Genome-wide association study implicates novel loci and reveals candidate effector genes for longitudinal pediatric bone accrual through variant-to-gene mapping

Author:

Cousminer Diana L.,Wagley Yadav,Pippin James A.,Elhakeem Ahmed,Way Gregory P.,McCormack Shana E.,Chesi Alessandra,Mitchell Jonathan A.,Kindler Joseph M.,Baird Denis,Hartley April,Howe Laura,Kalkwarf Heidi J.,Lappe Joan M.,Lu Sumei,Leonard Michelle,Johnson Matthew E.,Hakonarson Hakon,Gilsanz Vicente,Shepherd John A.,Oberfield Sharon E.,Greene Casey S.,Kelly Andrea,Lawlor Deborah,Voight Benjamin F.ORCID,Wells Andrew D.,Zemel Babette S.,Hankenson Kurt,Grant Struan F. A.

Abstract

Introductory paragraphBone accrual impacts lifelong skeletal health, but genetic discovery has been hampered by cross-sectional study designs and uncertainty about target effector genes. Here, we captured this dynamic phenotype by modeling longitudinal bone accrual across 11,000 bone scans followed by genome-wide association studies (GWAS). We revealed 40 loci (35 novel), half residing in topological associated domains harboring known bone genes. Variant-to-gene mapping identified contacts between GWAS loci and nearby gene promoters, and siRNA knockdown of gene expression clarified the putative effector gene at three specific loci in two osteoblast cell models. The resulting target genes highlight the cell fate decision between osteogenic and adipogenic lineages as important in normal bone accrual.

Publisher

Cold Spring Harbor Laboratory

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