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Innate and adaptive stimulation of murine diverse NKT cells result in distinct cellular responses

机译:先天和适应性的刺激小鼠多样化NKT细胞产生不同的细胞反应

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Abstract Natural killer T (NKT) cells recognize glycolipids presented on CD1d. They share features of adaptive T lymphocytes and innate NK cells, and mediate immunoregulatory functions via rapid production of cytokines. Invariant (iNKT) and diverse (dNKT) NKT cell subsets are defined by their TCR. The immunological role of dNKT cells, that do not express the invariant TCRα‐chain used by iNKT cells, is less well explored than that of iNKT cells. Here, we investigated signals driving Toll‐like receptor (TLR) ligand activation of TCR‐transgenic murine dNKT cells. IFN‐γ production by dNKT cells required dendritic cells (DC), cell‐to‐cell contact and presence of TLR ligands. TLR‐stimulated DC activated dNKT cells to secrete IFN‐γ in a CD1d‐, CD80/86‐ and type I IFN‐independent manner. In contrast, a requirement for IL‐12p40, and a TLR ligand‐selective dependence on IL‐18 or IL‐15 was observed. TLR ligand/DC stimulation provoked early secretion of pro‐inflammatory cytokines by both CD62L + and CD62L ? dNKT cells. However, proliferation was limited. In contrast, TCR/co‐receptor‐mediated activation resulted in proliferation and delayed production of a broader cytokine spectrum preferentially in CD62L ? dNKT cells. Thus, innate (TLR ligand/DC) and adaptive (TCR/co‐receptor) stimulation of dNKT cells resulted in distinct cellular responses that may contribute differently to the formation of immune memory.
机译:抽象的自然杀伤T (NKT细胞识别糖脂在CD1d。特性的自适应T淋巴细胞和天生的NK通过细胞,调节免疫调节功能细胞因子的快速生产。和多样化(dNKT) NKT细胞定义子集的细胞。不表达的细胞,不变的细胞受体αiNKT细胞使用的作业链,不太好探索比iNKT细胞。研究驾驶人数的类受体的信号(TLR)配体激活细胞的转基因小鼠dNKT细胞。树突状细胞(DC),细胞~所致细胞接触和TLR配体的存在。TLR刺激DC活化dNKT细胞分泌干扰素γ应承担在一个CD1d CD80/86和I型干扰素的独立的方式。要求地理IL 12 p40和TLR配体高选择性依赖IL 18或者IL 15观察到。早期的pro必经炎性细胞因子的分泌CD62L +和CD62L吗?扩散是有限的。识别/公司应承担的受体介导的激活导致扩散和延迟生产的细胞因子谱CD62L优先?细胞。(TCR / co检测受体)dNKT细胞的刺激导致不同的细胞反应,可能为免疫的形成贡献不同内存。

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