全血培养中单核细胞CD206上调与囊性纤维化患者肺功能相关:一项初步研究

Sonali Singh, Jessica Longmate, David Onion, Paul Williams, Miguel Camara, Alan R Smyth, Helen Barr, Luisa Martinez-Pomares
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引用次数: 0

摘要

慢性炎症在囊性纤维化(CF)的发病机制中占主导地位,有必要对CF免疫进行描述。全血培养为研究宿主环境中的免疫反应提供了一种经济有效且无创的方法。在这里,我们使用全血培养来研究CF (N=10)和对照组(N=8)在存在和不存在外源性巨噬细胞集落刺激因子(M-CSF)或粒细胞-巨噬细胞(GM)-CSF(含和不含白细胞介素(IL)-4)的情况下单核细胞(CD45+CD14+细胞)的分化潜力。在CF和对照培养中,CD45+CD14+细胞在所有情况下均上调HLA-DR表达,并且在GM-CSF(含和不含IL-4)存在时CD206升高,在GM-CSF和IL-4存在时CD209升高。在CF中,我们一致观察到CD206响应GM-CSF下调上调,CD206表达与肺功能呈正相关(FEV1)。这是培养单核细胞所特有的,在任何其他标记物上都没有看到。这些结果强调了全血培养在揭示与临床参数相关的分化单核细胞的细胞特征方面的潜力,这些特征可以指导CF中新的生物标志物的鉴定。
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CD206 upregulation in monocytes within whole blood cultures correlates with lung function in Cystic Fibrosis: a pilot study
Chronic inflammation dominates disease pathogenesis in Cystic Fibrosis (CF) and there is a need to characterise CF immunity. Whole blood cultures offer a cost-effective and non-invasive approach to investigate immune responses within the host environment. Here we used whole blood cultures to investigate the differentiation potential of monocytes (CD45+CD14+ cells) in CF (N=10) and controls (N=8) in the presence and absence of exogenous macrophage-colony stimulatory factor (M-CSF) or granulocyte-macrophage (GM)-CSF with and without interleukin (IL)-4. In CF and control cultures, CD45+CD14+ cells upregulated HLA-DR expression in all instances, and increased CD206 in the presence of GM-CSF with and without IL-4, and CD209 in the presence of GM-CSF and IL-4. In CF, we consistently observed reduced upregulation of CD206 in response to GM-CSF and a positive correlation between CD206 expression and lung function (FEV1). This was unique to cultured monocytes, and not seen with any other marker. These results highlight the potential of whole blood cultures to reveal cellular characteristics in differentiating monocytes related to clinical parameters that could guide the identification of novel biomarkers in CF.
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