Whole Genome Sequence Association with E-selectin Levels Reveals Loss-of-function Variant in African Americans

Overview

Journal Hum Mol Genet

Specialties Genetics
Molecular Biology

Date 2018 Oct 12

PMID 30307499

Citations 9

Authors

Linda M Polfus

Laura M Raffield

Marsha M Wheeler

Russell P Tracy

Leslie A Lange

Guillaume Lettre

Amanda Miller

Adolfo Correa

Russell P Bowler

Joshua C Bis

Shabnam Salimi

Nancy Swords Jenny

Nathan Pankratz

Biqi Wang

Michael H Preuss

Lisheng Zhou

Arden Moscati

Girish N Nadkarni

Ruth J F Loos

Xue Zhong

Bingshan Li

Jill M Johnsen

Deborah A Nickerson

Alex P Reiner

Paul L Auer

Affiliations

Soon will be listed here.

Abstract

E-selectin mediates the rolling of circulating leukocytes during inflammatory processes. Previous genome-wide association studies in European and Asian individuals have identified the ABO locus associated with E-selectin levels. Using Trans-Omics for Precision Medicine whole genome sequencing data in 2249 African Americans (AAs) from the Jackson Heart Study, we examined genome-wide associations with soluble E-selectin levels. In addition to replicating known signals at ABO, we identified a novel association of a common loss-of-function, missense variant in Fucosyltransferase 6 (FUT6; rs17855739,p.Glu274Lys, P = 9.02 × 10-24) with higher soluble E-selectin levels. This variant is considerably more common in populations of African ancestry compared to non-African ancestry populations. We replicated the association of FUT6 p.Glu274Lys with higher soluble E-selectin in an independent population of 748 AAs from the Women's Health Initiative and identified an additional pleiotropic association with vitamin B12 levels. Despite the broad role of both selectins and fucosyltransferases in various inflammatory, immune and cancer-related processes, we were unable to identify any additional disease associations of the FUT6 p.Glu274Lys variant in an electronic medical record-based phenome-wide association scan of over 9000 AAs.

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