毛细支气管炎婴幼儿鼻咽脂质组学表型与儿童哮喘风险的相关性:一项多中心前瞻性研究。
Nasopharyngeal lipidomic endotypes of infants with bronchiolitis and risk of childhood asthma: a multicentre prospective study.
机构信息
Department of Emergency Medicine, Massachusetts General Hospital, Boston, Massachusetts, USA
Department of Emergency Medicine, Massachusetts General Hospital, Boston, Massachusetts, USA.
出版信息
Thorax. 2022 Nov;77(11):1059-1069. doi: 10.1136/thorax-2022-219016. Epub 2022 Jul 30.
BACKGROUND
Bronchiolitis is the leading cause of hospitalisation of US infants and an important risk factor for childhood asthma. Recent evidence suggests that bronchiolitis is clinically heterogeneous. We sought to derive bronchiolitis endotypes by integrating clinical, virus and lipidomics data and to examine their relationship with subsequent asthma risk.
METHODS
This is a multicentre prospective cohort study of infants (age <12 months) hospitalised for bronchiolitis. We identified endotypes by applying clustering approaches to clinical, virus and nasopharyngeal airway lipidomic data measured at hospitalisation. We then determined their longitudinal association with the risk for developing asthma by age 6 years by fitting a mixed-effects logistic regression model. To account for multiple comparisons of the lipidomics data, we computed the false discovery rate (FDR). To understand the underlying biological mechanism of the endotypes, we also applied pathway analyses to the lipidomics data.
RESULTS
Of 917 infants with bronchiolitis (median age, 3 months), we identified clinically and biologically meaningful lipidomic endotypes: (A) cinicallipid (n=263), (B) clinicallipid (n=281), (C) clinicallipid (n=212) and (D) clinicallipid (n=161). Endotype A infants were characterised by 'classic' clinical presentation of bronchiolitis. Profile D infants were characterised by a higher proportion of parental asthma, IgE sensitisation and rhinovirus infection and low sphingolipids (eg, sphingomyelins, ceramides). Compared with endotype A, profile D infants had a significantly higher risk of asthma (22% vs 50%; unadjusted OR, 3.60; 95% CI 2.31 to 5.62; p<0.001). Additionally, endotype D had a significantly lower abundance of polyunsaturated fatty acids (eg, docosahexaenoic acid; FDR=0.01). The pathway analysis revealed that sphingolipid metabolism pathway was differentially expressed in endotype D (FDR=0.048).
CONCLUSIONS
In this multicentre prospective cohort study of infants with bronchiolitis, integrated clustering of clinical, virus and lipidomic data identified clinically and biologically distinct endotypes that have a significantly differential risk for developing asthma.Delete.
背景
毛细支气管炎是导致美国婴儿住院的主要原因,也是儿童哮喘的重要危险因素。最近的证据表明,毛细支气管炎在临床上具有异质性。我们试图通过整合临床、病毒和气道脂质组学数据来得出毛细支气管炎的表型,并研究它们与随后发生哮喘风险的关系。
方法
这是一项多中心前瞻性队列研究,纳入了因毛细支气管炎住院的婴儿(<12 个月龄)。我们通过应用聚类方法对住院时测量的临床、病毒和鼻咽气道脂质组学数据进行分析,从而确定表型。然后,我们通过拟合混合效应逻辑回归模型来确定这些表型与 6 岁时发展为哮喘风险之间的纵向关系。为了对脂质组学数据进行多次比较的校正,我们计算了错误发现率(FDR)。为了了解表型的潜在生物学机制,我们还对脂质组学数据进行了途径分析。
结果
在 917 名患有毛细支气管炎的婴儿(中位年龄 3 个月)中,我们确定了具有临床和生物学意义的脂质组学表型:(A)临床脂质(n=263)、(B)临床脂质(n=281)、(C)临床脂质(n=212)和(D)临床脂质(n=161)。表型 A 的婴儿以“经典”毛细支气管炎临床表现为特征。表型 D 的婴儿以较高的父母哮喘、IgE 致敏和鼻病毒感染比例以及较低的鞘脂(如神经鞘磷脂、神经酰胺)为特征。与表型 A 相比,表型 D 的婴儿发生哮喘的风险显著更高(22%比 50%;未调整的 OR,3.60;95%CI,2.31 至 5.62;p<0.001)。此外,表型 D 的多不饱和脂肪酸(如二十二碳六烯酸)丰度显著降低(FDR=0.01)。途径分析显示,鞘脂代谢途径在表型 D 中差异表达(FDR=0.048)。
结论
在这项多中心前瞻性队列研究中,对临床、病毒和脂质组学数据的综合聚类确定了具有明显临床和生物学差异的表型,这些表型在发展为哮喘的风险方面存在显著差异。
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