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首页> 外文期刊>Blood: The Journal of the American Society of Hematology >Epidermis instructs skin homing receptor expression in human T cells
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Epidermis instructs skin homing receptor expression in human T cells

机译:表皮指示人类T细胞中皮肤归巢受体的表达

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摘要

The localization of memory T cells to human skin is essential for long-term immune surveillance and the maintenance of barrier integrity. Although the mechanisms controlling memory T-cell migration to peripheral tissues are poorly understood, the current paradigm includes the localized secretion of "imprinting" signals from tissue-resident dendritic cells in the draining lymph nodes. Here we show that CCR8 expression by newly activated naive T cells is regulated by skin-specific factor(s) derived primarily from epidermal keratinocytes, thereby providing a mechanism for the preferential expression of CCR8 by skin-resident memory T cells. Importantly, no such effects were observed after coculture with primary cells from skin-unrelated epithelia, including mesothelium and small intestine. The keratinocyte-derived CCR8-inducing factor(s) were soluble, and independent of vitaminsAand D. Furthermore, the induction of CCR8 under these conditions correlated with an increase in cutaneous lymphocyte-associated antigen expression. Our findings challenge current tissue homing paradigms, especially those involving CCR10, and emphasize the importance of steady-state epidermis rather than tissue-resident dendritic cells in controlling the localization of memory T cells within human skin.
机译:记忆T细胞在人体皮肤中的定位对于长期免疫监视和维持屏障完整性至关重要。尽管对控制记忆T细胞迁移至周围组织的机制了解甚少,但当前的范例包括局部引流来自排水淋巴结中组织驻留的树突状细胞的“印迹”信号。在这里,我们显示新激活的幼稚T细胞的CCR8表达受到主要源自表皮角质形成细胞的皮肤特异性因子的调节,从而为驻留在皮肤的记忆T细胞优先表达CCR8提供了一种机制。重要的是,与皮肤无关的上皮细胞(包括间皮和小肠)的原代细胞共培养后,没有观察到这种作用。角质形成细胞来源的CCR8诱导因子是可溶的,并且独立于维生素A和D。此外,在这些条件下CCR8的诱导与皮肤淋巴细胞相关抗原表达的增加有关。我们的发现挑战了当前的组织归巢范式,尤其是涉及CCR10的归巢范式,并强调了稳态表皮而不是驻留于组织中的树突状细胞在控制人类皮肤中记忆T细胞的定位中的重要性。

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