Novel Susceptibility Loci for Moyamoya Disease Revealed by a Genome-Wide Association Study
Author:
Duan Lian1, Wei Ling1, Tian Yanghua1, Zhang Zhengshan1, Hu Panpan1, Wei Qiang1, Liu Sugang1, Zhang Jun1, Wang Yuyang1, Li Desheng1, Yang Weizhong1, Zong Rui1, Xian Peng1, Han Cong1, Bao Xiangyang1, Zhao Feng1, Feng Jie1, Liu Wei1, Cao Wuchun1, Zhou Guoping1, Zhu Chunyan1, Yu Fengqiong1, Yang Weimin1, Meng Yu1, Wang Jingye1, Chen Xianwen1, Wang Yu1, Shen Bing1, Zhao Bing1, Wan Jinghai1, Zhang Fengyu1, Zhao Gang1, Xu Aimin1, Zhang Xuejun1, Liu Jianjun1, Zuo Xianbo1, Wang Kai1
Affiliation:
1. From the Department of Neurosurgery, 307 Hospital, PLA Center for Cerebral Vascular Disease, Clinical Colleague of Anhui Medical University, Beijing, China (L.D., Z.Z., S.L., D.L., W.Y., R.Z., P.X., C.H., X.B., F.Z., J.F.); Department of Neurology (L.W., Y.T., P.H., Q.W., J.Z., W.Y., Y.M., J.W., X.C., Y.W., K.W.) and Department of Dermatology (F.Z., X. Zhang, X. Zuo), First Affiliated Hospital of Anhui Medical University, Hefei, China; Department of Neurosurgery, Second Affiliated Hospital of Anhui...
Abstract
Background and Purpose—
Moyamoya disease (MMD) is a rare cerebral vasculopathy characterized by bilateral internal carotid artery stenosis and often leads to stroke in children or young adults. Although familial inheritance is well recognized, the genetic basis of MMD remains poorly understood.
Methods—
A 2-stage genome-wide association study was conducted involving 1492 cases and 5084 controls. In the discovery stage, logistic regression was used to test associations, and imputation was conducted based on genotyped single-nucleotide polymorphisms (SNPs). In the validation stage, the top significant SNPs were again genotyped in an independent cohort. Fixed-effects inverse variance-weighted meta-analysis was used in the combined discovery and validation samples. Furthermore, association analysis was conducted in subgroups using patient clinical data.
Results—
The study identified 10 novel risk loci with genome-wide significance (
P
<5×10
−8
) and confirmed a previously reported locus on 17q25. No significant SNP showed evidence of heterogeneity between the 2 stages. Cumulatively, these SNPs explained 14.76% of disease risk variance—a substantial proportion of the 39.02% of risk variance explained by all genome-wide genotyped SNPs. One SNP, rs9916351 in
RNF213
(
P
combined
=4.57×10
−54
; odds ratio, 1.96), showed a stronger genetic effect on early-onset than late-onset MMD (
P
=0.003). Two novel SNPs in genes regulating homocysteine metabolism, rs9651118 in
MTHFR
(
P
combined
=2.49×10
−19
; odds ratio, 0.65) and rs117353193 in
TCN2
(
P
combined
=6.15×10
−13
; odds ratio, 1.43), were associated with high-serum homocysteine in MMD cases. Additionally, another SNP associated with MMD (rs2107595 in
HDAC9
;
P
combined
=1.49×10
−29
; odds ratio, 1.64) was previously implicated in large-vessel disease. Tissue enrichment analysis showed that the genes of associated loci were highly expressed in the immune system (false discovery rate, <0.05).
Conclusions—
This study identifies several novel susceptibility genes for MMD. The association with homocysteine metabolism and the immune system enrichment of susceptibility gene expression suggest that therapeutic interventions targeting these pathways may be effective approaches for MMD treatment.
Publisher
Ovid Technologies (Wolters Kluwer Health)
Subject
Advanced and Specialised Nursing,Cardiology and Cardiovascular Medicine,Clinical Neurology
Cited by
72 articles.
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