Leveraging global multi-ancestry meta-analysis in the study of idiopathic pulmonary fibrosis genetics.

The research of rare and devastating orphan diseases, such as idiopathic pulmonary fibrosis (IPF) has been limited by the rarity of the disease itself. The prognosis is poor-the prevalence of IPF is only approximately four times the incidence, limiting the recruitment of patients to trials and studies of the underlying biology. Global biobanking efforts can dramatically alter the future of IPF research. We describe a large-scale meta-analysis of IPF, with 8,492 patients and 1,355,819 population controls from 13 biobanks around the globe. Finally, we combine this meta-analysis with the largest available meta-analysis of IPF, reaching 11,160 patients and 1,364,410 population controls. We identify seven novel genome-wide significant loci, only one of which would have been identified if the analysis had been limited to European ancestry individuals. We observe notable pleiotropy across IPF susceptibility and severe COVID-19 infection and note an unexplained sex-heterogeneity effect at the strongest IPF locus MUC5B.

169 African American or Afro-Caribbean, African ancestry cases, 8,368 African American or Afro-Caribbean, African ancestry controls, 1,210 East Asian ancestry cases, 254,409 East Asian ancestry controls, 6,743 European ancestry cases, 1,056,693 European ancestry controls, 319 Hispanic or Latin American cases, 14,452 Hispanic or Latin American controls, 51 South Asian ancestry cases, 21,897 South Asian ancestry controls