Respiratory Research (May 2022)

Burden of rare coding variants reveals genetic heterogeneity between obese and non-obese asthma patients in the African American population

  • Yichuan Liu,
  • Hui-Qi Qu,
  • Jingchun Qu,
  • Xiao Chang,
  • Frank D. Mentch,
  • Kenny Nguyen,
  • Lifeng Tian,
  • Joseph Glessner,
  • Patrick M. A. Sleiman,
  • Hakon Hakonarson

DOI
https://doi.org/10.1186/s12931-022-02039-0
Journal volume & issue
Vol. 23, no. 1
pp. 1 – 6

Abstract

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Abstract Background Asthma is a complex condition largely attributed to the interactions among genes and environments as a heterogeneous phenotype. Obesity is significantly associated with asthma development, and genetic studies on obese vs. non-obese asthma are warranted. Methods To investigate asthma in the minority African American (AA) population with or without obesity, we performed a whole genome sequencing (WGS) study on blood-derived DNA of 4289 AA individuals, included 2226 asthma patients (1364 with obesity and 862 without obesity) and 2006 controls without asthma. The burden analysis of functional rare coding variants was performed by comparing asthma vs. controls and by stratified analysis of obese vs. non-obese asthma, respectively. Results Among the top 66 genes with P < 0.01 in the asthma vs. control analysis, stratified analysis by obesity showed inverse correlation of natural logarithm (LN) of P value between obese and non-obese asthma (r = − 0.757, P = 1.90E−13). Five genes previously reported in a genome-wide association study (GWAS) on asthma, including TSLP, SLC9A4, PSMB8, IGSF5, and IKZF4 were demonstrated association in the asthma vs. control analysis. The associations of IKZF4 and IGSF5 are only associated with obese asthma; and the association of SLC9A4 is only observed in non-obese asthma. In addition, the association of RSPH3 (the gene is related to primary ciliary dyskinesia) is observed in non-obese asthma. Conclusions These findings highlight genetic heterogeneity between obese and non-obese asthma in patients of AA ancestry.

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