Journal
BMC MEDICAL GENOMICS
Volume 7, Issue -, Pages -Publisher
BMC
DOI: 10.1186/1755-8794-7-48
Keywords
Genome-wide association study; Allergic rhinitis; Coexpression network; Expression single-nucleotide polymorphism; Coexpression module; Pathway; Mitochondria; Hay fever; Allergy
Categories
Funding
- National Institutes of Allergy and Infectious Disease [K08AI093538, AI070503, AI079139, AI061774, AI077439]
- National Heart, Lung, and Blood Institute [HL101651, HL087665, HL085197, HL072414, HL49596, HL064307, HL064313, HL075419, HL65899, HL083069, HL066289, HL101543, HL079055, HL087699, HL061768, HL076647, P30ES007048, P01ES011627, HL087680, HL078885, HL088133, HL069167]
- National Institute of Diabetes and Digestive and Kidney Diseases [DK064695]
- National Institutes of Environmental Health Sciences [ES020801, ES022719, ES007048, ES009581, R826708, RD831861, ES011627, ES015794]
- Division of Intramural Research of National Institutes of Health [Z01 ES049019]
- American Asthma Foundation
- Fund for Henry Ford Hospital
- Mary Beryl Patch Turnbull Scholar Program
- Flight Attendant Medical Research Institute (FAMRI)
- RWJF Amos Medical Faculty Development Award
- Sandler Foundation
- Fundacion Ramon Areces
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Background: Allergic rhinitis is a common disease whose genetic basis is incompletely explained. We report an integrated genomic analysis of allergic rhinitis. Methods: We performed genome wide association studies (GWAS) of allergic rhinitis in 5633 ethnically diverse North American subjects. Next, we profiled gene expression in disease-relevant tissue (peripheral blood CD4+ lymphocytes) collected from subjects who had been genotyped. We then integrated the GWAS and gene expression data using expression single nucleotide (eSNP), coexpression network, and pathway approaches to identify the biologic relevance of our GWAS. Results: GWAS revealed ethnicity-specific findings, with 4 genome-wide significant loci among Latinos and 1 genome-wide significant locus in the GWAS meta-analysis across ethnic groups. To identify biologic context for these results, we constructed a coexpression network to define modules of genes with similar patterns of CD4+ gene expression (coexpression modules) that could serve as constructs of broader gene expression. 6 of the 22 GWAS loci with P-value <= 1x10(-6) tagged one particular coexpression module (4.0-fold enrichment, P-value 0.0029), and this module also had the greatest enrichment (3.4-fold enrichment, P-value 2.6 x 10(-24)) for allergic rhinitis-associated eSNPs (genetic variants associated with both gene expression and allergic rhinitis). The integrated GWAS, coexpression network, and eSNP results therefore supported this coexpression module as an allergic rhinitis module. Pathway analysis revealed that the module was enriched for mitochondrial pathways (8.6-fold enrichment, P-value 4.5 x 10(-72)). Conclusions: Our results highlight mitochondrial pathways as a target for further investigation of allergic rhinitis mechanism and treatment. Our integrated approach can be applied to provide biologic context for GWAS of other diseases.
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