Functional Variants in the Gene Confer Shared Effects on Risk for Crohn's Disease and Parkinson's Disease

Overview

Journal Sci Transl Med

Specialties General Medicine
Science

Date 2018 Jan 12

PMID 29321258

Citations 193

Authors

Ken Y Hui

Heriberto Fernandez-Hernandez

Jianzhong Hu

Adam Schaffner

Nathan Pankratz

Nai-Yun Hsu

Ling-Shiang Chuang

Shai Carmi

Nicole Villaverde

Xianting Li

Manual Rivas

Adam P Levine

Xiuliang Bao

Philippe R Labrias

Talin Haritunians

Darren Ruane

Kyle Gettler

Ernie Chen

Dalin Li

Elena R Schiff

Nikolas Pontikos

Nir Barzilai

Steven R Brant

Susan Bressman

Adam S Cheifetz

Lorraine N Clark

Mark J Daly

Robert J Desnick

Richard H Duerr

Seymour Katz

Todd Lencz

Richard H Myers

Harry Ostrer

Laurie Ozelius

Haydeh Payami

Yakov Peter

John D Rioux

Anthony W Segal

William K Scott

Mark S Silverberg

Jeffery M Vance

Iban Ubarretxena-Belandia

Tatiana Foroud

Gil Atzmon

Itsik Peer

Yiannis Ioannou

Dermot P B McGovern

Zhenyu Yue

Eric E Schadt

Judy H Cho

Inga Peter

Affiliations

Soon will be listed here.

Abstract

Crohn's disease (CD), a form of inflammatory bowel disease, has a higher prevalence in Ashkenazi Jewish than in non-Jewish European populations. To define the role of nonsynonymous mutations, we performed exome sequencing of Ashkenazi Jewish patients with CD, followed by array-based genotyping and association analysis in 2066 CD cases and 3633 healthy controls. We detected association signals in the gene that conferred risk for CD (N2081D variant, = 9.5 × 10) or protection from CD (N551K variant, tagging R1398H-associated haplotype, = 3.3 × 10). These variants affected CD age of onset, disease location, LRRK2 activity, and autophagy. Bayesian network analysis of CD patient intestinal tissue further implicated in CD pathogenesis. Analysis of the extended locus in 24,570 CD cases, patients with Parkinson's disease (PD), and healthy controls revealed extensive pleiotropy, with shared genetic effects between CD and PD in both Ashkenazi Jewish and non-Jewish cohorts. The N2081D CD risk allele is located in the same kinase domain as G2019S, a mutation that is the major genetic cause of familial and sporadic PD. Like the G2019S mutation, the N2081D variant was associated with increased kinase activity, whereas neither N551K nor R1398H variants on the protective haplotype altered kinase activity. We also confirmed that R1398H, but not N551K, increased guanosine triphosphate binding and hydrolyzing enzyme (GTPase) activity, thereby deactivating LRRK2. The presence of shared alleles in CD and PD provides refined insight into disease mechanisms and may have major implications for the treatment of these two seemingly unrelated diseases.

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