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马传染性贫血病毒疫苗保护的包膜决定因素以及序列变异对免疫识别的影响。

Envelope determinants of equine infectious anemia virus vaccine protection and the effects of sequence variation on immune recognition.

作者信息

Tagmyer Tara L, Craigo Jodi K, Cook Sheila J, Even Deborah L, Issel Charles J, Montelaro Ronald C

机构信息

E1240 Biomedical Science Tower, Department of Microbiology and Molecular Genetics, School of Medicine, University of Pittsburgh, Pittsburgh, PA 15261, USA.

出版信息

J Virol. 2008 Apr;82(8):4052-63. doi: 10.1128/JVI.02028-07. Epub 2008 Jan 30.

Abstract

A highly effective attenuated equine infectious anemia virus (EIAV) vaccine (EIAV(D9)) capable of protecting 100% of horses from disease induced by a homologous Env challenge strain (EIAV(PV)) 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.

摘要

一种高效减毒马传染性贫血病毒(EIAV)疫苗(EIAV(D9))能够使100%的马匹免受同源Env攻击毒株(EIAV(PV))诱发疾病的侵害,最近在小马驹中进行了测试,以确定其对不同Env攻击毒株的保护水平(J.K.克雷戈、B.S.张、S.巴恩斯、T.L.塔格迈尔、S.J.库克、C.J.伊塞尔和R.C.蒙特拉罗,《美国国家科学院院刊》104:15105 - 15110,2007年)。观察到攻击毒株Env变异与疫苗对疾病的保护作用之间呈负相关。鉴于保护性免疫存在显著差异,我们推测分析针对Env蛋白的体液免疫和细胞免疫反应可能揭示疫苗保护的潜在决定因素。接种疫苗的小马驹免疫血清中针对同源Env或攻击毒株特异性Env的中和活性与对疾病的保护作用不相关。用Env肽库进行细胞分析未发现与疫苗对疾病的保护作用有关联。然而,当使用单个疫苗特异性Env肽时,发现8个细胞毒性T淋巴细胞(CTL)肽与疫苗保护密切相关。其中一个肽还产生了与保护性免疫相关的唯一淋巴细胞增殖反应。所鉴定的肽跨越了gp90的可变区和保守区。主要中和结构域和所鉴定肽内的氨基酸差异深刻影响免疫识别,这表现为无法检测到交叉反应性中和抗体以及某些肽特异性CTL反应发生改变。除了确定EIAV疫苗效力的潜在Env决定因素并证明特定Env变异对免疫识别的深远影响外,这些数据还说明了在慢病毒疫苗试验中,与肽库相比,单个肽在测量细胞免疫反应方面所具有的敏感性。

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