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Cytip regulates dendritic-cell function in contact hypersensitivity

机译:Cytip调节树突状细胞的功能联系超敏反应

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摘要

Cytohesin-interacting protein (Cytip) is induced during dendritic cell (DC) maturation and in T cells upon activation. It has also been shown to be involved in the regulation of immune responses. Here, we evaluated the functional consequences of Cytip deficiency in DCs using Cytip knockout (KO) mice. No difference in DC subpopulations in the skin draining lymph nodes (LNs) was found between Cytip KO mice and their wild-type counterparts, excluding a role in DC development. To investigate the function of Cytip in DCs in vivo, we used 2,4,6-trinitrochlorobenzene (TNCB)-induced contact hypersensitivity (CHS) as a model system. In the sensitization as well as in the elicitation phase, DCs derived from Cytip KO mice induced an increased inflammatory reaction indicated by more pronounced ear swelling. Furthermore, IL-12 production was increased in Cytip KO bone marrow-derived DCs (BMDCs) after CpG stimulation. Additionally, Cytip-deficient DCs loaded with ovalbumin induced stronger proliferation of antigen-specific CD4 + and CD8 + T cells in vitro. Finally, migration of skin DCs was not altered after TNCB application due to Cytip deficiency. Taken together, these data suggest a suppressive function for Cytip in mouse DCs in limiting immune responses.
机译:Cytohesin-interacting蛋白质(Cytip)是诱导在树突状细胞(DC)的成熟和T细胞活化。参与免疫的规定响应。Cytip缺乏症在DCs中使用的后果Cytip淘汰赛(KO)老鼠。亚种群在皮肤上淋巴结(LNs)被发现Cytip KO小鼠和他们之间的关系野生型相比,不含直流发展。在DCs体内,我们使用2、4、6-trinitrochlorobenzene TNCB全身接触过敏(CHS)作为一个模型系统。在敏化以及启发阶段,DCs来自Cytip KO小鼠诱导炎症反应增加显示更明显耳肿胀。此外,白介素产量增加Cytip KO骨骨髓来源DCs (BMDCs)之后CpG刺激。DCs富含卵白蛋白诱发更强增殖抗原特异的CD4 +和CD8 +T细胞在体外。TNCB应用程序由于后并没有改变吗Cytip缺乏症。建议Cytip抑制功能的鼠标DCs在限制免疫反应。

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