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首页> 外文期刊>Clinical immunology: The official journal of the Clinical Immunology Society >Both perforin and FasL are required for optimal CD8 T cell control of autoreactive B cells and autoantibody production in parent-into-F1 lupus mice
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Both perforin and FasL are required for optimal CD8 T cell control of autoreactive B cells and autoantibody production in parent-into-F1 lupus mice

机译:Perforin和FasL都是最佳的CD8 T细胞控制自动反应性B细胞和母体入狼犬小鼠中的自身抗体生产所必需的

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摘要

To test the relative roles of perforin (pfp) vs. FasL in CTL control of autoreactive B cell expansion, we used the parent-into-F1 model of murine graft-vs.–host disease in which donor CD8 CTL prevent lupus like disease by eliminating activated autoreactive B cells. F1 mice receiving either pfp or FasL defective donor T cells exhibited an intermediate short-term phenotype. Pairing of purified normal CD4 T cells with either pfp or FasL defective CD8 T cell subsets resulted in impaired host B cell elimination and mild lupus like disease that was roughly equivalent in the two experimental groups. Thus, in addition to major roles in tumor and intracellular pathogen control, pfp mediated CD8 CTL killing plays a significant role in controlling autoreactive B cell expansion and lupus downregulation that is comparable to that mediated by FasL killing. Importantly, both pathways are required for optimal elimination of activated autoreactive B cells.
机译:为了测试穿孔素(PFP)与FasL在自动反应B细胞扩张的CTL控制中的相对作用,我们使用了母细胞移植物 - 与宿主疾病的亲肠梗成型模型,其中供体CD8 CTL防止狼疮 消除激活的自动反应性B细胞。 接受PFP或FASL有缺陷的供体T细胞的F1小鼠表现出中间短期表型。 用PFP或FASL缺陷CD8 T细胞亚族的纯化的正常CD4 T细胞配对导致宿主B细胞消除受损,类似于两种实验组的疾病,如疾病。 因此,除了肿瘤和细胞内病原体对照中的主要作用之外,PFP介导的CD8 CTL杀伤在控制自身反应性B细胞膨胀和狼疮下调方面发挥着显着作用,其与FASL杀伤介导的狼疮相当。 重要的是,两种途径都是最佳消除活性的自身反应性B细胞所必需的。

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