Whole-genome sequencing in diverse subjects identifies genetic correlates of leukocyte traits: The NHLBI TOPMed program

全基因组关联研究 生物 遗传关联 遗传学 嗜酸性粒细胞 插补(统计学) 免疫学 单核苷酸多态性 基因型 基因 哮喘 缺少数据 计算机科学 机器学习
作者
Anna Mikhaylova,Caitlin McHugh,Linda M. Polfus,Laura M. Raffield,Meher Preethi Boorgula,Thomas W. Blackwell,Jennifer A. Brody,Jai Broome,Nathalie Chami,Ming-Huei Chen,Matthew P. Conomos,Corey Cox,Joanne E. Curran,Michelle Daya,Lynette Ekunwe,David C. Glahn,Nancy L. Heard‐Costa,Heather M. Highland,Brian D. Hobbs,Yann Ilboudo,Deepti Jain,Leslie A. Lange,Tyne W. Miller‐Fleming,Nancy Min,Jee-Young Moon,Michael Preuss,Jonathon Rosen,Kathleen A. Ryan,Albert V. Smith,Quan Sun,Praveen Surendran,Paul S. de Vries,Klaudia Walter,Zhe Wang,Marsha M. Wheeler,Lisa R. Yanek,Xue Zhong,Gonçalo R. Abecasis,Laura Almasy,Kathleen C. Barnes,Terri H. Beaty,Lewis C. Becker,John Blangero,Eric Boerwinkle,Adam S. Butterworth,Sameer Chavan,Michael H. Cho,Hélène Choquet,Adolfo Correa,Nancy J. Cox,Dawn L. DeMeo,Nauder Faraday,Myriam Fornage,Robert E. Gerszten,Lifang Hou,Andrew D. Johnson,Eric Jorgenson,Robert C. Kaplan,Charles Kooperberg,Kousik Kundu,Cecelia Laurie,Guillaume Lettre,Joshua P. Lewis,Bingshan Li,Yun Li,Donald M. Lloyd‐Jones,Ruth J. F. Loos,Ani Manichaikul,Deborah A. Meyers,Braxton D. Mitchell,Alanna C. Morrison,Debby Ngo,Deborah A. Nickerson,Suraj S. Nongmaithem,Kari E. North,Jeffrey R. O’Connell,Victor E. Ortega,Nathan Pankratz,James A. Perry,Bruce M. Psaty,Stephen S. Rich,Nicole Soranzo,Jerome I. Rotter,Edwin K. Silverman,Nicholas L. Smith,Hua Tang,Russell P. Tracy,Timothy A. Thornton,Ramachandran S. Vasan,Joe Zein,Rasika A. Mathias,Alexander P. Reiner,Paul L. Auer
出处
期刊:American Journal of Human Genetics [Elsevier]
卷期号:108 (10): 1836-1851 被引量:16
标识
DOI:10.1016/j.ajhg.2021.08.007
摘要

Many common and rare variants associated with hematologic traits have been discovered through imputation on large-scale reference panels. However, the majority of genome-wide association studies (GWASs) have been conducted in Europeans, and determining causal variants has proved challenging. We performed a GWAS of total leukocyte, neutrophil, lymphocyte, monocyte, eosinophil, and basophil counts generated from 109,563,748 variants in the autosomes and the X chromosome in the Trans-Omics for Precision Medicine (TOPMed) program, which included data from 61,802 individuals of diverse ancestry. We discovered and replicated 7 leukocyte trait associations, including (1) the association between a chromosome X, pseudo-autosomal region (PAR), noncoding variant located between cytokine receptor genes (CSF2RA and CLRF2) and lower eosinophil count; and (2) associations between single variants found predominantly among African Americans at the S1PR3 (9q22.1) and HBB (11p15.4) loci and monocyte and lymphocyte counts, respectively. We further provide evidence indicating that the newly discovered eosinophil-lowering chromosome X PAR variant might be associated with reduced susceptibility to common allergic diseases such as atopic dermatitis and asthma. Additionally, we found a burden of very rare FLT3 (13q12.2) variants associated with monocyte counts. Together, these results emphasize the utility of whole-genome sequencing in diverse samples in identifying associations missed by European-ancestry-driven GWASs.

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