Immunogenicity of the E1E2 proteins of hepatitis C virus expressed by recombinant adenoviruses

The El and E2 proteins of hepatitis C virus (HCV) are believed to be the vi ral envelope glycoproteins that are major candidate antigens for HCV vaccin e development. We reported previously that the replication-competent recomb inant adenovirus encoding core-E1-E2 genes of HCV (Ad/HCV) produces serolog ically reactive El and E2 proteins forming a heterodimer in substantial amo unts. Here, we examined immunogenicity of the E1E2 proteins copurified from HeLa cells infected with Ad/HCV virus in mice. Furthermore, we constructed a replication-defective recombinant adenovirus encoding the core-E1-E2 gen es of HCV (Ad.CMV.HCV) and examined immunogenicity of the virus in mice. Th e mice immunized intraperitoneally with the copurified E1E2 proteins induce d mainly antibodies to E2, but not to El by Western blot analysis. The sera of mice immunized with the E1E2 inhibited the binding of E2 protein to the major extracellular loop of human CD81. E2-specific cytotoxic T cells (CTL s), but not antibodies to the E1E2 antigens were induced in the mice intram uscularly immunized with Ad.CMV.HCV virus. When immunized with both Ad.CMV. HCV virus and the E1E2, mice elicited E2-specific CTLs and antibodies to th e E1E2 antigens. The results suggest that immunization of Ad.CMV.HCV virus combined with E2 protein is an effective modality to induce humoral as well as cellular immune response to E2 antigen. (C) 2001 Elsevier Science Ltd. All rights reserved.