TY - JOUR
T1 - Whole-genome sequencing association analysis of quantitative red blood cell phenotypes
T2 - The NHLBI TOPMed program
AU - NHLBI Trans-Omics for Precision Medicine (TOPMed) Consortium
AU - Hu, Yao
AU - Stilp, Adrienne M.
AU - McHugh, Caitlin P.
AU - Rao, Shuquan
AU - Jain, Deepti
AU - Zheng, Xiuwen
AU - Lane, John
AU - Méric de Bellefon, Sébastian
AU - Raffield, Laura M.
AU - Chen, Ming Huei
AU - Yanek, Lisa R.
AU - Wheeler, Marsha
AU - Yao, Yao
AU - Ren, Chunyan
AU - Broome, Jai
AU - Moon, Jee Young
AU - de Vries, Paul S.
AU - Hobbs, Brian D.
AU - Sun, Quan
AU - Surendran, Praveen
AU - Brody, Jennifer A.
AU - Blackwell, Thomas W.
AU - Choquet, Hélène
AU - Ryan, Kathleen
AU - Duggirala, Ravindranath
AU - Heard-Costa, Nancy
AU - Wang, Zhe
AU - Chami, Nathalie
AU - Preuss, Michael H.
AU - Min, Nancy
AU - Ekunwe, Lynette
AU - Lange, Leslie A.
AU - Cushman, Mary
AU - Faraday, Nauder
AU - Curran, Joanne E.
AU - Almasy, Laura
AU - Kundu, Kousik
AU - Smith, Albert V.
AU - Gabriel, Stacey
AU - Rotter, Jerome I.
AU - Fornage, Myriam
AU - Lloyd-Jones, Donald M.
AU - Vasan, Ramachandran S.
AU - Smith, Nicholas L.
AU - North, Kari E.
AU - Boerwinkle, Eric
AU - Becker, Lewis C.
AU - Lewis, Joshua P.
AU - Abecasis, Goncalo R.
AU - Blangero, John
N1 - Publisher Copyright:
© 2021 American Society of Human Genetics
PY - 2021/5/6
Y1 - 2021/5/6
N2 - Whole-genome sequencing (WGS), a powerful tool for detecting novel coding and non-coding disease-causing variants, has largely been applied to clinical diagnosis of inherited disorders. Here we leveraged WGS data in up to 62,653 ethnically diverse participants from the NHLBI Trans-Omics for Precision Medicine (TOPMed) program and assessed statistical association of variants with seven red blood cell (RBC) quantitative traits. We discovered 14 single variant-RBC trait associations at 12 genomic loci, which have not been reported previously. Several of the RBC trait-variant associations (RPN1, ELL2, MIDN, HBB, HBA1, PIEZO1, and G6PD) were replicated in independent GWAS datasets imputed to the TOPMed reference panel. Most of these discovered variants are rare/low frequency, and several are observed disproportionately among non-European Ancestry (African, Hispanic/Latino, or East Asian) populations. We identified a 3 bp indel p.Lys2169del (g.88717175_88717177TCT[4]) (common only in the Ashkenazi Jewish population) of PIEZO1, a gene responsible for the Mendelian red cell disorder hereditary xerocytosis (MIM: 194380), associated with higher mean corpuscular hemoglobin concentration (MCHC). In stepwise conditional analysis and in gene-based rare variant aggregated association analysis, we identified several of the variants in HBB, HBA1, TMPRSS6, and G6PD that represent the carrier state for known coding, promoter, or splice site loss-of-function variants that cause inherited RBC disorders. Finally, we applied base and nuclease editing to demonstrate that the sentinel variant rs112097551 (nearest gene RPN1) acts through a cis-regulatory element that exerts long-range control of the gene RUVBL1 which is essential for hematopoiesis. Together, these results demonstrate the utility of WGS in ethnically diverse population-based samples and gene editing for expanding knowledge of the genetic architecture of quantitative hematologic traits and suggest a continuum between complex trait and Mendelian red cell disorders.
AB - Whole-genome sequencing (WGS), a powerful tool for detecting novel coding and non-coding disease-causing variants, has largely been applied to clinical diagnosis of inherited disorders. Here we leveraged WGS data in up to 62,653 ethnically diverse participants from the NHLBI Trans-Omics for Precision Medicine (TOPMed) program and assessed statistical association of variants with seven red blood cell (RBC) quantitative traits. We discovered 14 single variant-RBC trait associations at 12 genomic loci, which have not been reported previously. Several of the RBC trait-variant associations (RPN1, ELL2, MIDN, HBB, HBA1, PIEZO1, and G6PD) were replicated in independent GWAS datasets imputed to the TOPMed reference panel. Most of these discovered variants are rare/low frequency, and several are observed disproportionately among non-European Ancestry (African, Hispanic/Latino, or East Asian) populations. We identified a 3 bp indel p.Lys2169del (g.88717175_88717177TCT[4]) (common only in the Ashkenazi Jewish population) of PIEZO1, a gene responsible for the Mendelian red cell disorder hereditary xerocytosis (MIM: 194380), associated with higher mean corpuscular hemoglobin concentration (MCHC). In stepwise conditional analysis and in gene-based rare variant aggregated association analysis, we identified several of the variants in HBB, HBA1, TMPRSS6, and G6PD that represent the carrier state for known coding, promoter, or splice site loss-of-function variants that cause inherited RBC disorders. Finally, we applied base and nuclease editing to demonstrate that the sentinel variant rs112097551 (nearest gene RPN1) acts through a cis-regulatory element that exerts long-range control of the gene RUVBL1 which is essential for hematopoiesis. Together, these results demonstrate the utility of WGS in ethnically diverse population-based samples and gene editing for expanding knowledge of the genetic architecture of quantitative hematologic traits and suggest a continuum between complex trait and Mendelian red cell disorders.
KW - base editing
KW - red blood cell traits
KW - whole-genome sequencing
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U2 - 10.1016/j.ajhg.2021.04.003
DO - 10.1016/j.ajhg.2021.04.003
M3 - Article
C2 - 33887194
AN - SCOPUS:85102361040
SN - 0002-9297
VL - 108
SP - 874
EP - 893
JO - American Journal of Human Genetics
JF - American Journal of Human Genetics
IS - 5
ER -