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ICOS regulates the pool of group 2 innate lymphoid cells under homeostatic and inflammatory conditions in mice

机译:国际安全和发展理事会先天淋巴组2的调节池在稳态和炎性细胞条件在老鼠身上

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摘要

Group 2 innate lymphoid cells (ILC2s) are innate effectors playing an important role in the defense against helminthic infections and in the pathogenesis of allergic inflammation. Cytokines have been identified as the major stimuli driving ILC2 activation and expansion. Conversely, it is unclear whether costimulatory molecules contribute to regulation of ILC2 functions. ILC2s display high expression of inducible T-cell costimulator (ICOS), which belongs to the CD28 superfamily, and which has been shown to control late effector T-cell functions, and is of utmost importance for the humoral immune response. However, the biological function of ICOS expression on ILC2s is unknown. Here, we show that ICOS signaling in mice regulates ILC2 homeostasis independently of T cells and B cells, by promoting proliferation and accumulation of mature ILC2s in lung and intestine. In a model of IL-33-induced airway inflammation, ICOS controls ILC2 activation and eosinophil infiltration in the lung. Our data identify a role of ICOS in innate immunity and indicate that not only cytokines, but also costimulatory pathways such as those involving ICOS, can contribute to regulate the ILC2 pool. Thus, ICOS costimulation blockade, which is currently under clinical evaluation for inhibiting the humoral immune response, could also target innate inflammatory circuits.
机译:组2 (ILC2s)是与生俱来的先天淋巴细胞效应器中发挥着重要的作用防御蠕虫感染的过敏性炎症的发病机制。已确定为最主要的刺激开车ILC2激活和扩张。不清楚costimulatory分子有助于调节ILC2功能。显示高表达的诱导t细胞costimulator(这个理事会),这属于CD28总科,可以控制后期效应t细胞的功能,是最大的体液免疫反应的重要性。国际安全和发展理事会的生物功能表情ILC2s是未知的。国际安全和发展理事会信号在老鼠调节ILC2独立于T细胞和B细胞内稳态,通过促进细胞增殖和积累成熟ILC2s在肺部和肠道。IL-33-induced气道炎症,这个理事会的控制ILC2激活和嗜酸性粒细胞浸润肺。先天免疫和表明不仅细胞因子,而且costimulatory通路这些涉及这个理事会,有助于调节ILC2池。封锁,目前在临床中评价抑制体液免疫反应,也可能目标天生的炎症电路。

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