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首页> 外文期刊>The Journal of Immunology: Official Journal of the American Association of Immunologists >Recombinant Canarypox Vaccine-Elicited CTL Specific for Dominant and Subdominant Simian Immunodeficiency Virus Epitopes in Rhesus Monkeys~1
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Recombinant Canarypox Vaccine-Elicited CTL Specific for Dominant and Subdominant Simian Immunodeficiency Virus Epitopes in Rhesus Monkeys~1

机译:恒河猴猴〜1中主要和主要的猿猴免疫缺陷病毒表位特异的重组金丝雀痘疫苗增强的CTL

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摘要

Since virus-specific CTL play a central role in containing HIV repilcation,a candidate AIDS vaccine should generate virus-specific CTL responses. In this study, the ability of a rcombinant canarypox virus expressing SIV Gag-Pol-Env (ALVAC/SIV gag-pol-env) was assessed for its ability to elicit both dominant and subdominant epitope-specific CTL responses in monkeys. Following a series of five immunizations, memory CTL responses specific for dominant Gag epitope could be demonstrated in the peripheral blood of vaccinated monkeys. Memory CTL responses to a subdominant Pol epitope were undetectable in these animals. Following challenge with SIV mac251, the experimentally vaccinated animals developed high frequency CTL responses specific for the dominant Gag epitope that emerged in temporal association with the early containment of viral replication. Interestingly, the experimentally vaccinated, but not the control vaccinated aminals, developed CTL responses to the subdominant Pol epitope that were detectable only after containment of early viremia. Thus, recombinant canarypox vaccination elicited low frequency, but durable memory CTL populations. The temporal association of the emergence of the dominant epitope-specific response with early viral containment following challenge suggests that this immune response played a role in the accelerated clearing of early viremia in these animals. The later emerging CTL response specific for the subdominant epitope may accelerated clearing of early viremia in these aminals. The later emerging CTL response specific for the subdominant epitope may contribute to the control of viral replication in the setting of chronic infection.
机译:由于特定于病毒的CTL在遏制HIV的复制中起着核心作用,因此候选艾滋病疫苗应产生特定于病毒的CTL反应。在这项研究中,评估了表达SIV Gag-Pol-Env的重组金丝雀痘病毒(ALVAC / SIV gag-pol-env)的能力,以引起猴子显性和显性表位特异性CTL反应。经过一系列的五次免疫接种后,在接种过的猴子的外周血中可以证明对显性Gag表位具有特异性的记忆CTL反应。在这些动物中无法检测到对主要的Pol表位的记忆CTL反应。在用SIV mac251攻击后,经过实验接种的动物产生了对显性Gag表位特异的高频CTL反应,该表位与病毒复制的早期遏制在时间上相关。有趣的是,经实验接种的疫苗,但未接种对照的接种的动物类动物,对主要的Pol表位产生了CTL反应,只有在遏制早期病毒血症后才能检测到。因此,重组金丝雀痘疫苗接种引起低频但持久的记忆CTL群体。挑战后显性抗原决定簇特异性反应的出现与早期病毒遏制之间的时间相关性表明,这种免疫反应在这些动物的早期病毒血症清除过程中发挥了作用。后来出现的针对主要表位的CTL反应可能会加速这些动物的早期病毒血症清除。后来出现的针对主要表位的特异性CTL反应可能有助于控制慢性感染环境中的病毒复制。

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