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Downregulated IL-21 Response and T Follicular Helper Cell Exhaustion Correlate with Compromised CD8 T Cell Immunity during Chronic Toxoplasmosis

机译:慢性弓形体病期间下调的IL-21反应和T卵泡辅助细胞的衰竭与CD8 T细胞免疫功能受损相关。

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摘要

CD8 T cells are important for maintaining the chronicity of Toxoplasma gondii infection. In a T. gondii encephalitis susceptible model, we recently demonstrated that CD4 T cells play an essential helper role in the maintenance of the effector response and CD8 T cell dysfunctionality was linked to CD4 T cell exhaustion. However, CD4 T cells are constituted of different subsets with various functions and the population(s) providing help to the CD8 T cells has not yet been determined. In the present study, T follicular helper cells (Tfh), which are known to be essential for B cell maturation and are one of the main sources of IL-21, were significantly increased during chronic toxoplasmosis. However, at week 7 p.i., when CD8 T cells are exhausted, the Tfh population exhibited increased expression of several inhibitory receptors and levels of IL-21 in the serum were decreased. The importance of IL-21 in the maintenance of CD8 T cells function after T. gondii infection was further demonstrated in IL-21R KO mouse model. Interestingly, while CD8 T cells from both knockout (KO) and wild-type mice expressed similar levels of PD-1, animals with defective IL-21 signaling exhibited lower polyfunctionality than wild-type controls. This reduced polyfunctional ability observed in CD8 T cells from KO mice was associated with a significant increase in other inhibitory receptors like Tim-3, LAG-3, and 2B4. Furthermore, the animals exhibited greater signs of Toxoplasma reactivation manifested by the reduced number of cysts and increased expression of tachyzoite (replicative form of the parasite) specific genes (SAG1 and ENO2) in the brain. Also, IL-21R KO mice displayed a higher frequency of tachyzoite-infected monocytes in the blood and spleen. Our findings suggest the importance of Tfh and IL-21 during chronic toxoplasmosis and establish a critical role for this cytokine in regulating CD8 T cell dysfunction by preventing the co-expression of multiple inhibitory receptors during chronic parasitic infection.
机译:CD8 T细胞对于维持弓形虫的慢性感染很重要。在刚地弓形虫脑炎易感模型中,我们最近证明CD4 T细胞在效应物反应的维持中起着重要的辅助作用,而CD8 T细胞功能障碍与CD4 T细胞衰竭有关。然而,CD4T细胞由具有各种功能的不同亚组构成,并且尚未确定向CD8T细胞提供帮助的群体。在本研究中,T卵泡辅助细胞(Tfh)被认为是B细胞成熟所必需的,并且是IL-21的主要来源之一,在慢性弓形体病期间显着增加。然而,在p.i.的第7周,当CD8 T细胞耗尽时,Tfh群体显示出几种抑制受体的表达增加,血清中的IL-21水平降低。 IL-21R KO小鼠模型进一步证明了弓形虫感染后IL-21在维持CD8 T细胞功能中的重要性。有趣的是,虽然来自敲除小鼠(KO)和野生型小鼠的CD8 T细胞表达相似的PD-1水平,但具有IL-21信号缺陷的动物却比野生型对照组的多功能性低。在来自KO小鼠的CD8 T细胞中观察到的这种降低的多功能能力与其他抑制性受体(如Tim-3,LAG-3和2B4)的显着增加有关。此外,这些动物表现出更大的弓形体再激活迹象,表现为囊肿数量减少和速殖子(寄生虫的复制形式)特异性基因(SAG1和ENO2)的表达增加。此外,IL-21R KO小鼠的血液和脾脏中被速殖子感染的单核细胞频率更高。我们的发现表明Tfh和IL-21在慢性弓形虫病中的重要性,并通过防止慢性寄生虫感染期间多种抑制性受体的共表达,在调节CD8 T细胞功能异常中为这种细胞因子发挥关键作用。

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