We use cookies to understand how you use our site and to improve your experience. This includes personalizing content and advertising. To learn more, click here. By continuing to use our site, you accept our use of cookies. Cookie Policy.

LabMedica

Download Mobile App
Recent News Expo Medica 2024 Clinical Chem. Molecular Diagnostics Hematology Immunology Microbiology Pathology Technology Industry Focus

Cyclophilin A Is the Key to Hepatitis C Virus Replication

By LabMedica International staff writers
Posted on 26 Aug 2009
A team of German molecular virologists has found that replication of the hepatitis C virus (HCV), a positive-strand RNA virus, depends on the host protein cyclophilin A (peptidylprolyl isomerase A), and that viral replication can be blocked by the drug cyclosporin and its analogues. Cyclophilins catalyze the proper folding of proteins and the formation of large protein assemblies.

Health care officials estimate that more than 200 million people around the world are infected with hepatitis C - an overall incidence of around 3.3% of the world's population. Approximately 80% of HCV patients are chronically infected and have a high risk of developing serious liver inflammation, liver cirrhosis, or liver cancer.

Previous studies had shown that cyclosporin, known to sequester cyclophilins by direct binding, profoundly blocked HCV replication in cultured human hepatoma cells. However, conflicting results were obtained as to the particular cyclophilin (Cyp) required for viral RNA replication and the underlying possible mode of action.

In the current study, investigators at the University of Heidelberg (Germany) worked with a set of cell lines with stable knockdown of CypA or CypB. They reported in the August 14, 2009, online edition of the journal PLoS Pathogens that replication of HCV replicons of different genotypes was reduced by CypA depletion up to 1,000-fold whereas knockdown of CypB had no effect. Normal replication was restored by over-expression of wild type CypA, but not by a mutant lacking isomerase activity.

The cyclosporin analogue used in these experiments was DEBIO-25, which inhibits CypA but does not generally suppress the immune system. "The therapeutic potential of inhibiting cellular factors essential for virus replication has thus far hardly been tapped," said senior author Dr. Ralf Bartenschlager, professor of molecular virology at the University of Heidelberg. "But this approach has the major advantage that resistance arises less frequently and to a lesser extent in comparison to therapies directly targeting viral factors."

Related Links:
University of Heidelberg



Visit expo >
New
Gold Member
Pneumocystis Jirovecii Detection Kit
Pneumocystis Jirovecii Real Time RT-PCR Kit
Antipsychotic TDM AssaysSaladax Antipsychotic Assays
New
Sulfidoleukotrienes (sLT) Assay
CAST ELISA
New
Automated Cell Counter
QuadCount

Latest BioResearch News

Genome Analysis Predicts Likelihood of Neurodisability in Oxygen-Deprived Newborns

Gene Panel Predicts Disease Progession for Patients with B-cell Lymphoma

New Method Simplifies Preparation of Tumor Genomic DNA Libraries



Other channels

Copyright © 2000 - 2024 Globetech Media.
All rights reserved.