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TLR signaling in human antigen-presenting cells regulates MR1-dependent activation of MAIT cells

机译:TLR信号在人类抗原递呈细胞”调节MR1-dependent MAIT细胞的激活

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摘要

Mucosal-associated invariant T (MAIT) cells are an abundant innate-like T lymphocyte population that are enriched in liver and mucosal tissues. They are restricted by MR1, which presents antigens derived from a metabolic precursor of riboflavin synthesis, a pathway present in many microbial species, including commensals. Therefore, MR1-mediated MAIT cell activation must be tightly regulated to prevent inappropriate activation and immunopathology. Using an in vitro model of MR1-mediated activation of primary human MAIT cells, we investigated the mechanisms by which it is regulated. Uptake of intact bacteria by antigen presenting cells (APCs) into acidified endolysosomal compartments was required for efficient MR1-mediated MAIT cell activation, while stimulation with soluble ligand was inefficient. Consistent with this, little MR1 was seen at the surface of human monocytic (THP1) and B-cell lines. Activation with a TLR ligand increased the amount of MR1 at the surface of THP1 but not B-cell lines, suggesting differential regulation in different cell types. APC activation and NF-kappa B signaling were critical for MR1-mediated MAIT cell activation. In primary cells, however, prolonged TLR signaling led to downregulation of MR1-mediated MAIT cell activation. Overall, MR1-mediated MAIT cell activation is a tightly regulated process, dependent on integration of innate signals by APCs.
机译:Mucosal-associated T (MAIT)细胞是一个不变的丰富innate-like T淋巴细胞数量在肝脏和粘膜组织丰富。抗原MR1限制,这礼物吗来自核黄素的代谢前体在许多微生物合成、通路礼物物种,包括共生体。必须严格MR1-mediated MAIT细胞的激活防止不适当的激活和调节免疫病理反应。人类MAIT MR1-mediated激活主细胞,我们调查的机制是监管。抗原呈递细胞(apc)酸化endolysosomal隔间所需高效MR1-mediated MAIT细胞激活,而与可溶性配体刺激效率低下。在人类单核细胞的表面(THP1)和b细胞线。增加了MR1的表面THP1但不是b细胞线,建议微分调节在不同的细胞类型。APC和nf -κB信号被激活的关键MR1-mediated MAIT细胞活化。然而,在主要细胞,延长TLR信号的差别导致了对这些MR1-mediatedMAIT细胞活化。细胞的激活是一个严格监管的过程,依赖于先天信号的集成装甲运兵车。

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