Four conserved RNA stem-loop structures designated SL47, SL87, SL248, and SL443 have been predicted in the hepatitis C virus (HCV) core encoding region. Moreover, alternative translation products have been detected from a reading frame overlapping the core gene (core؉1/ARFP/F). To study the importance of the core؉1 frame and core-RNA structures for HCV replication in cell culture and in vivo, a panel of core gene silent mutations predicted to abolish core؉1 translation and affecting core-RNA stem-loops were introduced into infectious-HCV genomes of the isolate JFH1. A mutation disrupting translation of all known forms of core؉1 and affecting SL248 did not alter virus production in Huh7 cells and in mice xenografted with human liver tissue. However, a combination of mutations affecting core؉1 at multiple codons and at the same time, SL47, SL87, and SL248, delayed RNA replication kinetics and substantially reduced virus titers. The in vivo infectivity of this mutant was impaired, and in virus genomes recovered from inoculated mice, SL87 was restored by reversion and pseudoreversion. Mutations disrupting the integrity of this stem-loop, as well as that of SL47, were detrimental for virus viability, whereas mutations disrupting SL248 and SL443 had no effect. This phenotype was not due to impaired RNA stability but to reduced RNA translation. Thus, SL47 and SL87 are important RNA elements contributing to HCV genome translation and robust replication in cell culture and in vivo.Hepatitis C virus (HCV) infection causes a wide spectrum of clinical manifestations, ranging from a healthy carrier state to acute and chronic hepatitis, liver cirrhosis, and hepatocellular carcinoma (17). More than 170 million people worldwide are chronically infected with the virus, which is responsible for more than 100,000 cases of liver cancer per year (39). A vaccine against the virus is not available at present, and therapeutic approaches are still limited (13,18).HCV is classified within the genus Hepacivirus of the family Flaviviridae (51). Seven major HCV genotypes and more than 100 subtypes have been identified (42). The single-stranded positive-sense RNA genome of HCV (ϳ9.6 kb in length) is flanked at both termini by conserved, highly structured nontranslated regions (NTRs) and encodes a polyprotein precursor of about 3,000 amino acids (4, 37). The NTRs are required for RNA translation and replication. An internal ribosome entry site (IRES) residing in the 5Ј NTR controls translation initiation, which is influenced by multiple transacting cellular factors via interaction either with the IRES sequence or core encoding sequences (20,33,40). Furthermore, long-range RNA-RNA interactions between the IRES and distally located sequences residing in the core coding region or 3Ј NTR, as well as interactions with the viral-protein core, nonstructural protein 4A (NS4A), NS4B, and NS5A, appear to modulate IRES activity.In the N-terminal region, the polyprotein, is processed by cellular proteases to yield the structural-protein core (C) and enve...
