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首页> 美国卫生研究院文献>American Journal of Physiology - Lung Cellular and Molecular Physiology >Macrophage/epithelial cell CCL2 contributes to rhinovirus-induced hyperresponsiveness and inflammation in a mouse model of allergic airways disease
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Macrophage/epithelial cell CCL2 contributes to rhinovirus-induced hyperresponsiveness and inflammation in a mouse model of allergic airways disease

机译:巨噬细胞/上皮细胞CCL2在过敏性气道疾病的小鼠模型中促进鼻病毒诱导的反应过度和炎症

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Human rhinovirus (HRV) infections lead to exacerbations of lower airways disease in asthmatic patients but not in healthy individuals. However, underlying mechanisms remain to be completely elucidated. We hypothesized that the Th2-driven allergic environment enhances HRV-induced CC chemokine production, leading to asthma exacerbations. Ovalbumin (OVA)-sensitized and -challenged mice inoculated with HRV showed significant increases in the expression of lung CC chemokine ligand (CCL)-2/monocyte chemotactic protein (MCP)-1, CCL4/macrophage inflammatory protein (MIP)-1β, CCL7/MCP-3, CCL19/MIP-3β, and CCL20/MIP3α compared with mice treated with OVA alone. Inhibition of CCL2 with neutralizing antibody significantly attenuated HRV-induced airways inflammation and hyperresponsiveness in OVA-treated mice. Immunohistochemical stains showed colocalization of CCL2 with HRV in epithelial cells and CD68-positive macrophages, and flow cytometry showed increased CCL2+, CD11b+ cells in the lungs of OVA-treated, HRV-infected mice. Compared with lung macrophages from naïve mice, macrophages from OVA-exposed mice expressed significantly more CCL2 in response to HRV infection ex vivo. Pretreatment of mouse lung macrophages and BEAS-2B human bronchial epithelial cells with interleukin (IL)-4 and IL-13 increased HRV-induced CCL2 expression, and mouse lung macrophages from IL-4 receptor knockout mice showed reduced CCL2 expression in response to HRV, suggesting that exposure to these Th2 cytokines plays a role in the altered HRV response. Finally, bronchoalveolar macrophages from children with asthma elaborated more CCL2 upon ex vivo exposure to HRV than cells from nonasthmatic patients. We conclude that CCL2 production by epithelial cells and macrophages contributes to HRV-induced airway hyperresponsiveness and inflammation in a mouse model of allergic airways disease and may play a role in HRV-induced asthma exacerbations.
机译:人鼻病毒(HRV)感染会导致哮喘患者下呼吸道疾病加重,但健康人不会。但是,底层机制仍有待完全阐明。我们假设Th2驱动的过敏环境增强了HRV诱导的CC趋化因子的产生,导致哮喘加重。接种HRV的卵清蛋白(OVA)致敏和攻击的小鼠显示肺CC趋化因子配体(CCL)-2 /单核细胞趋化蛋白(MCP)-1,CCL4 /巨噬细胞炎性蛋白(MIP)-1β的表达显着增加,与单独用OVA处理的小鼠相比,CCL7 / MCP-3,CCL19 /MIP-3β和CCL20 /MIP3α。用中和抗体抑制CCL2可显着减轻OVA治疗的小鼠中HRV诱导的气道炎症和高反应性。免疫组织化学染色显示上皮细胞和CD68阳性巨噬细胞中CCL2和HRV共定位,流式细胞仪显示OVA处理的肺中CCL2 + ,CD11b + 细胞增加,感染HRV的小鼠。与来自幼稚小鼠的肺巨噬细胞相比,来自暴露于OVA的小鼠的巨噬细胞对HRV感染的离体表达明显更多的CCL2。白介素(IL)-4和IL-13预处理小鼠肺巨噬细胞和BEAS-2B人支气管上皮细胞会增加HRV诱导的CCL2表达,而来自IL-4受体敲除小鼠的小鼠肺巨噬细胞则显示出对HRV的响应降低了CCL2表达,表明暴露于这些Th2细胞因子在改变的HRV反应中起作用。最后,来自哮喘患儿的支气管肺泡巨噬细胞在离体暴露于HRV后比非哮喘患者的细胞具有更多的CCL2。我们得出的结论是,在过敏性气道疾病的小鼠模型中,上皮细胞和巨噬细胞产生的CCL2有助于HRV诱导的气道高反应性和炎症,并且可能在HRV诱导的哮喘加重中发挥作用。

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