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Genetic overlap between diagnostic subtypes of ischemic stroke.

Authors :
Holliday EG
Traylor M
Malik R
Bevan S
Falcone G
Hopewell JC
Cheng YC
Cotlarciuc I
Bis JC
Boerwinkle E
Boncoraglio GB
Clarke R
Cole JW
Fornage M
Furie KL
Ikram MA
Jannes J
Kittner SJ
Lincz LF
Maguire JM
Meschia JF
Mosley TH
Nalls MA
Oldmeadow C
Parati EA
Psaty BM
Rothwell PM
Seshadri S
Scott RJ
Sharma P
Sudlow C
Wiggins KL
Worrall BB
Rosand J
Mitchell BD
Dichgans M
Markus HS
Levi C
Attia J
Wray NR
Source :
Stroke [Stroke] 2015 Mar; Vol. 46 (3), pp. 615-9. Date of Electronic Publication: 2015 Jan 22.
Publication Year :
2015

Abstract

Background and Purpose: Despite moderate heritability, the phenotypic heterogeneity of ischemic stroke has hampered gene discovery, motivating analyses of diagnostic subtypes with reduced sample sizes. We assessed evidence for a shared genetic basis among the 3 major subtypes: large artery atherosclerosis (LAA), cardioembolism, and small vessel disease (SVD), to inform potential cross-subtype analyses.<br />Methods: Analyses used genome-wide summary data for 12 389 ischemic stroke cases (including 2167 LAA, 2405 cardioembolism, and 1854 SVD) and 62 004 controls from the Metastroke consortium. For 4561 cases and 7094 controls, individual-level genotype data were also available. Genetic correlations between subtypes were estimated using linear mixed models and polygenic profile scores. Meta-analysis of a combined LAA-SVD phenotype (4021 cases and 51 976 controls) was performed to identify shared risk alleles.<br />Results: High genetic correlation was identified between LAA and SVD using linear mixed models (rg=0.96, SE=0.47, P=9×10(-4)) and profile scores (rg=0.72; 95% confidence interval, 0.52-0.93). Between LAA and cardioembolism and SVD and cardioembolism, correlation was moderate using linear mixed models but not significantly different from zero for profile scoring. Joint meta-analysis of LAA and SVD identified strong association (P=1×10(-7)) for single nucleotide polymorphisms near the opioid receptor μ1 (OPRM1) gene.<br />Conclusions: Our results suggest that LAA and SVD, which have been hitherto treated as genetically distinct, may share a substantial genetic component. Combined analyses of LAA and SVD may increase power to identify small-effect alleles influencing shared pathophysiological processes.<br /> (© 2015 American Heart Association, Inc.)

Details

Language :
English
ISSN :
1524-4628
Volume :
46
Issue :
3
Database :
MEDLINE
Journal :
Stroke
Publication Type :
Academic Journal
Accession number :
25613305
Full Text :
https://doi.org/10.1161/STROKEAHA.114.007930