• Am. J. Respir. Crit. Care Med. · Jan 2017

    Gene Expression Profiling in Blood Provides Reproducible Molecular Insights into Asthma Control.

    • Damien C Croteau-Chonka, Weiliang Qiu, Fernando D Martinez, Robert C Strunk, Robert F Lemanske, Andrew H Liu, Frank D Gilliland, Joshua Millstein, W James Gauderman, Carole Ober, Jerry A Krishnan, Steven R White, Edward T Naureckas, Dan L Nicolae, Kathleen C Barnes, Stephanie J London, Albino Barraza-Villarreal, Vincent J Carey, Scott T Weiss, Benjamin A Raby, and Asthma BioRepository for Integrative Genomic Exploration (Asthma BRIDGE) Consortium.
    • 1 Channing Division of Network Medicine and.
    • Am. J. Respir. Crit. Care Med. 2017 Jan 15; 195 (2): 179188179-188.

    RationaleMaintaining optimal symptom control remains the primary objective of asthma treatment. Better understanding of the biologic underpinnings of asthma control may lead to the development of improved clinical and pharmaceutical approaches.ObjectivesTo identify molecular pathways and interrelated genes whose differential expression was associated with asthma control.MethodsWe performed gene set enrichment analyses of asthma control in 1,170 adults with asthma, each with gene expression data derived from either whole blood (WB) or unstimulated CD4+ T lymphocytes (CD4), and a self-reported asthma control score representing either the preceding 6 months (chronic) or 7 days (acute). Our study comprised a discovery WB cohort (n = 245, chronic) and three independent, nonoverlapping replication cohorts: a second WB set (n = 448, acute) and two CD4 sets (n = 300, chronic; n = 77, acute).Measurements And Main ResultsIn the WB discovery cohort, we found significant overrepresentation of genes associated with asthma control in 1,106 gene sets from the Molecular Signatures Database (false discovery rate, <5%). Of these, 583 (53%) replicated in at least one replication cohort (false discovery rate, <25%). Suboptimal control was associated with signatures of eosinophilic and granulocytic inflammatory signals, whereas optimal control signatures were enriched for immature lymphocytic patterns. These signatures included two related biologic processes related to activation by TREM-1 (triggering receptor expressed on myeloid cells 1) and lipopolysaccharide.ConclusionsTogether, these results demonstrate the existence of specific, reproducible transcriptomic components in blood that vary with degree of asthma control and implicate a novel biologic target (TREM-1).

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