AI Article Synopsis
- The JFH-1 strain of hepatitis C virus (HCV) can replicate on its own in certain liver cells, while the J6 strain cannot without modification.
- Researchers created hybrid RNA combinations of J6 and JFH-1 to study which parts enable replication and infectious particle production.
- They found that two specific regions from the JFH-1 strain, NS3 helicase and NS5B-to-3'X, are essential for effective replication and the creation of infectious HCV particles in genotype 2a strains.
Article Abstract
The JFH-1 strain of hepatitis C virus (HCV) is a genotype 2a strain that can replicate autonomously in Huh7 cells. The J6 strain is also a genotype 2a strain, but its full genomic RNA does not replicate in Huh7 cells. However, chimeric J6/JFH-1 RNA that has J6 structural-protein-coding regions and JFH-1 nonstructural-protein-coding regions can replicate autonomously and produce infectious HCV particles. In order to determine the mechanisms underlying JFH-1 RNA replication, we constructed various J6/JFH-1 chimeras and tested their RNA replication and virus particle production abilities in Huh7 cells. Via subgenomic-RNA-replication assays, we found that both the JFH-1 NS5B-to-3'X (N5BX) and the NS3 helicase (N3H) regions are important for the replication of the J6CF replicon. We applied these results to full-length genomic RNA replication and analyzed replication using Northern blotting. We found that a chimeric J6 clone with JFH-1 N3H and N5BX could replicate autonomously but that a chimeric J6 clone with only JFH-1 N5BX had no replication ability. Finally, we tested the virus production abilities of these clones and found that a chimeric J6 clone with JFH-1 N3H and N5BX could produce infectious HCV particles. In conclusion, the JFH-1 NS3 helicase and NS5B-to-3'X regions are important for efficient replication and virus particle formation of HCV genotype 2a strains.
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| http://www.ncbi.nlm.nih.gov/pmc/articles/PMC1951293 | PMC |
| http://dx.doi.org/10.1128/JVI.02088-06 | DOI Listing |
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