Integrative approach identifies corticosteroid response variant in diverse populations with asthma

Abstract

Background: Although inhaled corticosteroid (ICS) medication is considered the cornerstone treatment for patients with persistent asthma, few ICS pharmacogenomic studies have involved nonwhite populations.

Objective: We sought to identify genetic predictors of ICS response in multiple population groups with asthma.

Methods: The discovery group comprised African American participants from the Study of Asthma Phenotypes and Pharmacogenomic Interactions by Race-Ethnicity (SAPPHIRE) who underwent 6 weeks of monitored ICS therapy (n = 244). A genome-wide scan was performed to identify single nucleotide polymorphism (SNP) variants jointly associated (ie, the combined effect of the SNP and SNP × ICS treatment interaction) with changes in asthma control. Top associations were validated by assessing the joint association with asthma exacerbations in 3 additional groups: African Americans (n = 803 and n = 563) and Latinos (n = 1461). RNA sequencing data from 408 asthmatic patients and 405 control subjects were used to examine whether genotype was associated with gene expression.

Results: One variant, rs3827907, was significantly associated with ICS-mediated changes in asthma control in the discovery set (P = 7.79 × 10^-8) and was jointly associated with asthma exacerbations in 3 validation cohorts (P = .023, P = .029, and P = .041). RNA sequencing analysis found the rs3827907 C-allele to be associated with lower RNASE2 expression (P = 6.10 × 10^-4). RNASE2 encodes eosinophil-derived neurotoxin, and the rs3827907 C-allele appeared to particularly influence ICS treatment response in the presence of eosinophilic inflammation (ie, high pretreatment eosinophil-derived neurotoxin levels or blood eosinophil counts).

Conclusion: We identified a variant, rs3827907, that appears to influence response to ICS treatment in multiple population groups and likely mediates its effect through eosinophils.

Keywords: EDDM3B; Pharmacogenetics; RNASE2; eosinophil-derived neurotoxin; eosinophils; transcriptome.

Figure 1.

Manhattan plot of the p-values from the genome wide association analysis of inhaled corticosteroid (ICS) response in the discovery set (n=244). Each p-value represents the statistical significance of jointly testing the contribution of both the SNP and SNP x ICS interaction terms. The Bonferroni-adjusted significance level (p=8.72×10⁻⁸) is shown as a solid gray line, and a pvalue threshold of 10⁻⁵ is shown as a dashed gray line.

Figure 2.

Relationship between rs3827907 genotype and absolute change in Asthma Control Test (ACT) composite score among African American participants in the SAPPHIRE cohort following 6 weeks of observed inhaled corticosteroid (ICS) treatment (n=244). Results are stratified by levels of patient ICS use (≤75% adherence was considered low use and >75% adherence was considered high use). Black lines connect the means for each group.

Figure 3.

Effect of baseline measures of eosinophil-derived neurotoxin (EDN) on relationship between rs3827907 C-allele carrier status and absolute change in Asthma Control Test (ACT) composite score among African American participants in the SAPPHIRE cohort following 6 weeks of observed inhaled corticosteroid (ICS) treatment (n=243). Results are stratified by levels of patient ICS use (≤75% adherence was considered low use and >75% adherence was considered high use) and baseline serum levels of EDN. Low and high EDN levels were defined as those ≤2.34 ng/mL and >2.34 ng/mL (the median level), respectively. Black lines connect the means for each group.

Figure 4.

Effect of baseline blood eosinophil counts on relationship between rs3827907 C-allele carrier status and absolute change in Asthma Control Test (ACT) composite score among African American participants in the SAPPHIRE cohort following 6 weeks of observed inhaled corticosteroid (ICS) treatment (n=113). Results are stratified by levels of patient ICS use (≤75% adherence was considered low use and >75% adherence was considered high use) and blood eosinophil counts measured before initiating ICS treatment. Low and high eosinophil counts were defined as those ≤222 cells/μL and >222 cells/ μL (the median level), respectively. Black lines connect the means for each group.