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Subtypes of type I IFN differentially enhance cytokine expression by suboptimally stimulated CD4+ T cells

机译:I型干扰素的亚型不同增强通过有效刺激细胞因子表达CD4 + T细胞

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摘要

Human type I interferons (IFNs) include IFN-β and 12 subtypes of IFN-α. During viral infection, infiltrating memory CD4+ T cells are exposed to IFNs, but their impact on memory T-cell function is poorly understood. To address this, we pretreated PBMCs with different IFNs for 16 h before stimulation with Staphylococcus aureus enterotoxin B and measured cytokine expression by flow cytometry. IFN-α8 and -α10 most potently enhanced expression of IFN-γ, IL-2, and IL-4. Potency among the subtypes differed most at doses between 10 and 100 U/mL. While enhancement of IL-2 and IL-4 correlated with the time of preincubation with type I IFN, IFN-γ production was enhanced best when IFN-α was added immediately preceding or simultaneously with T-cell stimulation. Comparison of T-cell responses to multiple doses of Staphylococcus aureus enterotoxin B and to peptide libraries from RSV or CMV demonstrated that IFN-α best enhanced cytokine expression when CD4+ T cells were suboptimally stimulated. We conclude that type I IFNs enhance Th1 and Th2 function with dose dependency and subtype specificity, and best when T-cell stimulation is suboptimal. While type I IFNs may beneficially enhance CD4+ T-cell memory responses to vaccines or viral pathogens, they may also enhance the function of resident Th2 cells and exacerbate allergic inflammation.
机译:人类I型干扰素(IFN)包括干扰素-β和12个亚型干扰素-α。浸润CD4 + T细胞暴露于记忆干扰素,但它们对内存的影响t细胞功能了解甚少。进行预处理PBMCs不同干扰素16 h在刺激与金黄色葡萄球菌肠毒素B和测量细胞因子表达流式细胞术。增强表达干扰素-γ- 2、il - 4。效力的亚型不同剂量最大10至100 U /毫升。和il - 4 - 2相关的时间预培养与I型干扰素干扰素-γ生产是最好提高干扰素-α是说什么时候立即之前或同时使用t细胞的刺激。应对多个剂量的葡萄球菌葡萄球菌肠毒素B和肽库从RSV或巨细胞病毒表明干扰素-α最好增强细胞因子表达当CD4 + T细胞有效刺激。I型干扰素加强Th1、Th2函数剂量依赖和亚型特异性和最佳当t细胞刺激是次优的。我干扰素可能有益提高CD4 + t细胞记忆对疫苗或病毒的病原体,他们也可能增强居民的功能Th2细胞和加重过敏炎症。

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