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Envelope Determinants of Equine Infectious Anemia Virus Vaccine Protection and the Effects of Sequence Variation on Immune Recognition▿

机译:马传染性贫血病毒疫苗保护的包膜决定因素和序列变异对免疫识别的影响▿

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摘要

A highly effective attenuated equine infectious anemia virus (EIAV) vaccine (EIAVD9) capable of protecting 100% of horses from disease induced by a homologous Env challenge strain (EIAVPV) was recently tested in ponies to determine the level of protection against divergent Env challenge strains (J. K. Craigo, B. S. Zhang, S. Barnes, T. L. Tagmyer, S. J. Cook, C. J. Issel, and R. C. Montelaro, Proc. Natl. Acad. Sci. USA 104:15105-15110, 2007). An inverse correlation between challenge strain Env variation and vaccine protection from disease was observed. Given the striking differences in protective immunity, we hypothesized that analysis of the humoral and cellular immune responses to the Env protein could reveal potential determinants of vaccine protection. Neutralization activity against the homologous Env or challenge strain-specific Env in immune sera from the vaccinated ponies did not correlate with protection from disease. Cellular analysis with Env peptide pools did not reveal an association with vaccine protection from disease. However, when individual vaccine-specific Env peptides were utilized, eight cytotoxic-T-lymphocyte (CTL) peptides were found to associate closely with vaccine protection. One of these peptides also yielded the only lymphoproliferative response associated with protective immunity. The identified peptides spanned both variable and conserved regions of gp90. Amino acid divergence within the principal neutralization domain and the identified peptides profoundly affected immune recognition, as illustrated by the inability to detect cross-reactive neutralizing antibodies and the observation that certain peptide-specific CTL responses were altered. In addition to identifying potential Env determinants of EIAV vaccine efficacy and demonstrating the profound effects of defined Env variation on immune recognition, these data also illustrate the sensitivity offered by individual peptides compared to peptide pools in measuring cellular immune responses in lentiviral vaccine trials.
机译:最近在马匹中测试了一种能够保护100%的马免于由同源Env攻击株(EIAVPV)诱发的疾病的高效减毒马传染性贫血病毒(EIAVD9)疫苗,以确定针对不同Env攻击株的保护水平(JK Craigo,BS Zhang,S.Barnes,TL Tagmyer,SJ Cook,CJ Issel和RC Montelaro,Proc.Natl.Acad.Sci.USA 104:15105-15110,2007年)。观察到挑战菌株Env变异与疫苗对疾病的保护之间呈负相关。鉴于保护性免疫的显着差异,我们假设对Env蛋白的体液和细胞免疫反应的分析可以揭示疫苗保护的潜在决定因素。在接种的小马的免疫血清中,针对同源Env或攻击菌株特异性Env的中和活性与对疾病的防护无关。使用Env肽库进行的细胞分析未显示与疫苗预防疾病的关联。但是,当使用单个疫苗特有的Env肽时,发现有八种细胞毒性T淋巴细胞(CTL)肽与疫苗保护密切相关。这些肽之一也产生了唯一的与保护性免疫有关的淋巴增生反应。鉴定的肽跨越gp90的可变区和保守区。主要中和域和鉴定出的肽段内的氨基酸差异极大地影响了免疫识别,如无法检测到交叉反应的中和抗体以及某些肽段特异性CTL反应发生改变的观察所表明。除了确定EIAV疫苗功效的潜在Env决定因素并证明已定义的Env变异对免疫识别的深远影响外,这些数据还说明了与慢病毒疫苗试验中的细胞免疫反应相比,单个肽与肽库相比具有更高的敏感性。

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