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首页> 外文期刊>Protein & Cell >Contact-dependent delivery of IL-2 by dendritic cells to CD4 T cells in the contraction phase promotes their long-term survival
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Contact-dependent delivery of IL-2 by dendritic cells to CD4 T cells in the contraction phase promotes their long-term survival

机译:在收缩阶段的树突细胞对CD4 T细胞的IL-2接触依赖性递送促进了它们的长期存活

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摘要

Common γ chain cytokines are important for immune memory formation. Among them, the role of IL-2 remains to be fully explored. It has been suggested that this cytokine is critically needed in the late phase of primary CD4 T cell activation. Lack of IL-2 at this stage sets for a diminished recall response in subsequent challenges. However, as IL-2 peak production is over at this point, the source and the exact mechanism that promotes its production remain elusive. We report here that resting, previously antigen-stimulated CD4 T cells maintain a minimalist response to dendritic cells after their peak activation in vitro . This subtle activation event may be induced by DCs without overt presence of antigen and appears to be stronger if IL-2 comes from the same dendritic cells. This encounter reactivates a miniature IL-2 production and leads a gene expression profile change in these previously activated CD4 T cells. The CD4 T cells so experienced show enhanced reactivation intensity upon secondary challenges later on. Although mostly relying on in vitro evidence, our work may implicate a subtle programing for CD4 T cell survival after primary activation in vivo .
机译:常见的γ链细胞因子对免疫记忆形成很重要。其中,IL-2的作用仍有待全面探索。已经提示,这种细胞因子在原发性CD4 T细胞活化的后期批判性需要。在此阶段缺乏IL-2,以便在随后的挑战中进行减少的召回响应。然而,随着IL-2峰值生产在此时,源头和促进其生产的确切机制仍然难以捉摸。我们在此报告休息,以前抗原刺激的CD4 T细胞在体外峰激活后对树突细胞保持极简主义反应。这种微妙的激活事件可以通过DCS诱导而没有明显存在抗原,如果IL-2来自相同的树突细胞,则似乎更强。这遭遇重新激活微型IL-2生产,并在这些先前活化的CD4 T细胞中引入基因表达谱变化。 CD4 T细胞如此经历的次要挑战时显示出增强的再活化强度。虽然大多数依赖于体外证据,但我们的作品可能致力于体内原发性激活后对CD4 T细胞存活的微妙编程。

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