4.7 Article

Multiomics analysis identifies BIRC3 as a novel glucocorticoid response-associated gene

JOURNAL OF ALLERGY AND CLINICAL IMMUNOLOGY (2022)

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Journal

JOURNAL OF ALLERGY AND CLINICAL IMMUNOLOGY
Volume 149, Issue 6, Pages 1981-1991

Publisher

MOSBY-ELSEVIER
DOI: 10.1016/j.jaci.2021.11.025

Keywords

Asthma; ChIP-Seq; genome-wide association study; glucocorticoid response; glucocorticoid receptor; inhaled corticosteroids; integrative analysis; multiomics; transcriptomics

Categories

Allergy Immunology

Funding

  1. National Institutes of Health awards [R01 HL133433, R01 HL141992, P30ES013508, K23HL151819, R01 HL117004, X01HL134589, R01HL155024, R01MD010443, R01ES015794]
  2. Spanish Ministry of Science and Innovation [RYC-2015-17205, FPU19/02175]
  3. European Academy of Allergy and Clinical Immunology Medium-Term Research Fellowship 2021
  4. Sandler Family Foundation
  5. American Asthma Foundation
  6. RWJF Amos Medical Faculty Development Program
  7. Harry Wm. and DianaV. Hind Distinguished in Pharmaceutical Sciences II

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By integrating multiple omics data sets, this study identified the association of BIRC3 gene with the response to ICS treatment and possible genetic correlations in asthma patients.
Background: Inhaled corticosteroid (ICS) response among patients with asthma is influenced by genetics, but biologically actionable insights based on associations have not been found. Various glucocorticoid response omics data sets are available to interrogate their biological effects. Objective: We sought to identify functionally relevant ICS response genetic associations by integrating complementary multiomics data sets. Methods: Variants with P values less than 10(-4) from a previous ICS-response genome-wide association study were reranked on the basis of integrative scores determined from (1) glucocorticoid receptor- and (2) RNA polymerase II-binding regions inferred from ChIP-Seq data for 3 airway cell types, (3) glucocorticoid response element motifs, (4) differentially expressed genes in response to glucocorticoid exposure according to 20 transcriptomic data sets, and (5) expression quantitative trait loci from GTEx. Candidate variants were tested for association with ICS response and asthma in 6 independent studies. Results: Four variants had significant (q value < 0.05) multiomics integrative scores. These variants were in a locus consisting of 52 variants in high linkage disequilibrium (r(2) >= 0.8) near glucocorticoid receptor-binding sites by the gene BIRC3. Variants were also BIRC3 expression quantitative trait loci in lung, and 2 were within/near putative glucocorticoid response element motifs. BIRC3 had increased RNA polymerase II occupancy and gene expression, with glucocorticoid exposure in 2 ChIP-Seq and 13 transcriptomic data sets. Some BIRC3 variants in the 52-variant locus were associated (P < .05) with ICS response in 3 independent studies and others with asthma in 1 study. Conclusions: BIRC3 should be prioritized for further functional studies of ICS response.

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