Multi-omic meta-analysis identifies functional signatures of airway microbiome in chronic obstructive pulmonary disease

微生物群 生物 基因组 转录组 代谢组 慢性阻塞性肺病 计算生物学 代谢组学 梭杆菌门 生物信息学 遗传学 基因 医学 基因表达 内科学 16S核糖体RNA 拟杆菌
作者
Zhang Wang,Yuqiong Yang,Zhengzheng Yan,Haiyue Liu,Boxuan Chen,Zhenyu Liang,Fengyan Wang,Bruce E. Miller,Ruth Tal‐Singer,Xinzhu Yi,Jintian Li,Martin R. Stämpfli,Hongwei Zhou,Christopher E. Brightling,James R. Brown,Martin Wu,Rongchang Chen,Wensheng Shu
出处
期刊:The ISME Journal [Springer Nature]
卷期号:14 (11): 2748-2765 被引量:54
标识
DOI:10.1038/s41396-020-0727-y
摘要

Abstract The interaction between airway microbiome and host in chronic obstructive pulmonary disease (COPD) is poorly understood. Here we used a multi-omic meta-analysis approach to characterize the functional signature of airway microbiome in COPD. We retrieved all public COPD sputum microbiome datasets, totaling 1640 samples from 16S rRNA gene datasets and 26 samples from metagenomic datasets from across the world. We identified microbial taxonomic shifts using random effect meta-analysis and established a global classifier for COPD using 12 microbial genera. We inferred the metabolic potentials for the airway microbiome, established their molecular links to host targets, and explored their effects in a separate meta-analysis on 1340 public human airway transcriptome samples for COPD. 29.6% of differentially expressed human pathways were predicted to be targeted by microbiome metabolism. For inferred metabolite–host interactions, the flux of disease-modifying metabolites as predicted from host transcriptome was generally concordant with their predicted metabolic turnover in microbiome, suggesting a synergistic response between microbiome and host in COPD. The meta-analysis results were further validated by a pilot multi-omic study on 18 COPD patients and 10 controls, in which airway metagenome, metabolome, and host transcriptome were simultaneously characterized. 69.9% of the proposed “microbiome-metabolite–host” interaction links were validated in the independent multi-omic data. Butyrate, homocysteine, and palmitate were the microbial metabolites showing strongest interactions with COPD-associated host genes. Our meta-analysis uncovered functional properties of airway microbiome that interacted with COPD host gene signatures, and demonstrated the possibility of leveraging public multi-omic data to interrogate disease biology.
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