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优化的 SIV DNA 疫苗可作为 Ad5 的加强针,提供针对高剂量 SIVmac251 挑战的部分保护。

An optimized SIV DNA vaccine can serve as a boost for Ad5 and provide partial protection from a high-dose SIVmac251 challenge.

机构信息

Department of Pathology and Laboratory Medicine, University of Pennsylvania, School of Medicine, Philadelphia, PA, United States.

出版信息

Vaccine. 2012 May 2;30(21):3202-8. doi: 10.1016/j.vaccine.2012.02.069. Epub 2012 Mar 8.

DOI:10.1016/j.vaccine.2012.02.069
PMID:22406458
Abstract

One limitation in the development of an improved cellular response needed for an effective HIV-vaccine is the inability to induce robust effector T-cells capable of suppressing a heterologous challenge. To improve cellular immune responses, we examined the ability of an optimized DNA vaccine to boost the cellular immune responses induced by a highly immunogenic Ad5 prime. Five Chinese rhesus macaques received pVax encoding consensus (con) gag/pol/env intramuscularly (IM) with electroporation followed by the Merck Ad5 gag/pol/nef vaccine. A second group of five animals were vaccinated with Merck Ad5 gag/pol/nef followed by pVax gag/pol/env. One year following vaccination, Ad5-prime DNA-boosted monkeys and four unvaccinated controls received an intrarectal challenge with 1000 ID50 SIV(mac)251. The quality and magnitude of the T-cell response was analyzed by ELISpot and polyfunctional flow cytometry. We observed that an Ad5-prime DNA-boost resulted in significantly elevated SIV-specific T-cell responses even compared with animals receiving a DNA-prime Ad5-boost. Ad5 prime DNA boosted animals were capable of suppressing a pathogenic SIV(mac)251 challenge. Peak control correlated with the expansion of HLA-DR(+) CD8(+) T-cells two weeks post-infection. These data illustrate that high optimization of a DNA vaccine can drive of immune responses primed by a robust vector system. This previously unachievable feature of these newly optimized DNAs warrants future studies of this strategy that may circumvent issues of serology associated with viral vector prime-boost systems.

摘要

一种改进的细胞反应的发展的限制对于有效的 HIV 疫苗是无法诱导强大的效应 T 细胞能够抑制异源挑战。为了提高细胞免疫应答,我们研究了优化的 DNA 疫苗的能力来增强由高度免疫原性的 Ad5 引发的细胞免疫应答。五只中国猕猴接受了 pVax 编码共识 (con) gag/pol/env 肌肉内 (IM) 与电穿孔,然后是默克公司的 Ad5 gag/pol/nef 疫苗。第二组五只动物用默克公司的 Ad5 gag/pol/nef 接种,然后用 pVax gag/pol/env。接种一年后,Ad5 疫苗增强的猴子和四只未接种的对照动物接受了 1000 ID50 SIV(mac)251 的直肠内挑战。T 细胞反应的质量和幅度通过 ELISpot 和多功能流式细胞术进行分析。我们观察到,Ad5 疫苗增强的 DNA 疫苗导致了明显升高的 SIV 特异性 T 细胞反应,甚至与接受 DNA 疫苗增强的 Ad5 疫苗的动物相比也是如此。Ad5 疫苗增强的动物能够抑制致病性 SIV(mac)251 挑战。峰值控制与 HLA-DR(+) CD8(+) T 细胞的扩张相关两周后感染。这些数据表明,DNA 疫苗的高度优化可以驱动由强大的载体系统引发的免疫反应。这些新优化的 DNA 以前无法实现的这一特性需要对该策略进行进一步研究,该策略可能回避与病毒载体增强疫苗系统相关的血清学问题。

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