| Literature DB >> 7930718 |
B S Graham1, G J Gorse, D H Schwartz, M C Keefer, M J McElrath, T J Matthews, P F Wright, R B Belshe, M L Clements, R Dolin.
Abstract
Priming with a live recombinant vector followed by subunit boosting is a promising strategy for human immunodeficiency virus (HIV) immunization. Twenty-nine vaccinia-naive volunteers were primed with gp160-recombinant vaccinia virus (HIVAC-1e) and boosted with recombinant (r) gp160 to define factors associated with the magnitude and specificity of antibody response after booster immunization. A longer interval between inoculation and boost, two inoculations of HIVAC-1e with lesion formation occurring after the first, and Western blot-detectable antibody to gp160 after inoculation were significantly associated with higher neutralizing antibody titers and fusion-inhibiting activity after boosting. HIVAC-1e-primed vaccinees were more likely to have antibody to V3- and CD4-binding regions of gp120 and less likely to have antibody to constant regions 2 and 3 than vaccinees immunized with rgp160 alone. Priming volunteers with HIVAC-1e was a key determinant of the epitope specificity and magnitude of functional antibody responses induced by rgp160 boosting.Entities:
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Year: 1994 PMID: 7930718 DOI: 10.1093/infdis/170.4.782
Source DB: PubMed Journal: J Infect Dis ISSN: 0022-1899 Impact factor: 5.226