• Title of article

    The low-density lipoprotein receptor plays a role in the infection of primary human hepatocytes by hepatitis C virus

  • Author/Authors

    Sonia Molina، نويسنده , , Valérie Castet، نويسنده , , Chantal Fournier-Wirth، نويسنده , , Lydiane Pichard-Garcia، نويسنده , , Rachel Avner، نويسنده , , Dror Harats، نويسنده , , Joseph Roitelman، نويسنده , , Ronald Barbaras، نويسنده , , Pierre Graber، نويسنده , , Paola Ghersa، نويسنده , , Moshe Smolarsky، نويسنده , , Ada Funaro، نويسنده , , Fabio Malavasi، نويسنده , , Dominique Larrey، نويسنده , , Joliette Coste، نويسنده , , Jean-Mi، نويسنده ,

  • Issue Information
    روزنامه با شماره پیاپی سال 2007
  • Pages
    9
  • From page
    411
  • To page
    419
  • Abstract
    Background/Aims The direct implication of low-density lipoprotein receptor (LDLR) in hepatitis C virus (HCV) infection of human hepatocyte has not been demonstrated. Normal primary human hepatocytes infected by serum HCV were used to document this point. Methods Expression and activity of LDLR were assessed by RT-PCR and LDL entry, in the absence or presence of squalestatin or 25-hydroxycholesterol that up- or down-regulates LDLR expression, respectively. Infection was performed in the absence or presence of LDL, HDL, recombinant soluble LDLR peptides encompassing full-length (r-shLDLR4-292) or truncated (r-shLDLR4-166) LDL-binding domain, monoclonal antibodies against r-shLDLR4-292, squalestatin or 25-hydroxycholesterol. Intracellular amounts of replicative and genomic HCV RNA strands used as end point of infection were assessed by RT-PCR. Results r-shLDLR4-292, antibodies against r-shLDLR4-292 and LDL inhibited viral RNA accumulation, irrespective of genotype, viral load or liver donor. Inhibition was greatest when r-shLDLR4-292 was present at the time of inoculation and gradually decreased as the delay between inoculation and r-shLDLR4-292 treatment increased. In hepatocytes pre-treated with squalestatin or 25-hydroxycholesterol before infection, viral RNA accumulation increased or decreased in parallel with LDLR mRNA expression and LDL entry. Conclusions LDLR is involved at an early stage in infection of normal human hepatocytes by serum-derived HCV virions.
  • Keywords
    Virus receptor , Virus entry , Genome replication
  • Journal title
    Journal of Hepatology
  • Serial Year
    2007
  • Journal title
    Journal of Hepatology
  • Record number

    581305