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首页> 外文期刊>Annals of the New York Academy of Sciences >The emergence of the IL-36 cytokine family as novel targets for inflammatory diseases
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The emergence of the IL-36 cytokine family as novel targets for inflammatory diseases

机译:IL-36细胞因子家族作为炎症性疾病的新靶标的出现

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摘要

The recently discovered interleukin (IL)-36 family of cytokines form part of the broader IL-1 family and are emerging as important mediators of inflammatory disease. The IL-36 subfamily consists of three ligands-IL-36 alpha, IL-36 beta, and IL-36 gamma-and the natural antagonist IL-36Ra. The cytokines exert their effects through a specific IL-36 receptor consisting of IL-36R and IL-1RAcP chains. IL-36 cytokines can direct both innate and adaptive immune responses by acting on parenchymal, stromal, and specific immune cell subsets. In humans, inactivating mutations in the gene encoding the IL-36R antagonist, which lead to unregulated IL-36R signaling, lead to an autoinflammatory condition termed deficiency of the IL-36R antagonist, which primarily manifests as a severe form of pustular psoriasis. While such discoveries have prompted deeper mechanistic studies highlighting the important role of IL-36 cytokines in psoriatic skin inflammation, it is now evident that IL-36 cytokines can also play important roles in inflammatory disorders in other organs, such as the gastrointestinal tract and the lungs. Given these emerging roles, strategies to specifically target the expression and activity of the IL-36 family have the potential to uncover novel therapeutic approaches aimed at treating inflammatory diseases in humans.
机译:最近发现的白细胞介素(IL)-36家族细胞因子构成了更广泛的IL-1家族的一部分,并且正在成为炎症性疾病的重要介质。 IL-36亚家族由三个配体-IL-36α,IL-36 beta和IL-36γ和天然拮抗剂IL-36Ra组成。细胞因子通过由IL-36R和IL-1RAcP链组成的特定IL-36受体发挥作用。 IL-36细胞因子可以通过作用于实质,基质和特异性免疫细胞亚群来指导先天性和适应性免疫反应。在人类中,编码IL-36R拮抗剂的基因失活突变导致IL-36R信号失控,导致称为IL-36R拮抗剂缺乏的自体炎症,主要表现为脓疱型牛皮癣的严重形式。虽然这些发现促使人们进行了更深入的机制研究,突出了IL-36细胞因子在牛皮癣皮肤炎症中的重要作用,但现在很明显,IL-36细胞因子在其他器官(例如胃肠道和皮肤)的炎症性疾病中也可以起重要作用。肺。考虑到这些新兴的作用,专门针对IL-36家族的表达和活性的策略具有发现旨在治疗人类炎症性疾病的新型治疗方法的潜力。

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