Genetic overlap between diagnostic subtypes of ischemic stroke

Elizabeth G. Holliday; Matthew Traylor; Rainer Malik; Steve Bevan; Guido Falcone; Jemma C. Hopewell; Yu Ching Cheng; Ioana Cotlarciuc; Joshua C. Bis; Eric Boerwinkle; Giorgio B. Boncoraglio; Robert Clarke; John W. Cole; Myriam Fornage; Karen L. Furie; M. Arfan Ikram; Jim Jannes; Steven J. Kittner; Lisa F. Lincz; Jane M. Maguire; James F. Meschia; Thomas H. Mosley; Mike A. Nalls; Christopher Oldmeadow; Eugenio A. Parati; Bruce M. Psaty; Peter M. Rothwell; Sudha Seshadri; Rodney J. Scott; Pankaj Sharma; Cathie Sudlow; Kerri L. Wiggins; Bradford B. Worrall; Jonathan Rosand; Braxton D. Mitchell; Martin Dichgans; Hugh S. Markus; Christopher Levi; John Attia; Naomi R. Wray

doi:10.1161/STROKEAHA.114.007930

Genetic overlap between diagnostic subtypes of ischemic stroke

Elizabeth G. Holliday, Matthew Traylor, Rainer Malik, Steve Bevan, Guido Falcone, Jemma C. Hopewell, Yu Ching Cheng, Ioana Cotlarciuc, Joshua C. Bis, Eric Boerwinkle, Giorgio B. Boncoraglio, Robert Clarke, John W. Cole, Myriam Fornage, Karen L. Furie, M. Arfan Ikram, Jim Jannes, Steven J. Kittner, Lisa F. Lincz, Jane M. MaguireJames F. Meschia, Thomas H. Mosley, Mike A. Nalls, Christopher Oldmeadow, Eugenio A. Parati, Bruce M. Psaty, Peter M. Rothwell, Sudha Seshadri, Rodney J. Scott, Pankaj Sharma, Cathie Sudlow, Kerri L. Wiggins, Bradford B. Worrall, Jonathan Rosand, Braxton D. Mitchell, Martin Dichgans, Hugh S. Markus, Christopher Levi, John Attia, Naomi R. Wray

Resultado de la investigación: Article › revisión exhaustiva

31 Citas (Scopus)

Resumen

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. 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. Results: High genetic correlation was identified between LAA and SVD using linear mixed models (r_g=0.96, SE=0.47, P=9×10^-4) and profile scores (r_g=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. 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.

Idioma original	English (US)
Páginas (desde-hasta)	615-619
Número de páginas	5
Publicación	Stroke
Volumen	46
N.º	3
DOI	https://doi.org/10.1161/STROKEAHA.114.007930
Estado	Published - mar 1 2015
Publicado de forma externa	Sí

ASJC Scopus subject areas

Clinical Neurology
Cardiology and Cardiovascular Medicine
Advanced and Specialized Nursing

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10.1161/STROKEAHA.114.007930

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Holliday, E. G., Traylor, M., Malik, R., Bevan, S., Falcone, G., Hopewell, J. C., Cheng, Y. C., Cotlarciuc, I., Bis, J. C., Boerwinkle, E., Boncoraglio, G. B., Clarke, R., Cole, J. W., Fornage, M., Furie, K. L., Ikram, M. A., Jannes, J., Kittner, S. J., Lincz, L. F., ... Wray, N. R. (2015). Genetic overlap between diagnostic subtypes of ischemic stroke. Stroke, 46(3), 615-619. https://doi.org/10.1161/STROKEAHA.114.007930

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 2015, 'Genetic overlap between diagnostic subtypes of ischemic stroke', Stroke, vol. 46, n.º 3, pp. 615-619. https://doi.org/10.1161/STROKEAHA.114.007930

@article{835409a041eb47ab83b3fd59ce172c93,

title = "Genetic overlap between diagnostic subtypes of ischemic stroke",

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. 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. 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. 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.",

keywords = "Atherosclerosis, Genetic epidemiology, Lacunar stroke",

author = "Holliday, {Elizabeth G.} and Matthew Traylor and Rainer Malik and Steve Bevan and Guido Falcone and Hopewell, {Jemma C.} and Cheng, {Yu Ching} and Ioana Cotlarciuc and Bis, {Joshua C.} and Eric Boerwinkle and Boncoraglio, {Giorgio B.} and Robert Clarke and Cole, {John W.} and Myriam Fornage and Furie, {Karen L.} and Ikram, {M. Arfan} and Jim Jannes and Kittner, {Steven J.} and Lincz, {Lisa F.} and Maguire, {Jane M.} and Meschia, {James F.} and Mosley, {Thomas H.} and Nalls, {Mike A.} and Christopher Oldmeadow and Parati, {Eugenio A.} and Psaty, {Bruce M.} and Rothwell, {Peter M.} and Sudha Seshadri and Scott, {Rodney J.} and Pankaj Sharma and Cathie Sudlow and Wiggins, {Kerri L.} and Worrall, {Bradford B.} and Jonathan Rosand and Mitchell, {Braxton D.} and Martin Dichgans and Markus, {Hugh S.} and Christopher Levi and John Attia and Wray, {Naomi R.}",

note = "Publisher Copyright: {\textcopyright} 2015 American Heart Association, Inc.",

year = "2015",

month = mar,

day = "1",

doi = "10.1161/STROKEAHA.114.007930",

language = "English (US)",

volume = "46",

pages = "615--619",

journal = "Stroke",

issn = "0039-2499",

publisher = "Lippincott Williams and Wilkins",

number = "3",

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TY - JOUR

T1 - Genetic overlap between diagnostic subtypes of ischemic stroke

AU - Holliday, Elizabeth G.

AU - Traylor, Matthew

AU - Malik, Rainer

AU - Bevan, Steve

AU - Falcone, Guido

AU - Hopewell, Jemma C.

AU - Cheng, Yu Ching

AU - Cotlarciuc, Ioana

AU - Bis, Joshua C.

AU - Boerwinkle, Eric

AU - Boncoraglio, Giorgio B.

AU - Clarke, Robert

AU - Cole, John W.

AU - Fornage, Myriam

AU - Furie, Karen L.

AU - Ikram, M. Arfan

AU - Jannes, Jim

AU - Kittner, Steven J.

AU - Lincz, Lisa F.

AU - Maguire, Jane M.

AU - Meschia, James F.

AU - Mosley, Thomas H.

AU - Nalls, Mike A.

AU - Oldmeadow, Christopher

AU - Parati, Eugenio A.

AU - Psaty, Bruce M.

AU - Rothwell, Peter M.

AU - Seshadri, Sudha

AU - Scott, Rodney J.

AU - Sharma, Pankaj

AU - Sudlow, Cathie

AU - Wiggins, Kerri L.

AU - Worrall, Bradford B.

AU - Rosand, Jonathan

AU - Mitchell, Braxton D.

AU - Dichgans, Martin

AU - Markus, Hugh S.

AU - Levi, Christopher

AU - Attia, John

AU - Wray, Naomi R.

PY - 2015/3/1

Y1 - 2015/3/1

N2 - 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. 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. 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. 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.

AB - 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. 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. 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. 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.

KW - Atherosclerosis

KW - Genetic epidemiology

KW - Lacunar stroke

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UR - http://www.scopus.com/inward/citedby.url?scp=84943277974&partnerID=8YFLogxK

U2 - 10.1161/STROKEAHA.114.007930

DO - 10.1161/STROKEAHA.114.007930

M3 - Article

C2 - 25613305

AN - SCOPUS:84943277974

SN - 0039-2499

VL - 46

SP - 615

EP - 619

JO - Stroke

JF - Stroke

IS - 3

ER -

Genetic overlap between diagnostic subtypes of ischemic stroke

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ASJC Scopus subject areas

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