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Development, cytokine profile and function of human interleukin 17-producing helper T cells.

机译:产生人白介素17的辅助T细胞的发育,细胞因子概况和功能。

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摘要

T(H)-17 cells are a distinct lineage of proinflammatory T helper cells that are essential for autoimmune disease. In mice, commitment to the T(H)-17 lineage is dependent on transforming growth factor-beta and interleukin 6 (IL-6). Here we demonstrate that IL-23 and IL-1beta induced the development of human T(H)-17 cells expressing IL-17A, IL-17F, IL-22, IL-26, interferon-gamma, the chemokine CCL20 and transcription factor RORgammat. In situ, T(H)-17 cells were identified by expression of the IL-23 receptor and the memory T cell marker CD45RO. Psoriatic skin lesions contained IL-23-producing dendritic cells and were enriched in the cytokines produced by human T(H)-17 cells that promote the production of antimicrobial peptides in human keratinocytes. Our data collectively indicate that human and mouse T(H)-17 cells require distinct factors during differentiation and that human T(H)-17 cells may regulate innate immunity in epithelial cells.
机译:T(H)-17细胞是自身免疫疾病必不可少的促炎性T辅助细胞谱系。在小鼠中,对T(H)-17谱系的承诺取决于转化生长因子β和白介素6(IL-6)。在这里,我们证明IL-23和IL-1beta诱导了表达TIL-17A,IL-17F,IL-22,IL-26,干扰素-γ,趋化因子CCL20和转录因子的人T(H)-17细胞的发育RORgammat。通过IL-23受体和记忆T细胞标志物CD45RO的表达原位鉴定T(H)-17细胞。银屑病皮肤损伤包含产生IL-23的树突状细胞,并富含人T(H)-17细胞产生的细胞因子,这些细胞因子可促进人角质形成细胞中抗菌肽的产生。我们的数据共同表明,人类和小鼠T(H)-17细胞在分化过程中需要不同的因子,而人类T(H)-17细胞可能会调节上皮细胞的先天免疫力。

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