Genetic variants influencing elevated myeloperoxidase levels increase risk of stroke

Chia Ling Phuah; Tushar Dave; Rainer Malik; Miriam R. Raffeld; Alison M. Ayres; Joshua N. Goldstein; Anand Viswanathan; Steven M. Greenberg; Jeremiasz M. Jagiella; Björn M. Hansen; Bo Norrving; Jordi Jimenez-Conde; Jaume Roquer; Alexander Pichler; Christian Enzinger; Joan Montaner; Israel Fernandez-Cadenas; Arne Lindgren; Agnieszka Slowik; Reinhold Schmidt; Alessandro Biffi; Natalia Rost; Carl D. Langefeld; Hugh S. Markus; Braxton D. Mitchell; Brad B. Worrall; Steven J. Kittner; Daniel Woo; Martin Dichgans; Jonathan Rosand; Christopher D. Anderson

doi:10.1093/brain/awx220

Genetic variants influencing elevated myeloperoxidase levels increase risk of stroke

Chia Ling Phuah, Tushar Dave, Rainer Malik, Miriam R. Raffeld, Alison M. Ayres, Joshua N. Goldstein, Anand Viswanathan, Steven M. Greenberg, Jeremiasz M. Jagiella, Björn M. Hansen, Bo Norrving, Jordi Jimenez-Conde, Jaume Roquer, Alexander Pichler, Christian Enzinger, Joan Montaner, Israel Fernandez-Cadenas, Arne Lindgren, Agnieszka Slowik, Reinhold SchmidtAlessandro Biffi, Natalia Rost, Carl D. Langefeld, Hugh S. Markus, Braxton D. Mitchell, Brad B. Worrall, Steven J. Kittner, Daniel Woo, Martin Dichgans, Jonathan Rosand, Christopher D. Anderson

Research output: Contribution to journal › Article › peer-review

11 Scopus citations

Abstract

Primary intracerebral haemorrhage and lacunar ischaemic stroke are acute manifestations of progressive cerebral microvascular disease. Current paradigms suggest atherosclerosis is a chronic, dynamic, inflammatory condition precipitated in response to endothelial injury from various environmental challenges. Myeloperoxidase plays a central role in initiation and progression of vascular inflammation, but prior studies linking myeloperoxidase with stroke risk have been inconclusive. We hypothesized that genetic determinants of myeloperoxidase levels influence the development of vascular instability, leading to increased primary intracerebral haemorrhage and lacunar stroke risk. We used a discovery cohort of 1409 primary intracerebral haemorrhage cases and 1624 controls from three studies, an extension cohort of 12 577 ischaemic stroke cases and 25 643 controls from NINDSSiGN, and a validation cohort of 10 307 ischaemic stroke cases and 29 326 controls from METASTROKE Consortium with genome-wide genotyping to test this hypothesis. A genetic risk score reflecting elevated myeloperoxidase levels was constructed from 15 common single nucleotide polymorphisms identified from prior genome-wide studies of circulating myeloperoxidase levels (P55 - 10 6). This genetic risk score was used as the independent variable in multivariable regression models for association with primary intracerebral haemorrhage and ischaemic stroke subtypes. We used fixed effects meta-analyses to pool estimates across studies. We also used Cox regression models in a prospective cohort of 174 primary intracerebral haemorrhage survivors for association with intracerebral haemorrhage recurrence. We present effects of myeloperoxidase elevating single nucleotide polymorphisms on stroke risk per risk allele, corresponding to a one allele increase in the myeloperoxidase increasing genetic risk score. Genetic determinants of elevated circulating myeloperoxidase levels were associated with both primary intracerebral haemorrhage risk (odds ratio, 1.07, P = 0.04) and recurrent intracerebral haemorrhage risk (hazards ratio, 1.45, P = 0.006). In analysis of ischaemic stroke subtypes, the myeloperoxidase increasing genetic risk score was strongly associated with lacunar subtype only (odds ratio, 1.05, P = 0.0012). These results, demonstrating that common genetic variants that increase myeloperoxidase levels increase risk of primary intracerebral haemorrhage and lacunar stroke, directly implicate the myeloperoxidase pathway in the pathogenesis of cerebral small vessel disease. Because genetic variants are not influenced by environmental exposures, these results provide new support for a causal rather than bystander role for myeloperoxidase in the progression of cerebrovascular disease. Furthermore, these results support a rationale for chronic inflammation as a potential modifiable stroke risk mechanism, and suggest that immune-targeted therapies could be useful for treatment and prevention of cerebrovascular disease.

Original language	English
Pages (from-to)	2663-2672
Number of pages	10
Journal	Brain
Volume	140
Issue number	10
DOIs	https://doi.org/10.1093/brain/awx220
State	Published - Oct 1 2017

Keywords

genetics
inflammation
intracerebral haemorrhage
myeloperoxidase
stroke

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10.1093/brain/awx220

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Phuah, C. L., Dave, T., Malik, R., Raffeld, M. R., Ayres, A. M., Goldstein, J. N., Viswanathan, A., Greenberg, S. M., Jagiella, J. M., Hansen, B. M., Norrving, B., Jimenez-Conde, J., Roquer, J., Pichler, A., Enzinger, C., Montaner, J., Fernandez-Cadenas, I., Lindgren, A., Slowik, A., ... Anderson, C. D. (2017). Genetic variants influencing elevated myeloperoxidase levels increase risk of stroke. Brain, 140(10), 2663-2672. https://doi.org/10.1093/brain/awx220

@article{507f55f6eb1e4d7e8a4daed2544852ca,

title = "Genetic variants influencing elevated myeloperoxidase levels increase risk of stroke",

abstract = "Primary intracerebral haemorrhage and lacunar ischaemic stroke are acute manifestations of progressive cerebral microvascular disease. Current paradigms suggest atherosclerosis is a chronic, dynamic, inflammatory condition precipitated in response to endothelial injury from various environmental challenges. Myeloperoxidase plays a central role in initiation and progression of vascular inflammation, but prior studies linking myeloperoxidase with stroke risk have been inconclusive. We hypothesized that genetic determinants of myeloperoxidase levels influence the development of vascular instability, leading to increased primary intracerebral haemorrhage and lacunar stroke risk. We used a discovery cohort of 1409 primary intracerebral haemorrhage cases and 1624 controls from three studies, an extension cohort of 12 577 ischaemic stroke cases and 25 643 controls from NINDSSiGN, and a validation cohort of 10 307 ischaemic stroke cases and 29 326 controls from METASTROKE Consortium with genome-wide genotyping to test this hypothesis. A genetic risk score reflecting elevated myeloperoxidase levels was constructed from 15 common single nucleotide polymorphisms identified from prior genome-wide studies of circulating myeloperoxidase levels (P55 - 10 6). This genetic risk score was used as the independent variable in multivariable regression models for association with primary intracerebral haemorrhage and ischaemic stroke subtypes. We used fixed effects meta-analyses to pool estimates across studies. We also used Cox regression models in a prospective cohort of 174 primary intracerebral haemorrhage survivors for association with intracerebral haemorrhage recurrence. We present effects of myeloperoxidase elevating single nucleotide polymorphisms on stroke risk per risk allele, corresponding to a one allele increase in the myeloperoxidase increasing genetic risk score. Genetic determinants of elevated circulating myeloperoxidase levels were associated with both primary intracerebral haemorrhage risk (odds ratio, 1.07, P = 0.04) and recurrent intracerebral haemorrhage risk (hazards ratio, 1.45, P = 0.006). In analysis of ischaemic stroke subtypes, the myeloperoxidase increasing genetic risk score was strongly associated with lacunar subtype only (odds ratio, 1.05, P = 0.0012). These results, demonstrating that common genetic variants that increase myeloperoxidase levels increase risk of primary intracerebral haemorrhage and lacunar stroke, directly implicate the myeloperoxidase pathway in the pathogenesis of cerebral small vessel disease. Because genetic variants are not influenced by environmental exposures, these results provide new support for a causal rather than bystander role for myeloperoxidase in the progression of cerebrovascular disease. Furthermore, these results support a rationale for chronic inflammation as a potential modifiable stroke risk mechanism, and suggest that immune-targeted therapies could be useful for treatment and prevention of cerebrovascular disease.",

keywords = "genetics, inflammation, intracerebral haemorrhage, myeloperoxidase, stroke",

author = "Phuah, {Chia Ling} and Tushar Dave and Rainer Malik and Raffeld, {Miriam R.} and Ayres, {Alison M.} and Goldstein, {Joshua N.} and Anand Viswanathan and Greenberg, {Steven M.} and Jagiella, {Jeremiasz M.} and Hansen, {Bj{\"o}rn M.} and Bo Norrving and Jordi Jimenez-Conde and Jaume Roquer and Alexander Pichler and Christian Enzinger and Joan Montaner and Israel Fernandez-Cadenas and Arne Lindgren and Agnieszka Slowik and Reinhold Schmidt and Alessandro Biffi and Natalia Rost and Langefeld, {Carl D.} and Markus, {Hugh S.} and Mitchell, {Braxton D.} and Worrall, {Brad B.} and Kittner, {Steven J.} and Daniel Woo and Martin Dichgans and Jonathan Rosand and Anderson, {Christopher D.}",

note = "Funding Information: Our research was supported in part by the NIH-NINDS through K23NS086873, K23NS064052, R01NS059727 and P50NS061343, R01NS36695, U01NS069763, U01NS069208 and R01NS30678 and the NIH-NIA through R01AG26484. This work was further supported by grants from the German Federal Ministry of Education and Research(e:Med program e:AtheroSysMed), the FP7 European Union (EU) project CVgenes{at}target(261123), the DFG(CRC 1123, B3), the Corona Foundation, the Fondation Leducq (Transatlantic Network of Excellence on the Pathogenesis of Small Vessel Disease of the Brain). This project has received funding from the European Union{\textquoteright}s Horizon 2020 research and innovation program under grant agreement No 667375. Part of this project was funded by Generacion project (PI15/01978) Instituto de Salud Carlos III. Lund Stroke Register (LSR) has been supported by the Swedish Heart and Lung Foundation, Sk{\aa}ne University Hospital, Region Sk{\aa}ne, the Freemasons Lodge of Instruction EOS in Lund, King Gustaf V and Queen Victoria{\textquoteright}s Foundation, Lund University, and the Swedish Stroke Association, and Spain{\textquoteright}s Ministry of Health (Ministerio de Sanidad y Consumo, Instituto de Salud Carlos III FEDER, RD16/0019/0002. INVICTUS-PLUS). Hugh S. Markus is supported by an NIHR Senior Investigator award and his work is supported by the Cambridge University Hospital Comprehensive Biomedical Research Centre. Publisher Copyright: {\textcopyright} The Author (2017).",

year = "2017",

month = oct,

day = "1",

doi = "10.1093/brain/awx220",

language = "English",

volume = "140",

pages = "2663--2672",

journal = "Brain",

issn = "0006-8950",

number = "10",

}

Phuah, CL, Dave, T, Malik, R, Raffeld, MR, Ayres, AM, Goldstein, JN, Viswanathan, A, Greenberg, SM, Jagiella, JM, Hansen, BM, Norrving, B, Jimenez-Conde, J, Roquer, J, Pichler, A, Enzinger, C, Montaner, J, Fernandez-Cadenas, I, Lindgren, A, Slowik, A, Schmidt, R, Biffi, A, Rost, N, Langefeld, CD, Markus, HS, Mitchell, BD, Worrall, BB, Kittner, SJ, Woo, D, Dichgans, M, Rosand, J & Anderson, CD 2017, 'Genetic variants influencing elevated myeloperoxidase levels increase risk of stroke', Brain, vol. 140, no. 10, pp. 2663-2672. https://doi.org/10.1093/brain/awx220

TY - JOUR

T1 - Genetic variants influencing elevated myeloperoxidase levels increase risk of stroke

AU - Phuah, Chia Ling

AU - Dave, Tushar

AU - Malik, Rainer

AU - Raffeld, Miriam R.

AU - Ayres, Alison M.

AU - Goldstein, Joshua N.

AU - Viswanathan, Anand

AU - Greenberg, Steven M.

AU - Jagiella, Jeremiasz M.

AU - Hansen, Björn M.

AU - Norrving, Bo

AU - Jimenez-Conde, Jordi

AU - Roquer, Jaume

AU - Pichler, Alexander

AU - Enzinger, Christian

AU - Montaner, Joan

AU - Fernandez-Cadenas, Israel

AU - Lindgren, Arne

AU - Slowik, Agnieszka

AU - Schmidt, Reinhold

AU - Biffi, Alessandro

AU - Rost, Natalia

AU - Langefeld, Carl D.

AU - Markus, Hugh S.

AU - Mitchell, Braxton D.

AU - Worrall, Brad B.

AU - Kittner, Steven J.

AU - Woo, Daniel

AU - Dichgans, Martin

AU - Rosand, Jonathan

AU - Anderson, Christopher D.

N1 - Funding Information: Our research was supported in part by the NIH-NINDS through K23NS086873, K23NS064052, R01NS059727 and P50NS061343, R01NS36695, U01NS069763, U01NS069208 and R01NS30678 and the NIH-NIA through R01AG26484. This work was further supported by grants from the German Federal Ministry of Education and Research(e:Med program e:AtheroSysMed), the FP7 European Union (EU) project CVgenes{at}target(261123), the DFG(CRC 1123, B3), the Corona Foundation, the Fondation Leducq (Transatlantic Network of Excellence on the Pathogenesis of Small Vessel Disease of the Brain). This project has received funding from the European Union’s Horizon 2020 research and innovation program under grant agreement No 667375. Part of this project was funded by Generacion project (PI15/01978) Instituto de Salud Carlos III. Lund Stroke Register (LSR) has been supported by the Swedish Heart and Lung Foundation, Skåne University Hospital, Region Skåne, the Freemasons Lodge of Instruction EOS in Lund, King Gustaf V and Queen Victoria’s Foundation, Lund University, and the Swedish Stroke Association, and Spain’s Ministry of Health (Ministerio de Sanidad y Consumo, Instituto de Salud Carlos III FEDER, RD16/0019/0002. INVICTUS-PLUS). Hugh S. Markus is supported by an NIHR Senior Investigator award and his work is supported by the Cambridge University Hospital Comprehensive Biomedical Research Centre. Publisher Copyright: © The Author (2017).

PY - 2017/10/1

Y1 - 2017/10/1

N2 - Primary intracerebral haemorrhage and lacunar ischaemic stroke are acute manifestations of progressive cerebral microvascular disease. Current paradigms suggest atherosclerosis is a chronic, dynamic, inflammatory condition precipitated in response to endothelial injury from various environmental challenges. Myeloperoxidase plays a central role in initiation and progression of vascular inflammation, but prior studies linking myeloperoxidase with stroke risk have been inconclusive. We hypothesized that genetic determinants of myeloperoxidase levels influence the development of vascular instability, leading to increased primary intracerebral haemorrhage and lacunar stroke risk. We used a discovery cohort of 1409 primary intracerebral haemorrhage cases and 1624 controls from three studies, an extension cohort of 12 577 ischaemic stroke cases and 25 643 controls from NINDSSiGN, and a validation cohort of 10 307 ischaemic stroke cases and 29 326 controls from METASTROKE Consortium with genome-wide genotyping to test this hypothesis. A genetic risk score reflecting elevated myeloperoxidase levels was constructed from 15 common single nucleotide polymorphisms identified from prior genome-wide studies of circulating myeloperoxidase levels (P55 - 10 6). This genetic risk score was used as the independent variable in multivariable regression models for association with primary intracerebral haemorrhage and ischaemic stroke subtypes. We used fixed effects meta-analyses to pool estimates across studies. We also used Cox regression models in a prospective cohort of 174 primary intracerebral haemorrhage survivors for association with intracerebral haemorrhage recurrence. We present effects of myeloperoxidase elevating single nucleotide polymorphisms on stroke risk per risk allele, corresponding to a one allele increase in the myeloperoxidase increasing genetic risk score. Genetic determinants of elevated circulating myeloperoxidase levels were associated with both primary intracerebral haemorrhage risk (odds ratio, 1.07, P = 0.04) and recurrent intracerebral haemorrhage risk (hazards ratio, 1.45, P = 0.006). In analysis of ischaemic stroke subtypes, the myeloperoxidase increasing genetic risk score was strongly associated with lacunar subtype only (odds ratio, 1.05, P = 0.0012). These results, demonstrating that common genetic variants that increase myeloperoxidase levels increase risk of primary intracerebral haemorrhage and lacunar stroke, directly implicate the myeloperoxidase pathway in the pathogenesis of cerebral small vessel disease. Because genetic variants are not influenced by environmental exposures, these results provide new support for a causal rather than bystander role for myeloperoxidase in the progression of cerebrovascular disease. Furthermore, these results support a rationale for chronic inflammation as a potential modifiable stroke risk mechanism, and suggest that immune-targeted therapies could be useful for treatment and prevention of cerebrovascular disease.

AB - Primary intracerebral haemorrhage and lacunar ischaemic stroke are acute manifestations of progressive cerebral microvascular disease. Current paradigms suggest atherosclerosis is a chronic, dynamic, inflammatory condition precipitated in response to endothelial injury from various environmental challenges. Myeloperoxidase plays a central role in initiation and progression of vascular inflammation, but prior studies linking myeloperoxidase with stroke risk have been inconclusive. We hypothesized that genetic determinants of myeloperoxidase levels influence the development of vascular instability, leading to increased primary intracerebral haemorrhage and lacunar stroke risk. We used a discovery cohort of 1409 primary intracerebral haemorrhage cases and 1624 controls from three studies, an extension cohort of 12 577 ischaemic stroke cases and 25 643 controls from NINDSSiGN, and a validation cohort of 10 307 ischaemic stroke cases and 29 326 controls from METASTROKE Consortium with genome-wide genotyping to test this hypothesis. A genetic risk score reflecting elevated myeloperoxidase levels was constructed from 15 common single nucleotide polymorphisms identified from prior genome-wide studies of circulating myeloperoxidase levels (P55 - 10 6). This genetic risk score was used as the independent variable in multivariable regression models for association with primary intracerebral haemorrhage and ischaemic stroke subtypes. We used fixed effects meta-analyses to pool estimates across studies. We also used Cox regression models in a prospective cohort of 174 primary intracerebral haemorrhage survivors for association with intracerebral haemorrhage recurrence. We present effects of myeloperoxidase elevating single nucleotide polymorphisms on stroke risk per risk allele, corresponding to a one allele increase in the myeloperoxidase increasing genetic risk score. Genetic determinants of elevated circulating myeloperoxidase levels were associated with both primary intracerebral haemorrhage risk (odds ratio, 1.07, P = 0.04) and recurrent intracerebral haemorrhage risk (hazards ratio, 1.45, P = 0.006). In analysis of ischaemic stroke subtypes, the myeloperoxidase increasing genetic risk score was strongly associated with lacunar subtype only (odds ratio, 1.05, P = 0.0012). These results, demonstrating that common genetic variants that increase myeloperoxidase levels increase risk of primary intracerebral haemorrhage and lacunar stroke, directly implicate the myeloperoxidase pathway in the pathogenesis of cerebral small vessel disease. Because genetic variants are not influenced by environmental exposures, these results provide new support for a causal rather than bystander role for myeloperoxidase in the progression of cerebrovascular disease. Furthermore, these results support a rationale for chronic inflammation as a potential modifiable stroke risk mechanism, and suggest that immune-targeted therapies could be useful for treatment and prevention of cerebrovascular disease.

KW - genetics

KW - inflammation

KW - intracerebral haemorrhage

KW - myeloperoxidase

KW - stroke

UR - http://www.scopus.com/inward/record.url?scp=85030710874&partnerID=8YFLogxK

U2 - 10.1093/brain/awx220

DO - 10.1093/brain/awx220

M3 - Article

C2 - 28969386

AN - SCOPUS:85030710874

SN - 0006-8950

VL - 140

SP - 2663

EP - 2672

JO - Brain

JF - Brain

IS - 10

ER -

Genetic variants influencing elevated myeloperoxidase levels increase risk of stroke

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