Genetic Analyses of Blood Cell Structure for Biological and Pharmacological Inference

Author:

Akbari ParsaORCID,Vuckovic DraganaORCID,Jiang Tao,Kundu KousikORCID,Kreuzhuber Roman,Bao Erik L.ORCID,Mayer LouisaORCID,Collins Janine H.ORCID,Downes KateORCID,Georges Michel,Grassi LuigiORCID,Guerrero Jose A.ORCID,Kaptoge Stephen,Knight Julian C.ORCID,Meacham StuartORCID,Sambrook Jennifer,Seyres DenisORCID,Stegle OliverORCID,Verboon Jeffrey M.,Walter KlaudiaORCID,Watkins Nicholas A.,Danesh John,Roberts David J.ORCID,Di Angelantonio EmanueleORCID,Sankaran Vijay G.ORCID,Frontini MattiaORCID,Burgess StephenORCID,Kuijpers TacoORCID,Peters James E.ORCID,Butterworth Adam S.ORCID,Ouwehand Willem H.ORCID,Soranzo NicoleORCID,Astle William J.ORCID

Abstract

SUMMARYThousands of genetic associations with phenotypes of blood cells are known, but few are with phenotypes relevant to cell function. We performed GWAS of 63 flow-cytometry phenotypes, including measures of cell granularity, nucleic acid content, and reactivity, in 39,656 participants in the INTERVAL study, identifying 2,172 variant-trait associations. These include associations mediated by functional cellular structures such as secretory granules, implicated in vascular, thrombotic, inflammatory and neoplastic diseases. By integrating our results with epigenetic data and with signals from molecular abundance/disease GWAS, we infer the hematopoietic origins of population phenotypic variation and identify the transcription factor FOG2 as a regulator of plateletα-granularity. We show how flow cytometry genetics can suggest cell types mediating complex disease risk and suggest efficacious drug targets, presenting Daclizumab/Vedolizumab in autoimmune disease as positive controls. Finally, we add to existing evidence supporting IL7/IL7-R as drug targets for multiple sclerosis.

Publisher

Cold Spring Harbor Laboratory

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