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白细胞介素-4介导人树突状细胞对白细胞介素-12p70产生的精细调节。

IL-4-mediated fine tuning of IL-12p70 production by human DC.

作者信息

Guenova Emmanuella, Volz Thomas, Sauer Karin, Kaesler Susanne, Müller Martin R, Wölbing Florian, Chen KoMing, Schwärzler Christoph, Brossart Peter, Röcken Martin, Biedermann Tilo

机构信息

Department of Dermatology, Eberhard Karls University, Tübingen, Germany.

出版信息

Eur J Immunol. 2008 Nov;38(11):3138-49. doi: 10.1002/eji.200838463.

Abstract

IL-4 is expressed at high levels in allergic diseases and dominates the early phases of multiple acquired immune responses. However, the precise role of IL-4 during early inflammation and its impact on the differentiation of newly recruited DC precursors remains elusive. In order to characterize the impact of IL-4 on the differentiation of human DC, we investigated the role of IL-4 on the differentiation of monocytes into DC. Human DC were differentiated from peripheral blood precursors under either low or high concentrations of IL-4. We analyzed their cytokine profile and capacity to polarize T-cell differentiation. Concentrations of 5 (low) and 50 (high) ng/mL IL-4 induced two distinct types of DC. DC differentiated under low-dose IL-4 (5 ng/mL) produced almost no IL-12p70, and primed naïve CD4+ T cells allowing IL-4 secretion and Th2 induction. In contrast, DC generated under high concentrations of IL-4 (50 ng/mL) produced large amounts of IL-12p70, low IL-10 and primed naïve CD4+ T cells to become Th1 cells. Thus, we demonstrate that the Th2 cell cytokine IL-4 decisively determines the phenotype of ongoing immune responses by orchestrating the functional phenotype of newly immigrating DC precursors.

摘要

白细胞介素-4(IL-4)在过敏性疾病中高水平表达,并在多种获得性免疫反应的早期阶段起主导作用。然而,IL-4在早期炎症过程中的精确作用及其对新招募的树突状细胞(DC)前体分化的影响仍不清楚。为了明确IL-4对人DC分化的影响,我们研究了IL-4在单核细胞分化为DC过程中的作用。在低浓度或高浓度IL-4条件下,使人DC从外周血前体分化而来。我们分析了它们的细胞因子谱以及极化T细胞分化的能力。5(低)和50(高)ng/mL的IL-4浓度诱导产生了两种不同类型的DC。在低剂量IL-4(5 ng/mL)条件下分化的DC几乎不产生IL-12p70,并启动初始CD4+ T细胞分泌IL-4并诱导Th2细胞分化。相反,在高浓度IL-4(50 ng/mL)条件下生成的DC产生大量IL-12p70、少量IL-10,并启动初始CD4+ T细胞分化为Th1细胞。因此,我们证明Th2细胞细胞因子IL-4通过协调新迁入的DC前体的功能表型,决定性地决定了正在进行的免疫反应的表型。

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