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首页> 外文期刊>Immunity >Peripheral Prepositioning and Local CXCL9 Chemokine-Mediated Guidance Orchestrate Rapid Memory CD8+ T Cell Responses in the Lymph Node
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Peripheral Prepositioning and Local CXCL9 Chemokine-Mediated Guidance Orchestrate Rapid Memory CD8+ T Cell Responses in the Lymph Node

机译:外周定位和局部CXCL9趋化因子介导的指导在淋巴结中编排快速记忆CD8 + T细胞反应

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摘要

After an infection, the immune system generates long-lived memory lymphocytes whose increased frequency and altered state of differentiation enhance host defense against reinfection. Recently, the spatial distribution of memory cells was found to contribute to their protective function. Effector memory CD8+ T cells reside in peripheral tissue sites of initial pathogen encounter, in apparent anticipation of reinfection. Here we show that within lymph nodes (LNs), memory CD8+ T cells were concentrated near peripheral entry portals of lymph-borne pathogens, promoting rapid engagement of infected sentinel macrophages. A feed-forward CXCL9-dependent circuit provided additional chemotactic cues that further increase local memory cell density. Memory CD8+ T cells also produced effector responses to local cytokine triggers, but their dynamic behavior differed from that seen after antigen recognition. These data reveal the distinct localization and dynamic behavior of naive versus memory T cells within LNs and how these differences contribute to host defense.
机译:感染后,免疫系统会产生长寿命的记忆淋巴细胞,其频率增加和分化状态改变会增强宿主抵抗再感染的防御能力。最近,发现存储单元的空间分布有助于它们的保护功能。效应记忆的CD8 + T细胞驻留在最初病原体遭遇的外周组织部位,这显然是对再感染的预期。在这里,我们显示在淋巴结(LNs)内,记忆CD8 + T细胞集中在淋巴传播的病原体的外围进入门附近,从而促进受感染的前哨巨噬细胞的快速参与。前馈依赖CXCL9的电路提供了其他趋化线索,进一步增加了本地存储单元的密度。记忆CD8 + T细胞也对局部细胞因子触发物产生效应反应,但其动态行为与抗原识别后所见不同。这些数据揭示了LN内幼稚T细胞与记忆T细胞的独特定位和动态行为以及这些差异如何促进宿主防御。

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