The simian human immunodeficiency virus (SHIV) macaque model of AIDS has provided a very useful system for evaluation of envelope-based candidate vaccines against HIV-1. Eight rhesus macaques were immunized with monomeric recombinant gp120 of HIV-1LAI (rgp120) and used to evaluate whether this vaccine conferred protection against challenge with pathogenic SHIVs (SHIVKU-2 and SHIV89.6P). The vaccinated macaques developed high titers of antibodies against rgp120 that reacted efficiently with the envelope proteins of homologous SHIV (SHIVKU-2) and poorly with the SHIV89.6P envelope, a heterologous strain of SHIV. This vaccine also induced neutralizing antibodies but only against SHIVKU-2. Vaccine-induced antibodies were of high avidity and predominantly against linear epitopes on the protein. Vaccinated macaques developed gp120-specific T-helper cells but no consistent cytotoxic T lymphocytes. However, cellular immune responses were short-lived in all eight vaccinates. At week 22 postimmunization, four vaccinates were challenged with SHIVKU-2 and the other four with SHIV89.6P. Four unvaccinated control macaques were also infected: two with SHIVKU-2 and two with SHIV89.6P. Vaccinated macaques generally showed anamnestic antibody and T-helper cell responses. However, T-helper responses were again short-lived. Upon challenge, the level of productive virus replication was indistinguishable between vaccine and control groups, suggesting that rgp120 did not confer protection against virus replication when animals were challenged with homologous or heterologous SHIV viruses.
Read full abstract