Immunization with a vaccinia virus recombinant expressing herpes simplex virus type 1 glycoprotein D: long-term protection and effect of revaccination.

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J Virol. 1988 May; 62(5): 1530-1534

Immunization with a vaccinia virus recombinant expressing herpes simplex virus type 1 glycoprotein D: long-term protection and effect of revaccination.

J F Rooney, C Wohlenberg, K J Cremer, B Moss and A L Notkins

Laboratory of Oral Medicine, National Institute of Dental Research, Bethesda, Maryland 20892.

ABSTRACT

Previously we showed that mice immunized with a vaccinia virusvector expressing the herpes simplex virus type 1 (HSV-1) glycoproteinD (gD) gene (vaccinia/gD) were protected against both lethaland latent infections with HSV-1 for at least 6 weeks afterimmunization (K. J. Cremer, M. Mackett, C. Wohlenberg, A. L.Notkins, and B. Moss, Science 228:737-740, 1985). In the experimentsdescribed here, we examined long-term immunity to HSV followingvaccinia/gD vaccination, the effect of revaccination with vaccinia/gD,and the impact of previous immunity to vaccinia virus on immunizationwith the gD recombinant. Mice immunized with vaccinia/gD showed100, 100, and 80% protection against lethal infection with HSV-1at 18, 44, and 60 weeks postimmunization, respectively. Protectionagainst latent trigeminal ganglionic infection was 70, 50, and31% at 6, 41, and 60 weeks postvaccination, respectively. Tostudy the effect of reimmunization on antibody levels, micevaccinated with vaccinia/gD were given a second immunization(booster dose) 3 months after the first. These mice developeda 10-fold increase in neutralizing-antibody titer (221 to 2,934)and demonstrated a significant increase in protection againstlethal HSV-1 challenge compared with animals that received onlyone dose of vaccinia/gD. To determine whether preexisting immunityto vaccinia virus inhibited the response to vaccination withvaccinia/gD virus, mice were immunized with a recombinant vacciniavirus vector expressing antigens from either influenza A orhepatitis B virus and were then immunized (2 to 3 months later)with vaccinia/gD. These mice showed reduced titers of neutralizingantibody to HSV-1 and decreased protection against both lethaland latent infections with HSV-1 compared with animals vaccinatedonly with vaccinia/gD. We conclude that vaccination with vaccinia/gDproduces immunity against HSV-1 that lasts over 1 year and thatthis immunity can be increased by a booster but that prior immunizationwith a vaccinia recombinant virus expressing a non-HSV genereduces the levels of neutralizing antibody and protective immunityagainst HSV-1 challenge.

J Virol. 1988 May; 62(5): 1530-1534

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