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The impact of IL‐10 and IL‐17 on myeloid‐derived suppressor cells in vitro and in vivo in a murine model of asthma

机译:IL-10 和 IL-17 对小鼠哮喘模型中髓源性抑制细胞体外和体内的影响

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Abstract Myeloid‐derived suppressor cells (MDSCs) hold promise for clinical applications due to their immunosuppressive properties, particularly in the context of inflammation. In the present study, the number and immunosuppressive activity of MDSCs isolated from na?ve Il10?/?, Il17?/?, and WT mice as control, as well as from house dust mite extract (HDM)‐induced asthmatic Il10?/? and Il17?/? mice, were investigated. IL‐10 deficiency increased the number of polymorphonuclear (PMN)‐MDSCs in the lung, spleen, and bone marrow, without concurrent impairment of their suppressive activity in vitro. In the asthma model, the IL‐17 knockout was concomitant with a lower number and activity of monocytic (M)‐MDSCs and an altered inflammatory reaction with impaired lung function. Additionally, we found a higher baseline inflammation of the Il17?/? mice in the lung, manifested in increased airway resistance. We conclude that the impact of IL‐10 and IL‐17 deficiency on MDSCs differs in the context of inflammation. Accordingly, the in vitro experiments demonstrated an increased number of PMN‐MDSCs across tissues in Il10?/? mice, which indicates that IL‐10 might serve a pivotal role in preserving immune homeostasis under physiological circumstances. In the context of HDM‐induced airway inflammation, IL‐17 was found to be an important player in the suppression of pulmonary inflammation and regulation of M‐MDSCs.
机译:摘要 髓源性抑制细胞 (MDSC) 由于其免疫抑制特性,特别是在炎症情况下,有望在临床应用中应用。在本研究中,从作为对照的幼稚 Il10?/?、Il17?/?和 WT 小鼠以及从屋尘螨提取物 (HDM) 诱导的哮喘 Il10?/?和 Il17?/?小鼠,进行了调查。IL-10 缺陷增加了肺、脾和骨髓中多形核 (PMN)-MDSCs 的数量,而它们在体外的抑制活性没有同时受损。在哮喘模型中,IL-17 敲除伴随着单核细胞 (M)-MDSC 的数量和活性较低,炎症反应改变伴肺功能受损。此外,我们发现 Il17?/?小鼠在肺中,表现为气道阻力增加。我们得出结论,IL-10 和 IL-17 缺陷对 MDSC 的影响在炎症的背景下有所不同。因此,体外实验表明 Il10?/?小鼠,这表明 IL-10 可能在生理情况下保持免疫稳态方面发挥关键作用。在 HDM 诱导的气道炎症的情况下,发现 IL-17 在抑制肺部炎症和调节 M-MDSC 中起重要作用。

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