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Dendritic cells Trigger IFN‐γ secretion by NK cells independent of IL‐12 and IL‐18

机译:树突细胞触发干扰素γ分泌的NK独立于细胞IL 12和IL 18

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Abstract It is commonly believed that IL‐12 produced by DCs in response to pathogens is the first signal that stimulates the production of IFN‐γ by NK cells. However, IL‐12 production by DCs in response to bacterial LPS depends on either engagement of CD40 by CD40L on activated T cells or IFN‐γ from NK cells. This suggests that during the primary immune response, NK cells produce IFN‐γ before IL‐12 production by DCs. Here, using single‐cell measurements, cell sorting and mouse lines deficient in IL‐12, IL‐23, type I IFN receptor and the IL‐18 receptor, we show that a subset of BM‐derived DCs characterized by low expression of MHC class II (MHCIIlow) stimulates IFN‐γ production by NK cells. The expression of Toll‐like Receptor (TLR) 4 on DCs but not NK cells was required for such NK‐derived IFN‐γ. In addition, soluble factor(s) produced by LPS‐activated MHCIIlow DCs were sufficient to induce IFN‐γ production by NK cells independent of IL‐12, IL‐23, and IL‐18. This response was enhanced in the presence of a low dose of IL‐2. These results delineate a previously unknown pathway of DC‐mediated IFN‐γ production by NK cells, which is independent of commonly known cytokines.
机译:摘要一般认为,IL 12由DCs在应对病原体第一个信号刺激生产干扰素γ的NK细胞。DCs在细菌LPS取决于要么CD40 CD40L在激活T的订婚从NK细胞细胞或者干扰素γ。在初次免疫反应,NK细胞产生干扰素γ应承担的由DCs IL 12应承担的生产之前。这里,使用单量细胞测量,细胞排序和鼠标线缺乏IL 12,IL高23在I型干扰素受体和IL 18受体,我们显示的一个子集BM派生DCs的特点是低表达MHC II级(MHCIIlow)刺激干扰素γ生产NK细胞。4在DCs但不需要NK细胞等NK派生干扰素γ应承担的。由有限合伙人优先激活MHCIIlow DCs足以通过NK细胞诱导干扰素γ应承担的生产独立的地理IL 12日IL高23和IL 18。反应是增强在存在低剂量IL 2。未知的途径的直流检测介导干扰素γ生产的NK细胞,这是独立的通常已知的细胞因子。

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