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T细胞对病毒的记忆隐私性。

The privacy of T cell memory to viruses.

作者信息

Welsh R M, Kim S K, Cornberg M, Clute S C, Selin L K, Naumov Y N

机构信息

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

出版信息

Curr Top Microbiol Immunol. 2006;311:117-53. doi: 10.1007/3-540-32636-7_5.

Abstract

T cell responses to viral infections can mediate either protective immunity or damaging immunopathology. Viral infections induce the proliferation of T cells specific for viral antigens and cause a loss in the number of T cells with other specificities. In immunologically naive hosts, viruses will induce T cell responses that, dependent on the MHC, recognize a distinct hierarchy of virus-encoded T cell epitopes. This hierarchy can change if the host has previously encountered another pathogen that elicited a memory pool ofT cells specific to a cross-reactive epitope. This heterologous immunity can deviate the normal immune response and result in either beneficial or harmful effects on the host. Each host has a unique T cell repertoire caused by the random DNA rearrangement that created it, so the specific T cells that create the epitope hierarchy differ between individuals. This "private specificity" seems of little significance in the T cell response of a naive host to infection, but it is of profound importance under conditions of heterologous immunity, where a small subset of a cross-reactive memory pool may expand and dominate a response. Examples are given of how the private specificities of immune responses under conditions of heterologous immunity influence the pathogenesis of murine and human viral infections.

摘要

T细胞对病毒感染的反应既可以介导保护性免疫,也可以导致有害的免疫病理反应。病毒感染会诱导针对病毒抗原的T细胞增殖,并导致具有其他特异性的T细胞数量减少。在免疫未成熟的宿主中,病毒会诱导T细胞反应,这种反应依赖于主要组织相容性复合体(MHC),识别病毒编码的T细胞表位的不同等级。如果宿主先前遇到过另一种引发了针对交叉反应性表位的T细胞记忆库的病原体,这种等级可能会发生变化。这种异源免疫可以使正常免疫反应发生偏差,对宿主产生有益或有害的影响。由于随机DNA重排产生了独特的T细胞库,每个宿主都有其独特的T细胞库,因此产生表位等级的特定T细胞在个体之间存在差异。这种“个体特异性”在未成熟宿主对感染的T细胞反应中似乎意义不大,但在异源免疫条件下却至关重要,在这种情况下,交叉反应性记忆库的一小部分可能会扩增并主导反应。文中给出了异源免疫条件下免疫反应的个体特异性如何影响小鼠和人类病毒感染发病机制的例子。

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