Trans-ethnic Meta-analysis of Genome-wide Association Studies for Hirschsprung Disease

Overview

Journal Hum Mol Genet

Specialties Genetics
Molecular Biology

Date 2016 Oct 6

PMID 27702942

Citations 27

Authors

Clara Sze-Man Tang

Hongsheng Gui

Ashish Kapoor

Jeong-Hyun Kim

Berta Luzon-Toro

Anna Pelet

Grzegorz Burzynski

Francesca Lantieri

Man-Ting So

Courtney Berrios

Hyoung Doo Shin

Raquel M Fernandez

Thuy-Linh Le

Joke B G M Verheij

Ivana Matera

Stacey S Cherny

Priyanka Nandakumar

Hyun Sub Cheong

Guillermo Antinolo

Jeanne Amiel

Jeong-Meen Seo

Dae-Yeon Kim

Jung-Tak Oh

Stanislas Lyonnet

Salud Borrego

Isabella Ceccherini

Robert M W Hofstra

Aravinda Chakravarti

Hyun-Young Kim

Pak Chung Sham

Paul K H Tam

Maria-Merce Garcia-Barcelo

Affiliations

Soon will be listed here.

Abstract

Hirschsprung disease (HSCR) is the most common cause of neonatal intestinal obstruction. It is characterized by the absence of ganglia in the nerve plexuses of the lower gastrointestinal tract. So far, three common disease-susceptibility variants at the RET, SEMA3 and NRG1 loci have been detected through genome-wide association studies (GWAS) in Europeans and Asians to understand its genetic etiologies. Here we present a trans-ethnic meta-analysis of 507 HSCR cases and 1191 controls, combining all published GWAS results on HSCR to fine-map these loci and narrow down the putatively causal variants to 99% credible sets. We also demonstrate that the effects of RET and NRG1 are universal across European and Asian ancestries. In contrast, we detected a European-specific association of a low-frequency variant, rs80227144, in SEMA3 [odds ratio (OR) = 5.2, P = 4.7 × 10-10]. Conditional analyses on the lead SNPs revealed a secondary association signal, corresponding to an Asian-specific, low-frequency missense variant encoding RET p.Asp489Asn (rs9282834, conditional OR = 20.3, conditional P = 4.1 × 10-14). When in trans with the RET intron 1 enhancer risk allele, rs9282834 increases the risk of HSCR from 1.1 to 26.7. Overall, our study provides further insights into the genetic architecture of HSCR and has profound implications for future study designs.

Citing Articles

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The interplay of common genetic variants NRG1 rs2439302 and RET rs2435357 increases the risk of developing Hirschsprung's disease.

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