Genetic regulation of gene expression in the lung identifies CST3 and CD22 as potential causal genes for airflow obstruction

Maxime Lamontagne, Wim Timens, Ke Hao, Yohan Bossé, Michel Laviolette, Katrina Steiling, Joshua D. Campbell, Christian Couture, Massimo Conti, Karen Sherwood, James C. Hogg, Corry Anke Brandsma, Maarten Van Den Berge, Andrew Sandford, Stephen Lam, Marc E. Lenburg, Avrum Spira, Peter D. Paré, David Nickle, Don D. SinDirkje S. Postma

Research output: Contribution to journalArticlepeer-review

23 Scopus citations


Background: COPD is a complex chronic disease with poorly understood pathogenesis. Integrative genomic approaches have the potential to elucidate the biological networks underlying COPD and lung function. We recently combined genome-wide genotyping and gene expression in 1111 human lung specimens to map expression quantitative trait loci (eQTL). Objective: To determine causal associations between COPD and lung function-associated single nucleotide polymorphisms (SNPs) and lung tissue gene expression changes in our lung eQTL dataset. Methods: We evaluated causality between SNPs and gene expression for three COPD phenotypes: FEV1% predicted, FEV1/FVC and COPD as a categorical variable. Different models were assessed in the three cohorts independently and in a meta-analysis. SNPs associated with a COPD phenotype and gene expression were subjected to causal pathway modelling and manual curation. In silico analyses evaluated functional enrichment of biological pathways among newly identified causal genes. Biologically relevant causal genes were validated in two separate gene expression datasets of lung tissues and bronchial airway brushings. Results: High reliability causal relations were found in SNP-mRNA-phenotype triplets for FEV1% predicted (n=169) and FEV1/FVC (n=80). Several genes of potential biological relevance for COPD were revealed. eQTL-SNPs upregulating cystatin C (CST3) and CD22 were associated with worse lung function. Signalling pathways enriched with causal genes included xenobiotic metabolism, apoptosis, protease-antiprotease and oxidant-antioxidant balance. Conclusions: By using integrative genomics and analysing the relationships of COPD phenotypes with SNPs and gene expression in lung tissue, we identified CST3 and CD22 as potential causal genes for airflow obstruction. This study also augmented the understanding of previously described COPD pathways.

Original languageEnglish
Pages (from-to)997-1004
Number of pages8
Issue number11
StatePublished - 1 Nov 2014


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