the HCV ATPase/Helicase NS3 protein but not against the HCV RNA-dependent RNA polymerase (NS5B protein). NS3 inhibition was mediated by a direct and specific interaction between hLF and an allosteric binding site on NS3. Taken together, our findings reveal a new antiviral mechanism of action by which hLF inhibits intracellular HCV replication. (C) 2014 Elsevier B.V. All rights reserved.
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