Genetic Modifiers of Cystic Fibrosis Lung Disease Severity: Whole-Genome Analysis of 7,840 Patients.

Yi‐Hui Zhou ,Jia Wen,Weifang Liu ,Scott M Blackman ,Ronald L Gibson ,Kati J Buckingham ,Yun Li ,Fred A Wright ,Garry R Cutting ,Anna Faino ,Frankline Onchiri ,Quan Sun ,Kymberleigh A Pagel ,Kurt N Hetrick ,Margaret Rosenfeld ,Melis A Aksit ,Harriet Corvol ,Elizabeth Pugh ,Paul J Gallins ,Hua Liu ,Michael J Bamshad ,William W Gordon ,Joseph M Collaco ,Wanda K O’neal ,Rhonda G Pace ,Elizabeth Blue ,Karen S Raraigh ,Hong Dang ,Lisa J Strug ,Michael R Knowles

doi:10.1164/rccm.202209-1653oc

Abstract

Rationale: Lung disease is the major cause of morbidity and mortality in persons with cystic fibrosis (pwCF). Variability in CF lung disease has substantial non-CFTR (CF transmembrane conductance regulator) genetic influence. Identification of genetic modifiers has prognostic and therapeutic importance. Objectives: Identify genetic modifier loci and genes/pathways associated with pulmonary disease severity. Methods: Whole-genome sequencing data on 4,248 unique pwCF with pancreatic insufficiency and lung function measures were combined with imputed genotypes from an additional 3,592 patients with pancreatic insufficiency from the United States, Canada, and France. This report describes association of approximately 15.9 million SNPs using the quantitative Kulich normal residual mortality-adjusted (KNoRMA) lung disease phenotype in 7,840 pwCF using premodulator lung function data. Measurements and Main Results: Testing included common and rare SNPs, transcriptome-wide association, gene-level, and pathway analyses. Pathway analyses identified novel associations with genes that have key roles in organ development, and we hypothesize that these genes may relate to dysanapsis and/or variability in lung repair. Results confirmed and extended previous genome-wide association study findings. These whole-genome sequencing data provide finely mapped genetic information to support mechanistic studies. No novel primary associations with common single variants or rare variants were found. Multilocus effects at chr5p13 (SLC9A3/CEP72) and chr11p13 (EHF/APIP) were identified. Variant effect size estimates at associated loci were consistently ordered across the cohorts, indicating possible age or birth cohort effects. Conclusions: This premodulator genomic, transcriptomic, and pathway association study of 7,840 pwCF will facilitate mechanistic and postmodulator genetic studies and the development of novel therapeutics for CF lung disease.

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