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Dendritic cell – regulatory T-cell interaction

机译:树突状细胞–调节性T细胞相互作用

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The one of the main modes of homeostasis protection is maintaining the balance between antimicrobial immunological reactions and mechanisms involved in immune response suppression. The interaction between dendritic and T cells plays a crucial role in inducing both an immune response and immunological tolerance. Dendritic cells are also able to affect the differentiation, migration, and activation of CD4+ T cells using cell-to-cell contact and/or cytokine production. The proper cytokine microenvironment can influence the induction of FoxP3 transcription factor in T cells, determining the regulatory properties of these cells. However, it is still unclear what is more substantial for Treg induction: th e cytokines in the microenvironment, stimulation by a specific DC population, or the type of antigens presented by DC. Activated natural Treg as well as induced Treg cells use similar mechanisms to generate tolerance, for example by the production of such anti-inflammatory cytokines as TGF-β or IL-10 and by direct contact with target cells. Recently, some reports have described the possibility that Treg cells lose FoxP3 expression followed by loss of suppressive function directed against proliferating T lymphocytes.
机译:体内平衡保护的主要模式之一是维持抗菌素免疫反应与免疫反应抑制机制之间的平衡。树突状细胞与T细胞之间的相互作用在诱导免疫反应和免疫耐受中起着至关重要的作用。树突细胞还能够使用细胞间接触和/或细胞因子产生影响CD4 + T细胞的分化,迁移和激活。适当的细胞因子微环境可以影响T细胞中FoxP3转录因子的诱导,从而决定这些细胞的调节特性。然而,尚不清楚什么是更有意义的Treg诱导:微环境中的细胞因子,特定DC群体的刺激或DC呈递的抗原类型。活化的天然Treg细胞和诱导的Treg细胞使用类似的机制产生耐受性,例如通过产生抗炎细胞因子如TGF-β或IL-10并与靶细胞直接接触。最近,一些报道描述了Treg细胞丧失FoxP3表达,然后丧失针对增殖性T淋巴细胞的抑制功能的可能性。

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