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Death receptor 3 is essential for generating optimal protective CD4 1 T-cell immunity against Salmonella

机译:死亡受体3生成至关重要最优保护CD4 1 t细胞免疫力沙门氏菌

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摘要

The TNF receptor superfamily member death receptor 3 (DR3) exacerbates Th2- and Th17-cell-mediated inflammatory and autoimmune conditions, yet no role in host defence has been reported. Here, we examined the role of DR3 during infection with Salmonella enterica serovar Typhimurium. Infection resulted in protracted expression of the DR3 ligand TL1A but not the related TNF superfamily proteins OX40L or CD30L. TL1A expression was localized to splenic F4/80 + macrophages where S. enterica Typhimurium replicates, and temporally coincided with the onset of CD4 +-cell expansion. To address the relevance of the TL1A-DR3 interaction, we examined immune responses to S. enterica Typhimurium in mice lacking DR3. Infected DR3 -/- mice harboured reduced numbers of antigen-experienced and proliferating CD4 + T cells compared with WT mice. Furthermore, the frequency of IFN-γ + CD4 + T cells in DR3 -/- mice was lower throughout the time of bacterial clearance. Importantly, bacterial clearance, which is dependent on Th1 cells, was also impaired in DR3 -/- mice. This defect was intrinsic to CD4 + T cells as evidenced by an increase in bacterial burden in RAG2-deficient mice receiving DR3 -/- CD4 + T cells compared with WT CD4 +-cell recipients. These data establish for the first time a role for DR3 in a host defence responce.
机译:肿瘤坏死因子受体超家族成员死亡受体3 (DR3)加剧Th2和Th17-cell-mediated炎症和自身免疫状况,但没有在宿主防御作用报道。检查期间DR3感染的作用感染导致了旷日持久的表达DR3配体TL1A但不相关的肿瘤坏死因子总科蛋白质OX40L或CD30L。表达式是脾F4/80 +本地化巨噬细胞,血清培养的复制和暂时的正值发病的CD4 +细胞扩张。TL1A-DR3交互的相关性,我们检查美国血清的免疫反应沙门氏菌感染小鼠缺乏DR3。老鼠怀有的数量减少antigen-experienced和增殖CD4 + T细胞与WT老鼠。干扰素-γ+ CD4 + T细胞的频率在DR3 - / -老鼠是降低整个时间的细菌间隙。依赖Th1细胞,也是吗DR3 - / -小鼠受损。固有的CD4 + T细胞就是明证增加细菌在RAG2-deficient负担老鼠接受DR3 - / - CD4 + T细胞进行比较与WT CD4 +细胞。首次建立DR3的角色宿主的防御反应。

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