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通过分子模拟解决CD8记忆T细胞对痘苗病毒攻击的保护作用。

Protection against vaccinia virus challenge by CD8 memory T cells resolved by molecular mimicry.

作者信息

Cornberg Markus, Sheridan Brian S, Saccoccio Frances M, Brehm Michael A, Selin Liisa K

机构信息

Department of Pathology, University of Massachusetts Medical School, 55 Lake Avenue North, Worcester, MA 01655, USA.

出版信息

J Virol. 2007 Jan;81(2):934-44. doi: 10.1128/JVI.01280-06. Epub 2006 Nov 1.

Abstract

Live vaccinia virus (VV) vaccination has been highly successful in eradicating smallpox. However, the mechanisms of immunity involved in mediating this protective effect are still poorly understood, and the roles of CD8 T-cell responses in primary and secondary VV infections are not clearly identified. By applying the concept of molecular mimicry to identify potential CD8 T-cell epitopes that stimulate cross-reactive T cells specific to lymphocytic choriomeningitis virus (LCMV) and VV, we identified after screening only 115 peptides two VV-specific immunogenic epitopes that mediated protective immunity against VV. An immunodominant epitope, VV-e7r130, did not generate cross-reactive T-cell responses to LCMV, and a subdominant epitope, VV-a11r198, did generate cross-reactive responses to LCMV. Infection with VV induced strong epitope-specific responses which were stable into long-term memory and peaked at the time virus was cleared, consistent with CD8 T cells assisting in the control of VV. Two different approaches, direct adoptive transfer of VV-e7r-specific CD8 T cells and prior immunization with a VV-e7r-expressing ubiquitinated minigene, demonstrated that memory CD8 T cells alone could play a significant role in protective immunity against VV. These studies suggest that exploiting cross-reactive responses between viruses may be a useful tool to complement existing technology in predicting immunogenic epitopes to large viruses, such as VV, leading to a better understanding of the role CD8 T cells play during these viral infections.

摘要

活痘苗病毒(VV)疫苗接种在根除天花方面非常成功。然而,介导这种保护作用的免疫机制仍知之甚少,并且CD8 T细胞反应在原发性和继发性VV感染中的作用尚未明确。通过应用分子模拟的概念来鉴定潜在的CD8 T细胞表位,这些表位可刺激针对淋巴细胞性脉络丛脑膜炎病毒(LCMV)和VV的交叉反应性T细胞,我们在筛选仅115种肽后鉴定出两种介导针对VV的保护性免疫的VV特异性免疫原性表位。一个免疫显性表位VV-e7r130不会产生针对LCMV的交叉反应性T细胞反应,而一个亚显性表位VV-a11r198会产生针对LCMV的交叉反应性反应。VV感染诱导了强烈的表位特异性反应,这些反应稳定为长期记忆并在病毒清除时达到峰值,这与CD8 T细胞协助控制VV一致。两种不同的方法,即直接过继转移VV-e7r特异性CD8 T细胞和用表达VV-e7r的泛素化小基因进行预先免疫,证明仅记忆CD8 T细胞就可以在针对VV的保护性免疫中发挥重要作用。这些研究表明,利用病毒之间的交叉反应性反应可能是一种有用的工具,可补充现有技术来预测针对大型病毒(如VV)的免疫原性表位,从而更好地理解CD8 T细胞在这些病毒感染期间所起的作用。

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