气道和全身干扰素反应失调会促使城市儿童哮喘病情加重。
Dysregulation of airway and systemic interferon responses promotes asthma exacerbations in urban children.
作者信息
Gaberino Courtney L, Altman Matthew C, Gill Michelle A, Bacharier Leonard B, Gruchalla Rebecca S, O'Connor George T, Kumar Rajesh, Khurana Hershey Gurjit K, Kattan Meyer, Liu Andrew H, Teach Stephen J, Zoratti Edward M, Becker Patrice M, Togias Alkis, Visness Cynthia, Gern James E, Busse William W, Jackson Daniel J
机构信息
Department of Pediatrics, University of Wisconsin School of Medicine and Public Health, Madison, Wis.
Immunology Division, Benaroya Research Institute Systems, and the Department of Medicine, University of Washington, Seattle, Wash.
出版信息
J Allergy Clin Immunol. 2025 May;155(5):1499-1509. doi: 10.1016/j.jaci.2024.12.1090. Epub 2025 Jan 7.
BACKGROUND
Determining why some upper respiratory illnesses provoke asthma exacerbations remains an unmet need.
OBJECTIVE
We sought to identify transcriptome-wide gene expression changes associated with colds that progress to exacerbation.
METHODS
Two hundred eight urban children (6-17 years) with exacerbation-prone asthma were prospectively monitored for up to 2 cold illnesses. Exacerbation illnesses (Ex), defined as colds leading to asthma exacerbations requiring systemic corticosteroids within 10 days, were compared to colds that resolved without exacerbation (Ex). Peripheral blood and nasal lavage samples were collected at baseline and during colds for RNA sequencing. Interferon gene expression was compared between Ex and Ex illnesses. Generalized additive modeling revealed interferon response kinetics. Multiple linear regression models compared interferon expression to clinical variables.
RESULTS
One hundred six participants were evaluated during 154 colds. There was greater upregulation of differentially expressed interferon genes during Ex illnesses compared to Ex. Ex illnesses had greater average and steeper rise in interferon expression. Within 3 days of illness, interferon expression was positively associated with nasal rhinovirus quantity (nasal: adjusted R = 0.48, P = .015; blood: adjusted R = 0.22, P = .013), and interferon expression was negatively associated with percentage predicted forced expiratory volume in 1 second (nasal: β = -0.010, P = .048; blood: β = -0.008, P = .023). Participants with lower baseline interferon expression had shorter time to exacerbation, higher risk for exacerbation with viral illnesses, and greater increase in interferon expression during viral colds (nasal: β = -0.80, P < .0001; blood: β = -0.75, P < .0001).
CONCLUSION
Dysregulated interferon responses are important contributors to asthma exacerbation risk in children. Low baseline interferon expression followed by greater upregulation of interferon pathways in airway and blood during respiratory illnesses increased exacerbation risk. Targeting this pathway in at-risk individuals holds promise for the personalized prevention of asthma exacerbations.
背景
确定为何某些上呼吸道疾病会引发哮喘加重仍是一项未满足的需求。
目的
我们试图识别与进展为加重的感冒相关的全转录组基因表达变化。
方法
对208名(6 - 17岁)易加重型哮喘的城市儿童进行前瞻性监测,观察多达2次感冒。将加重型疾病(Ex)定义为在10天内导致需要全身使用糖皮质激素的哮喘加重的感冒,并与未加重而痊愈的感冒(Ex)进行比较。在基线和感冒期间采集外周血和鼻腔灌洗样本用于RNA测序。比较Ex和Ex疾病之间的干扰素基因表达。广义相加模型揭示了干扰素反应动力学。多元线性回归模型将干扰素表达与临床变量进行比较。
结果
在154次感冒期间对106名参与者进行了评估。与Ex相比,Ex疾病期间差异表达的干扰素基因上调更明显。Ex疾病中干扰素表达的平均上升幅度更大且更陡峭。在患病3天内,干扰素表达与鼻腔鼻病毒数量呈正相关(鼻腔:调整后R = 0.48,P = 0.015;血液:调整后R = 0.22,P = 0.013),并且干扰素表达与预测的1秒用力呼气量百分比呈负相关(鼻腔:β = -0.010,P = 0.048;血液:β = -0.008,P = 0.023)。基线干扰素表达较低的参与者加重时间较短,病毒感染时加重风险较高,且病毒感冒期间干扰素表达增加幅度更大(鼻腔:β = -0.80,P < 0.0001;血液:β = -0.75,P < 0.0001)。
结论
干扰素反应失调是儿童哮喘加重风险的重要因素。呼吸道疾病期间气道和血液中基线干扰素表达较低,随后干扰素通路上调幅度更大,增加了加重风险。针对高危个体的这一通路进行干预有望实现哮喘加重的个性化预防。
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