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ADCC Develops Over Time during Persistent Infection with Live-Attenuated SIV and Is Associated with Complete Protection against SIVmac251 Challenge

机译:ADCC在持续感染活弱化SIV的过程中会随着时间的流逝而发展并与针对SIVmac251挑战的全面保护相关

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摘要

Live-attenuated strains of simian immunodeficiency virus (SIV) routinely confer apparent sterilizing immunity against pathogenic SIV challenge in rhesus macaques. Understanding the mechanisms of protection by live-attenuated SIV may provide important insights into the immune responses needed for protection against HIV-1. Here we investigated the development of antibodies that are functional against neutralization-resistant SIV challenge strains, and tested the hypothesis that these antibodies are associated with protection. In the absence of detectable neutralizing antibodies, Env-specific antibody-dependent cell-mediated cytotoxicity (ADCC) emerged by three weeks after inoculation with SIVΔnef, increased progressively over time, and was proportional to SIVΔnef replication. Persistent infection with SIVΔnef elicited significantly higher ADCC titers than immunization with a non-persistent SIV strain that is limited to a single cycle of infection. ADCC titers were higher against viruses matched to the vaccine strain in Env, but were measurable against viruses expressing heterologous Env proteins. In two separate experiments, which took advantage of either the strain-specificity or the time-dependent maturation of immunity to overcome complete protection against SIVmac251 challenge, measures of ADCC activity were higher among the SIVΔnef-inoculated macaques that remained uninfected than among those that became infected. These observations show that features of the antibody response elicited by SIVΔnef are consistent with hallmarks of protection by live-attenuated SIV, and reveal an association between Env-specific antibodies that direct ADCC and apparent sterilizing protection by SIVΔnef.
机译:猿猴免疫缺陷病毒(SIV)的减毒活毒株通常赋予恒河猴猕猴明显的针对病原性SIV攻击的灭菌免疫力。了解减毒活病毒SIV的保护机制可能为了解预防HIV-1所需的免疫应答提供重要见解。在这里,我们研究了具有抗中和性SIV攻击菌株功能的抗体的开发,并检验了这些抗体与保护作用相关的假设。在没有可检测到的中和抗体的情况下,接种SIVΔnef后三周出现Env特异性抗体依赖性细胞介导的细胞毒性(ADCC),随着时间的推移逐渐增加,并且与SIVΔnef复制成比例。 SIVΔnef的持续感染引起的ADCC滴度明显高于非持久性SIV株(仅限于单个感染周期)的免疫接种。对于与Env中的疫苗株匹配的病毒,ADCC滴度较高,但对于表达异源Env蛋白的病毒则可测量。在两个单独的实验中,它们利用了菌株的特异性或免疫力的时间依赖性来克服针对SIVmac251攻击的完全保护,在未感染SIVΔnef的猕猴中,ADCC活性的测量值更高。已感染。这些观察结果表明,由SIVΔnef引发的抗体应答的特征与减毒活SIV的保护标志一致,并且揭示了指导ADCC的Env特异性抗体与SIVΔnef的明显灭菌保护之间的关联。

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