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Effector CD4 T-cell transition to memory requires late cognate interactions that induce autocrine IL-2.效应性CD4 T细胞向记忆性T细胞的转变需要诱导自分泌白细胞介素-2的晚期同源相互作用。
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TLR4 ligands lipopolysaccharide and monophosphoryl lipid a differentially regulate effector and memory CD8+ T Cell differentiation.TLR4 配体脂多糖和单磷酰脂质 A 可差异化调节效应和记忆 CD8+T 细胞的分化。
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The TNF family in T cell differentiation and function--unanswered questions and future directions.肿瘤坏死因子家族在T细胞分化和功能中的作用——未解决的问题与未来方向
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IL-12 and type I interferon prolong the division of activated CD8 T cells by maintaining high-affinity IL-2 signaling in vivo.白细胞介素-12 和 I 型干扰素通过维持体内高亲和力白细胞介素-2 信号来延长激活的 CD8 T 细胞的分裂。
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Key roles of adjuvants in modern vaccines.佐剂在现代疫苗中的关键作用。
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Interleukin 35: a key mediator of suppression and the propagation of infectious tolerance.白细胞介素35:抑制作用及传染性耐受传播的关键介质。
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The contextual role of TNFR family members in CD8(+) T-cell control of viral infections.TNFR 家族成员在 CD8(+) T 细胞控制病毒感染中的语境作用。
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对脂多糖(LPS)的反应增强了效应性CD8 T细胞在信号1和信号2之外的积累。

Responses to LPS boost effector CD8 T-cell accumulation outside of signals 1 and 2.

作者信息

Liu Wenhai, Menoret Antoine, Vella Anthony T

机构信息

Department of Immunology, School of Medicine, University of Connecticut Health Center, Farmington, CT 06030, USA.

出版信息

Cell Mol Immunol. 2017 Mar;14(3):254-253. doi: 10.1038/cmi.2015.69. Epub 2015 Jul 20.

DOI:10.1038/cmi.2015.69
PMID:26189366
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC5360877/
Abstract

Immunization with adjuvant plus antigen induces durable T-cell immunity and is a mainstay of vaccines. Here, the consequence of separating antigen stimulation of T cells from the adjuvant response was studied in a re-transfer model. Effector CD8 T cells in recipient mice were exposed to lipopolysaccharide (LPS), the Toll-like receptor 4 (TLR4) ligand, which significantly increased persistence. While accumulation in lymphoid and non-lymphoid organs was evident, this result depended upon the timing of LPS administration and the presence of the TLR4 adaptor TRIF in the recipient mice. Interestingly, there was very little impact of the LPS response on subset differentiation, which rather appeared to be programmed by antigen and costimulation. To discern factors that limit accumulation, interleukin 10 (IL-10) was targeted since it is a product of TLR4 triggering and mitigates inflammation. Blockade of IL-10 increased accumulation even though the effector CD8 T cells were well past the priming phase, but upon recall interferon-γ secretion was not affected as would be expected when IL-10 is present during priming. Thus, the adjuvant-altered microenvironment is effective not only in the presence of antigen but also during a window of effector CD8 T-cell stasis, suggesting that pathogen-associated molecular pattern molecules released during co-infection, or by vaccines, could alter the survival fate of specific effector T cells.Cellular & Molecular Immunology advance online publication, 20 July 2015; doi:10.1038/cmi.2015.69.

摘要

使用佐剂加抗原进行免疫接种可诱导持久的T细胞免疫,是疫苗的主要手段。在此,我们在再转移模型中研究了将T细胞的抗原刺激与佐剂反应分开的后果。受体小鼠中的效应CD8 T细胞暴露于脂多糖(LPS),即Toll样受体4(TLR4)配体,这显著增加了其持久性。虽然在淋巴器官和非淋巴器官中的积累很明显,但这一结果取决于LPS给药的时间以及受体小鼠中TLR4接头TRIF的存在。有趣的是,LPS反应对亚群分化的影响很小,亚群分化似乎更多地由抗原和共刺激编程。为了识别限制积累的因素,我们将白细胞介素10(IL-10)作为靶点,因为它是TLR4触发的产物并减轻炎症。阻断IL-10即使在效应CD8 T细胞已过启动阶段时仍会增加积累,但在再次刺激时,干扰素-γ分泌并未像在启动阶段存在IL-10时预期的那样受到影响。因此,佐剂改变的微环境不仅在存在抗原时有效,而且在效应CD8 T细胞静止期的一个窗口内也有效,这表明在合并感染期间或由疫苗释放的病原体相关分子模式分子可能会改变特定效应T细胞的存活命运。《细胞与分子免疫学》在线优先发表,2015年7月20日;doi:10.1038/cmi.2015.69 。