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首页> 外文期刊>Immunological reviews. >Compartmentalization of dendritic cell and T‐cell interactions in the lymph node: Anatomy of T‐cell fate decisions
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Compartmentalization of dendritic cell and T‐cell interactions in the lymph node: Anatomy of T‐cell fate decisions

机译:淋巴结中树突细胞和T细胞相互作用的分区化:T细胞命运决策的解剖学

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Summary Upon receiving cognate and co‐stimulatory priming signals from antigen (Ag)‐presenting dendritic cells (DCs) in secondary lymphoid tissues, na?ve CD4 + T cells differentiate into distinct effector and memory populations. These alternate cell fate decisions, which ultimately control the T‐cell functional attributes, are dictated by programming signals provided by Ag‐bearing DCs and by other cells that are present in the microenvironment in which T‐cell priming occurs. We know that DCs can be subdivided into multiple populations and that the various DC subsets exhibit differential capacities to initiate development of the different CD4 + T‐helper populations. What is less well understood is why different subanatomic regions of secondary lymphoid tissues are colonized by distinct populations of Ag‐presenting DCs and how the location of these DCs influences the type of T‐cell response that will be generated. Here we review how chemokine receptors and their ligands, which position allergen and nematode‐activated DCs within different microdomains of secondary lymphoid tissues, contribute to the establishment of IL‐4 committed follicular helper T and type 2 helper cell responses.
机译:发明内容在次级淋巴组织中的抗原(Ag) - 蛋白质的树突细胞(DCS)中接受来自抗原(Ag)的共刺激引发信号,Na've CD4 + T细胞分化为不同的效应和记忆群。这些最终控制T细胞功能属性的这些替代细胞命运决定是通过通过轴承DC提供的编程信号和存在于T细胞喷射的微环境中存在的其他细胞来决定。我们知道DC可以细分为多个群体,并且各种DC子集呈现差异容量,以启动不同的CD4 + T辅助群体的开发。更易于理解的是为什么通过初始淋巴组织的不同的副淋巴组织区域通过不同的AG呈递DC的群体和这些DCS的位置如何影响将产生的T细胞响应的类型。在这里,我们审查了趋化因素受体和它们的配体,其在次级淋巴组织的不同微粒中的过敏原和线虫活化DC的态度如何导致IL-4犯下卵泡辅助T和型辅助细胞反应的贡献。

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