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首页> 外文期刊>The Journal of Experomental Medicine >Role of IL-17 and regulatory T lymphocytes in a systemic autoimmune disease
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Role of IL-17 and regulatory T lymphocytes in a systemic autoimmune disease

机译:IL-17和调节性T淋巴细胞在全身性自身免疫性疾病中的作用

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To explore the interactions between regulatory T cells and pathogenic effector cytokines, we have developed a model of a T cell–mediated systemic autoimmune disorder resembling graft-versus-host disease. The cytokine responsible for tissue inflammation in this disorder is interleukin (IL)-17, whereas interferon (IFN)-γ produced by Th1 cells has a protective effect in this setting. Because of the interest in potential therapeutic approaches utilizing transfer of regulatory T cells and inhibition of the IL-2 pathway, we have explored the roles of these in the systemic disease. We demonstrate that the production of IL-17 and tissue infiltration by IL-17–producing cells occur and are even enhanced in the absence of IL-2. Regulatory T cells favor IL-17 production but prevent the disease when administered early in the course by suppressing expansion of T cells. Thus, the pathogenic or protective effects of cytokines and the therapeutic capacity of regulatory T cells are crucially dependent on the timing and the nature of the disease.
机译:为了探索调节性T细胞与致病性效应细胞因子之间的相互作用,我们建立了类似于移植物抗宿主病的T细胞介导的系统性自身免疫疾病模型。在这种疾病中,负责组织炎症的细胞因子是白介素(IL)-17,而Th1细胞产生的干扰素(IFN)-γ在这种情况下具有保护作用。由于对潜在的利用调节性T细胞转移和抑制IL-2途径的治疗方法的兴趣,我们已经探索了它们在全身性疾病中的作用。我们证明,在没有IL-2的情况下,甚至会增强IL-17的产生和IL-17产生细胞的组织浸润。调节性T细胞有利于IL-17的产生,但在病程中早期给药时可通过抑制T细胞的扩增来预防这种疾病。因此,细胞因子的致病或保护作用以及调节性T细胞的治疗能力至关重要地取决于疾病的时机和性质。

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