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Opposing roles of endothelial and leukocyte-expressed IL-7Rα in the regulation of psoriasis-like skin inflammation

机译:内皮细胞和白细胞表达的IL-7Rα在调节牛皮癣样皮肤炎症中的作用相反

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摘要

The interleukin 7 receptor alpha chain (IL-7Rα) is predominately expressed by lymphocytes, and activation by its ligand IL-7 supports the development and maintenance of T cells and boosts T-cell mediated immunity. We recently reported that lymphatic endothelial cells (LECs) in dermal lymphatics also express IL-7 and its receptor chains (IL-7Rα and CD132) and that IL-7 supports lymphatic drainage. This suggested that activation of IL-7Rα signaling in lymphatics could exert inflammation-resolving activity, by promoting the clearance of excess tissue fluid. Here we investigated how the potentially opposing effects of IL-7Rα signaling in immune cells and in the lymphatic vasculature would affect the development and progression of psoriasis-like skin inflammation. We found that during acute and chronic skin inflammation mice with an endothelial-specific deletion of IL-7Rα (IL-7RαΔEC mice) developed more edema compared to control mice, as a consequence of impaired lymphatic drainage. However, systemic treatment of wild-type mice with IL-7 exacerbated edema and immune cell infiltration in spite of increasing lymphatic drainage, whereas treatment with IL-7Rα blocking antibody ameliorated inflammatory symptoms. These data identify IL-7Rα signaling as a new pathway in psoriasis-like skin inflammation and show that its pro-inflammatory effects on the immune compartment override its anti-inflammatory, drainage-enhancing effects on the endothelium.
机译:白细胞介素7受体α链(IL-7Rα)主要由淋巴细胞表达,其配体IL-7的激活支持T细胞的发育和维持,并增强T细胞介导的免疫力。我们最近报道了真皮淋巴管中的淋巴管内皮细胞(LEC)也表达IL-7及其受体链(IL-7Rα和CD132),并且IL-7支持淋巴引流。这表明激活淋巴管中的IL-7Rα信号可以通过促进多余组织液的清除而发挥消炎活性。在这里,我们研究了免疫细胞和淋巴管系统中IL-7Rα信号的潜在相反作用将如何影响牛皮癣样皮肤炎症的发生和发展。我们发现,在急性和慢性皮肤炎症过程中,由于淋巴引流受损,内皮细胞特异性缺失IL-7Rα的小鼠(IL-7RαΔEC小鼠)比对照组小鼠出现了更多的水肿。然而,尽管淋巴引流增加,但用IL-7全身性治疗野生型小鼠可加剧水肿和免疫细胞浸润,而用IL-7Rα阻断抗体治疗可减轻炎症症状。这些数据将IL-7Rα信号转导为牛皮癣样皮肤炎症中的新途径,并表明其对免疫区隔的促炎作用超过了对内皮的抗炎,引流增强作用。

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