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Efficacy of DNA and Fowlpox Virus Priming/Boosting Vaccines for Simian/Human Immunodeficiency Virus

机译:DNA和鸡痘病毒启动/加强免疫疫苗对猿猴/人类免疫缺陷病毒的功效

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摘要

Further advances are required in understanding protection from AIDS by T-cell immunity. We analyzed a set of multigenic simian/human immunodeficiency virus (SHIV) DNA and fowlpox virus priming and boosting vaccines for immunogenicity and protective efficacy in outbred pigtail macaques. The number of vaccinations required, the effect of DNA vaccination alone, and the effect of cytokine (gamma interferon) coexpression by the fowlpox virus boost was also studied. A coordinated induction of high levels of broadly reactive CD4 and CD8 T-cell immune responses was induced by sequential DNA and fowlpox virus vaccination. The immunogenicity of regimens utilizing fowlpox virus coexpressing gamma interferon, a single DNA priming vaccination, or DNA vaccines alone was inferior. Significant control of a virulent SHIV challenge was observed despite a loss of SHIV-specific proliferating T cells. The outcome of challenge with virulent SHIVmn229 correlated with vaccine immunogenicity except that DNA vaccination alone primed for protection almost as effectively as the DNA/fowlpox virus regimen despite negligible immunogenicity by standard assays. These studies suggest that priming of immunity with DNA and fowlpox virus vaccines could delay AIDS in humans.
机译:在了解通过T细胞免疫预防艾滋病的保护方面,还需要进一步的发展。我们分析了一套多基因猿猴/人类免疫缺陷病毒(SHIV)DNA和鸡痘病毒引发和加强疫苗,对近缘猪尾猕猴具有免疫原性和保护功效。还研究了所需的疫苗接种次数,单独的DNA疫苗接种效果以及禽痘病毒加强免疫引起的细胞因子(γ干扰素)共表达的效果。连续的DNA和禽痘病毒疫苗接种诱导了高水平的广泛反应性CD4和CD8 T细胞免疫应答的协同诱导。使用共表达γ-干扰素的鸡痘病毒,单次DNA初次接种疫苗或单独使用DNA疫苗的方案的免疫原性较差。尽管丧失了SHIV特异性增殖性T细胞,但仍观察到了对强毒SHIV攻击的有效控制。尽管标准方法的免疫原性可忽略不计,但用强力SHIVmn229攻击的结果与疫苗的免疫原性相关,只是单独的DNA疫苗接种可以起到与DNA /禽痘病毒方案几乎相同的保护作用。这些研究表明,用DNA和鸡痘病毒疫苗引发免疫力可能会延缓人类的艾滋病。

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