首页> 外文期刊>Folia histochemica et cytobiologica >Bronchial macrophages in asthmatics reveal decreased CD16 expression and substantial levels of receptors for IL-10, but not IL-4 and IL-7.
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Bronchial macrophages in asthmatics reveal decreased CD16 expression and substantial levels of receptors for IL-10, but not IL-4 and IL-7.

机译:哮喘患者的支气管巨噬细胞显示CD16表达降低,IL-10受体水平显着升高,但IL-4和IL-7却没有。

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The role of different subpopulations of bronchial macrophages (BMs) in asthma pathogenesis has not yet been completely elucidated. In addition, little is known about potential in vivo responsiveness of BMs to pro- and anti-inflam-matory cytokines present in the bronchial milieu. We aimed to characterize asthmatic patients' BM subpopulations delineated by common markers of macrophage/monocyte cells, CD16 and CD14, and subsequently to analyze cytokine receptor expression on those subsets. Subjects included eighteen patients with moderate asthma (six steroid-naive and twelve steroid-treated) and ten healthy control subjects. Flow cytometry was used to analyze phenotypical features of BMs including expression of receptors for IL-10, IL-4 and IL-7. Exhaled nitric oxide analysis and induced sputum eosinophil counts were used to assess airway inflammation. BMs from both steroid-naive and steroid-treated asthmatic patients showed significantly decreased expression of CD16, as compared to healthy subjects' BMs.CD16, but not CD14, expression inversely correlated with exhaled nitric oxide levels and sputum eosinophilia. Short-term administration of inhaled cortiocosteroids (ICS) in steroid-naive asthmatic patients led to significant reduction of CD16 expression and enhancement of CD14 expression. Next, we analyzed the expression of receptors for IL-10, IL-4 and IL-7 on the surface of BM subpopulations characterized by different levels of CD14 and CD16 expression. We observed substantial levels of IL-10R on the surface of BMs collected from asthmatic and healthy subjects. Interestingly, IL-10R was found mostly on those macrophages that co-expressed CD14. In contrast, independently on co-expression of CD14, the levels of IL-4R and IL-7R on BMs were low in both asthmatic and healthy subjects. The results suggest that different BM subsets may be differentially involved in regulating the inflammatory response in allergic asthma.
机译:支气管巨噬细胞(BMs)的不同亚群在哮喘发病机理中的作用尚未完全阐明。另外,关于BM对支气管环境中存在的促炎和抗炎细胞因子的潜在体内应答性知之甚少。我们的目的是通过巨噬细胞/单核细胞,CD16和CD14的常见标志物描绘哮喘患者的BM亚群,并随后分析这些亚群上的细胞因子受体表达。受试者包括18例中度哮喘患者(6例未接受类固醇激素治疗和12例接受类固醇治疗)和10例健康对照受试者。流式细胞仪用于分析BMs的表型特征,包括IL-10,IL-4和IL-7受体的表达。呼出气一氧化氮分析和诱导的痰嗜酸性粒细胞计数用于评估气道炎症。与健康受试者的BM相比,未接受类固醇治疗和接受类固醇治疗的哮喘患者的BM均显示CD16的表达显着降低.CD16而非CD14的表达与呼出一氧化氮水平和痰嗜酸性粒细胞增多呈负相关。初次使用类固醇的哮喘患者短期吸入皮质类固醇激素(ICS)可导致CD16表达显着降低和CD14表达增强。接下来,我们分析了以CD14和CD16表达水平不同为特征的BM亚群表面IL-10,IL-4和IL-7受体的表达。我们观察到从哮喘和健康受试者收集的BMs表面上有大量IL-10R水平。有趣的是,IL-10R主要在共表达CD14的那些巨噬细胞上发现。相反,在哮喘和健康受试者中,独立于CD14的共表达,BMs上的IL-4R和IL-7R水平较低。结果表明,不同的BM亚型可能在调节过敏性哮喘的炎症反应中有差异。

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