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Bronchial gene expression signature associated with rate of subsequent FEV1 decline in individuals with and at risk of COPD

慢性阻塞性肺病 医学 基因表达 基因签名 基因 基因表达谱 微阵列 内科学 转录组 微阵列分析技术 生物信息学 免疫学 生物 遗传学
作者
Elizabeth J. Becker,Alen Faiz,Maarten van den Berge,Wim Timens,Pieter S. Hiemstra,Kristopher Clark,Gang Liu,Xiaohui Xiao,Yuriy O. Alekseyev,George O'connor,Stephen Lam,Avrum Spira,Marc E. Lenburg,Katrina Steiling
出处
期刊:Thorax [BMJ]
卷期号:77 (1): 31-39 被引量:11
标识
DOI:10.1136/thoraxjnl-2019-214476
摘要

Background COPD is characterised by progressive lung function decline. Leveraging prior work demonstrating bronchial airway COPD-associated gene expression alterations, we sought to determine if there are alterations associated with differences in the rate of FEV 1 decline. Methods We examined gene expression among ever smokers with and without COPD who at baseline had bronchial brushings profiled by Affymetrix microarrays and had longitudinal lung function measurements (n=134; mean follow-up=6.38±2.48 years). Gene expression profiles associated with the rate of FEV 1 decline were identified by linear modelling. Results Expression differences in 171 genes were associated with rate of FEV 1 decline (false discovery rate <0.05). The FEV 1 decline signature was replicated in an independent dataset of bronchial biopsies from patients with COPD (n=46; p=0.018; mean follow-up=6.76±1.32 years). Genes elevated in individuals with more rapid FEV 1 decline are significantly enriched among the genes altered by modulation of XBP1 in two independent datasets (Gene Set Enrichment Analysis (GSEA) p<0.05) and are enriched in mucin-related genes (GSEA p<0.05). Conclusion We have identified and replicated an airway gene expression signature associated with the rate of FEV 1 decline. Aspects of this signature are related to increased expression of XBP1-regulated genes, a transcription factor involved in the unfolded protein response, and genes related to mucin production. Collectively, these data suggest that molecular processes related to the rate of FEV 1 decline can be detected in airway epithelium, identify a possible indicator of FEV 1 decline and make it possible to detect, in an early phase, ever smokers with and without COPD most at risk of rapid FEV 1 decline.

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