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首页> 外文期刊>Clinical & developmental immunology. >Rapid development of Th2 activity during T cell priming.
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Rapid development of Th2 activity during T cell priming.

机译:T细胞启动期间Th2活性的快速发展。

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The paradigm of T helper-1 (Th-1) and Th-2 cells developing from non-committed naive precursors is firmly established. Th1 cells are characterized by IFNgamma production and, in mice, the selective switching to IgG2a. Conversely IL-4 production and selective switching to IgG1 and IgE characterize Th2 cells. Analysis of Th2 induction in vitro indicates that this polarization develops gradually in T cells activated by anti-CD3 in the presence of IL-4; conversely anti-CD3 and IFNgamma induce Th1 cells. In this report, we explore evidence that indicates that the T helper cell polarization in vivo cannot solely be explained by the cytokine environment. This is provided by studying the early acquisition of Th1 and Th2 activities during responses to a mixture of Th1 and Th2-inducing antigens. It is shown that these divergent forms of T cell help can rapidly develop in cells within a single lymph node. It is argued that early polarization to show Th-1 or Th-2 behavior can be induced by signals delivered duringcognate interaction between virgin T cells and dendritic cells, in the absence of type 1 or type 2 cytokines. This contrasts with the critical role of the cytokines in reinforcing the Th-phenotype and selectively expanding T helper clones.
机译:从无承诺的幼稚前体发育的T辅助细胞1(Th-1)和Th-2细胞的范例已得到牢固确立。 Th1细胞的特征是产生IFNγ,而在小鼠中则有选择地转换为IgG2a。相反,IL-4的产生以及向IgG1和IgE的选择性转换是Th2细胞的特征。在体外对Th2诱导的分析表明,这种极化在IL-4存在下在被抗CD3激活的T细胞中逐渐发展。相反,抗CD3和IFNgamma诱导Th1细胞。在本报告中,我们探索了证据表明体内T辅助细胞的极化不能仅由细胞因子环境来解释。这是通过研究在诱导Th1和Th2的抗原混合物反应期间Th1和Th2活性的早期获得而提供的。结果表明,这些不同形式的T细胞帮助可以在单个淋巴结内的细胞中迅速发育。有人认为,在没有1型或2型细胞因子的情况下,原始T细胞与树突状细胞之间的同源相互作用过程中传递的信号可以诱导显示Th-1或Th-2行为的早期极化。这与细胞因子在增强Th表型和选择性扩展T辅助克隆中的关键作用形成对比。

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