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Comparative phenotypic and functional analysis of migratory dendritic cell subsets from human oral mucosa and skin

机译:人口腔黏膜和皮肤迁移性树突状细胞亚型的比较表型和功能分析

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摘要

Antigen exposure to oral mucosa is generally thought to lead to immune tolerance induction. However, very little is known about the subset composition and function of dendritic cells (DC) migrating from human oral mucosa. Here we show that migratory DC from healthy human gingival explants consist of the same phenotypic subsets in the same frequency distribution as DC migrating from human skin. The gingival CD1a+ Langerhans cell and interstitial DC subsets lacked CXCR4 expression in contrast to their cutaneous counterparts, pointing to different migration mechanisms, consistent with previous observations in constructed skin and gingival equivalents. Remarkably, without any exogenous conditioning, gingival explants released higher levels of inflammatory cytokines than human skin explants, resulting in higher DC migration rates and a superior ability of migrated DC to prime allogeneic T cells and to induce type-1 effector T cell differentiation. From these observations we conclude that rather than an intrinsic ability to induce T cell tolerance, DC migrating from oral mucosa may have a propensity to induce effector T cell immunity and maintain a high state of alert against possible pathogenic intruders in the steady state. These findings may have implications for oral immunization strategies.
机译:通常认为抗原暴露于口腔粘膜会导致免疫耐受诱导。但是,关于从人口腔粘膜迁移的树突状细胞(DC)的子集组成和功能了解甚少。在这里,我们显示健康人牙龈外植体的迁徙DC由与从人皮肤迁移的DC相同的频率分布的相同表型子集组成。与皮肤对应物相比,牙龈CD1a + 朗格汉斯细胞和间质DC亚群缺乏CXCR4表达,指出了不同的迁移机制,这与先前在人造皮肤和牙龈等效物中的观察结果一致。值得注意的是,在没有任何外源条件的情况下,牙龈外植体释放的炎症细胞因子水平高于人类皮肤外植体,从而导致更高的DC迁移速率,以及迁移DC引发异体T细胞和诱导1型效应子T细胞分化的卓越能力。从这些观察结果我们得出结论,从口腔粘膜迁移的DC可能不是诱导T细胞耐受的内在能力,而是倾向于诱导效应T细胞免疫,并在稳态下保持高度警惕,以防可能的病原体入侵。这些发现可能对口服免疫策略有影响。

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