Leveraging Health Systems Data to Characterize a Large Effect Variant Conferring Risk for Liver Disease in Puerto Ricans

Overview

Journal Am J Hum Genet

Publisher Cell Press

Specialty Genetics

Date 2021 Oct 22

PMID 34678161

Citations 4

Authors

Gillian M Belbin

Stephanie Rutledge

Tetyana Dodatko

Sinead Cullina

Michael C Turchin

Sumita Kohli

Denis Torre

Muh-Ching Yee

Christopher R Gignoux

Noura S Abul-Husn

Sander M Houten

Eimear E Kenny

Affiliations

Soon will be listed here.

Abstract

The integration of genomic data into health systems offers opportunities to identify genomic factors underlying the continuum of rare and common disease. We applied a population-scale haplotype association approach based on identity-by-descent (IBD) in a large multi-ethnic biobank to a spectrum of disease outcomes derived from electronic health records (EHRs) and uncovered a risk locus for liver disease. We used genome sequencing and in silico approaches to fine-map the signal to a non-coding variant (c.2784-12T>C) in the gene ABCB4. In vitro analysis confirmed the variant disrupted splicing of the ABCB4 pre-mRNA. Four of five homozygotes had evidence of advanced liver disease, and there was a significant association with liver disease among heterozygotes, suggesting the variant is linked to increased risk of liver disease in an allele dose-dependent manner. Population-level screening revealed the variant to be at a carrier rate of 1.95% in Puerto Rican individuals, likely as the result of a Puerto Rican founder effect. This work demonstrates that integrating EHR and genomic data at a population scale can facilitate strategies for understanding the continuum of genomic risk for common diseases, particularly in populations underrepresented in genomic medicine.

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