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CD8+ T cell dysfunction and increase in murine gammaherpesvirus latent viral burden in the absence of 4-1BB ligand.在缺乏4-1BB配体的情况下,CD8 + T细胞功能障碍及小鼠γ疱疹病毒潜伏病毒载量增加。
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Control of memory CD4 T cell recall by the CD28/B7 costimulatory pathway.通过CD28/B7共刺激途径对记忆性CD4 T细胞应答的调控。
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CD80 and CD86 control antiviral CD8+ T-cell function and immune surveillance of murine gammaherpesvirus 68.CD80和CD86调控抗小鼠γ疱疹病毒68的CD8⁺T细胞功能及免疫监视。
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Duration of the initial TCR stimulus controls the magnitude but not functionality of the CD8+ T cell response.初始TCR刺激的持续时间控制CD8 + T细胞反应的强度,但不影响其功能。
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10
Signals required for programming effector and memory development by CD8+ T cells.CD8+ T细胞编程效应器和记忆细胞发育所需的信号。
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在回忆反应期间,通过CD80/CD86-CD28共刺激对记忆性CD8 + T细胞分化的控制以及通过IL-2进行的恢复。

Control of memory CD8+ T cell differentiation by CD80/CD86-CD28 costimulation and restoration by IL-2 during the recall response.

作者信息

Fuse Shinichiro, Zhang Weijun, Usherwood Edward J

机构信息

Department of Microbiology and Immunology, Dartmouth Medical School, Lebanon, NH 03756, USA.

出版信息

J Immunol. 2008 Jan 15;180(2):1148-57. doi: 10.4049/jimmunol.180.2.1148.

DOI:10.4049/jimmunol.180.2.1148
PMID:18178855
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC2954438/
Abstract

Memory CD8+ T cell responses have been considered to be independent of CD80/CD86-CD28 costimulation. However, recall responses are often severely blunted in CD28-/- mice. Whether this impairment represents a requirement for CD28 costimulation for proper memory CD8+ T cell development or a requirement during the recall response is unknown. Furthermore, how CD28 costimulation affects the phenotype and function of memory CD8+ T cells has not been characterized in detail. In this study, we investigate these questions by studying the role of the CD28 costimulatory pathway in memory CD8+ T cell responses to acute and persistent DNA virus infections. Memory CD8+ T cells against vaccinia virus (VV) infection which develop without CD28 costimulation exhibit lower expression of differentiation markers CD27 and CD122 (IL-15Rbeta). These memory CD8+ T cells also fail to produce IL-2. Our data indicate that for an optimal recall response, CD28 costimulation is required both for T cell priming and also during the recall response. Similar requirements were observed for memory CD8+ T cell responses during persistent infection with murine gammaherpesvirus 68 (MHV-68) infection, indicating CD28 may play the same role in both acute and persistent infections. Finally, we show deficits in the recall response are restored by IL-2 signaling during recall, but not during priming. The data presented show that CD28 costimulation not only controls the magnitude of the primary response but also affects development of memory CD8+ T cells and is required during the recall response in addition to initial T cell priming.

摘要

记忆性CD8 + T细胞反应一直被认为独立于CD80/CD86 - CD28共刺激。然而,在CD28基因敲除小鼠中,回忆反应常常严重减弱。这种缺陷是代表记忆性CD8 + T细胞正常发育需要CD28共刺激,还是回忆反应过程中需要CD28共刺激尚不清楚。此外,CD28共刺激如何影响记忆性CD8 + T细胞的表型和功能尚未得到详细描述。在本研究中,我们通过研究CD28共刺激途径在记忆性CD8 + T细胞对急性和持续性DNA病毒感染反应中的作用来探讨这些问题。在没有CD28共刺激的情况下产生的针对痘苗病毒(VV)感染的记忆性CD8 + T细胞,其分化标志物CD27和CD122(IL - 15Rβ)的表达较低。这些记忆性CD8 + T细胞也无法产生IL - 2。我们的数据表明,为了获得最佳的回忆反应,在T细胞启动阶段和回忆反应期间都需要CD28共刺激。在小鼠γ疱疹病毒68(MHV - 68)持续性感染期间的记忆性CD8 + T细胞反应中也观察到类似的需求,表明CD28在急性和持续性感染中可能发挥相同的作用。最后,我们表明回忆反应期间的缺陷可通过IL - 2信号恢复,但启动阶段不行。所呈现的数据表明,CD28共刺激不仅控制初次反应的强度,还影响记忆性CD8 + T细胞的发育,并且除了初始T细胞启动外,在回忆反应期间也是必需的。