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单核细胞中较低的白细胞介素-7 受体表达会损害结核病患者的抗分枝杆菌效应功能。

Lower IL-7 Receptor Expression of Monocytes Impairs Antimycobacterial Effector Functions in Patients with Tuberculosis.

机构信息

Department of General Pediatrics, Medical Faculty, University Hospital Düsseldorf, Heinrich-Heine-University Düsseldorf, Düsseldorf, Germany.

Kumasi Centre for Collaborative Research in Tropical Medicine, Kumasi, Ghana.

出版信息

J Immunol. 2021 May 15;206(10):2430-2440. doi: 10.4049/jimmunol.2001256. Epub 2021 Apr 28.

Abstract

Altered monocyte differentiation and effector functions characterize immune pathogenesis of tuberculosis. IL-7 is an important factor for proliferation of T cells and impaired IL-7 sensitivity due to decreased IL-7 receptor α-chain (IL-7Rα) expression was found in patients with acute tuberculosis. Peripheral blood monocytes have moderate IL-7Rα expression and increased IL-7Rα levels were described for inflammatory diseases. In this study, we investigated a potential role of IL-7 and IL-7Rα expression for monocyte functions in tuberculosis. We analyzed the phenotype of monocytes in the blood from tuberculosis patients ( = 33), asymptomatic contacts of tuberculosis patients (contacts; = 30), and healthy controls ( = 20) from Ghana by multicolor flow cytometry. Mycobacterial components were analyzed for their capacity to induce IL-7Rα expression in monocytes. Functional effects of monocyte to IL-7 were measured during signaling and by using an antimycobacterial in vitro kill assay. Monocytes were more frequent in peripheral blood from patients with tuberculosis and especially higher proportions of CD14/CD16 (M1/2) monocytes with increased PD-L1 expression characterized acute tuberculosis. IL-7Rα expression was decreased particularly on M1/2 monocytes from patients with tuberculosis and aberrant low expression IL-7Rα correlated with high PD-L1 levels. Constitutive low pSTAT5 levels of monocytes ex vivo and impaired IL-7 response confirmed functionally decreased monocyte IL-7 sensitivity of patients with tuberculosis. Mycobacteria and mycobacterial cell wall components induced IL-7 receptor expression in monocytes and IL-7 boosted mycobacterial killing by monocyte-derived macrophages in vitro. We demonstrated impaired monocyte IL-7 receptor expression as well as IL-7 sensitivity in tuberculosis with potential effects on antimycobacterial effector functions.

摘要

单核细胞分化和效应功能改变是结核病免疫发病机制的特征。白细胞介素 7(IL-7)是 T 细胞增殖的重要因素,急性结核病患者中发现由于 IL-7 受体 α 链(IL-7Rα)表达减少而导致 IL-7 敏感性受损。外周血单核细胞具有中等水平的 IL-7Rα 表达,并且在炎症性疾病中描述了增加的 IL-7Rα 水平。在这项研究中,我们研究了 IL-7 和 IL-7Rα 表达在结核病中单核细胞功能中的潜在作用。我们通过多色流式细胞术分析了来自加纳的结核病患者(n=33)、结核病无症状接触者(接触者;n=30)和健康对照者(n=20)血液中的单核细胞表型。分析了分枝杆菌成分诱导单核细胞中 IL-7Rα 表达的能力。在信号转导过程中和使用抗分枝杆菌体外杀伤测定法测量了单核细胞对 IL-7 的功能效应。结核病患者外周血中单核细胞更为常见,特别是具有增加 PD-L1 表达的 CD14/CD16(M1/2)单核细胞比例更高,这是急性结核病的特征。结核病患者的单核细胞中 IL-7Rα 的表达尤其降低,并且异常低表达的 IL-7Rα 与高 PD-L1 水平相关。体外单核细胞的固有低 pSTAT5 水平和受损的 IL-7 反应证实了结核病患者单核细胞 IL-7 敏感性降低。分枝杆菌和分枝杆菌细胞壁成分诱导单核细胞中 IL-7 受体的表达,并且 IL-7 增强了单核细胞来源的巨噬细胞体外对分枝杆菌的杀伤作用。我们证明了结核病中单核细胞 IL-7 受体表达和 IL-7 敏感性受损,这可能对抗分枝杆菌效应功能产生影响。

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