Gene gun-based nucleic acid immunization alone or in combination with recombinant vaccinia vectors suppresses virus burden in rhesus macaques challenged with a heterologous SIV

被引:65
作者
Fuller, DH
Simpson, L
Cole, KS
Clements, JE
Panicali, DL
Montelaro, RC
MurpheyCorb, M
Haynes, JR
机构
[1] GENIVA, MIDDLETON, WI USA
[2] TULANE REG PRIMATE RES CTR, COVINGTON, LA USA
[3] UNIV PITTSBURGH, SCH MED, PITTSBURGH, PA USA
[4] JOHNS HOPKINS UNIV, SCH MED, BALTIMORE, MD USA
[5] THERION BIOL, CAMBRIDGE, MA USA
[6] HESKA CORP, FT COLLINS, CO USA
关键词
gene gun; nucleic acid immunization; recombinant vaccinia virus; rhesus macaque; SIV;
D O I
10.1038/icb.1997.61
中图分类号
Q2 [细胞生物学];
学科分类号
071009 ; 090102 ;
摘要
Gene gun-based DNA immunization alone or in combination with recombinant vaccinia vectors was evaluated for the ability to elicit protective immune responses in rhesus macaques challenged with a pathogenic, heterologous simian immunodeficiency virus (SIV). Six monkeys primed with seven consecutive doses of DNA encoding SIVmac239 gp120 and gp160 (DNA+DNA) were divided into two groups. Three of these animals received another DNA booster immunization and the remaining three received a booster immunization containing a homologous, live recombinant vaccinia virus expressing SIVmac251 gp160 (DNA+VAC). In addition, a group of 15 animals primed with recombinant vaccinia vectors were divided into two groups. One group of six monkeys received another immunization of vaccinia (VAC+VAC) and the other nine animals received a DNA (mac239) booster immunization (VAC+DNA). Geometric mean end-point IgG titres in the DNA+VAC and VAC+DNA groups were substantially higher than the responses seen in the VAC+VAC and DNA+DNA groups, demonstrating a synergistic relationship between DNA-based vaccines and recombinant vaccinia virus-based vaccines. All vaccinates and five naive controls were challenged 19 weeks after the final booster immunization with 10 animal infectious doses of SIVDelta/B670. The vaccines did not prevent infection. However, all vaccine groups showed significant virus load reductions from seven to 56 days post challenge when compared to controls. Although the DNA+DNA group developed the lowest prechallenge antibody responses, the most significant reduction (200-fold) in virus load was associated with this group. In addition, a significant delay in CD4+ T cell loss relative to controls was observed in the DNA+DNA group. These results demonstrate that a gene gun-based DNA vaccine provided some attenuation of infection and CD4(+) T cell loss after a heterologous challenge.
引用
收藏
页码:389 / 396
页数:8
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