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Impaired humoral immunity and tolerance in K14-VEGFR-3-Ig mice that lack dermal lymphatic drainage

机译:在缺乏真皮淋巴引流的K14-VEGFR-3-IG小鼠中受损的体液免疫和耐受性受损

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摘要

Lymphatic vessels transport interstitial fluid, soluble antigen, and immune cells from peripheral tissues to lymph nodes (LNs), yet the contribution of peripheral lymphatic drainage to adaptive immunity remains poorly understood. We examined immune responses to dermal vaccination and contact hypersensitivity (CHS) challenge in K14-VEGFR-3-Ig mice, which lack dermal lymphatic capillaries and experience markedly depressed transport of solutes and dendritic cells from the skin to draining LNs. In response to dermal immunization, K14-VEGFR-3-Ig mice produced lower antibody titers. In contrast, although delayed, T cell responses were robust after 21 days, including high levels of antigen-specific CD8+ T cells and production of IFN-γ, IL-4 and IL-10 upon restimulation. T cell-mediated CHS responses were strong in K14-VEGFR-3-Ig mice, but importantly, their ability to induce CHS tolerance in the skin was impaired. Additionally, one-year-old mice displayed multiple signs of autoimmunity. These data suggest that lymphatic drainage plays more important roles in regulating humoral immunity and peripheral tolerance than in effector T cell immunity.
机译:淋巴管将组织液,可溶性抗原和免疫细胞从周围组织转运到淋巴结(LNs),但对外周淋巴引流对适应性免疫的作用仍知之甚少。我们在K14-VEGFR-3-Ig小鼠中检查了对皮肤疫苗接种和接触超敏反应(CHS)挑战的免疫反应,这些小鼠缺乏真皮淋巴毛细血管,并经历了从皮肤到排水性LNs的溶质和树突状细胞运输明显降低。响应皮肤免疫,K14-VEGFR-3-Ig小鼠产生较低的抗体滴度。相反,尽管延迟,但T细胞反应在21天后仍然很强,包括高水平的抗原特异性CD8 + T细胞以及重新刺激后产生IFN-γ,IL-4和IL-10。 T细胞介导的CHS反应在K14-VEGFR-3-Ig小鼠中很强,但是重要的是,它们诱导皮肤中CHS耐受的能力受损。另外,一岁的小鼠表现出多种自身免疫迹象。这些数据表明,淋巴引流在调节体液免疫和外周耐受中起着比效应T细胞免疫更重要的作用。

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