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Home NEWS Science News Health

Large-scale genetic study provides new insight into the causes of stroke

Bioengineer by Bioengineer
March 12, 2018
in Health
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Credit: University of Virginia Health System

An international research consortium studying 520,000 individuals from around the world has identified 22 new genetic risk factors for stroke, thus tripling the number of gene regions known to affect stroke risk. The results demonstrate shared genetic influences with multiple related vascular conditions, especially blood pressure, but also coronary artery disease, venous thromboembolism and others. Linking these results with extensive biological databases provides novel clues on stroke mechanisms and illustrates the potential of genetics to identify drug targets for stroke therapy.

The results of the largest genetic study on stroke thus far were published online in the journal Nature Genetics today, 12 March 2018. The study was based on DNA samples of 520,000 European, North- and South American, Asian, African, and Australian participants of whom 67,000 had a stroke. These were derived from 29 large studies. From the millions of genetic variants analyzed, 32 independent genomic regions were shown to be associated with stroke of which two thirds are novel.

The study was conducted by members of MEGASTROKE, a large-scale international collaboration launched by the International Stroke Genetics Consortium, an international multi-disciplinary collaborative of experts in stroke genetics from around the world who have been working together for the past 10 years. MEGASTROKE members include research groups from Germany, France, the UK, Japan, USA, Iceland, Spain, Switzerland, Italy, Belgium, the Netherlands, Denmark, Sweden, Norway, Finland, Estonia, Poland, Singapore, Australia, and Canada.

"Because the extent to which individual variants modify stroke risk is very small, it required a large number of subjects to discover these variants. Our group has leveraged extensive datasets set up by numerous researchers over the past few years," said Martin Dichgans, Professor of Neurology and Director at the Institute for Stroke and Dementia Research (ISD), University Hospital, Ludwig-Maximilians-University (LMU) Munich, and one of the leaders of the current study.

"We can't overstate the importance of international collaboration across different ethnic origins when studying genetics of complex, common diseases like stroke. This large-scale collaboration across continents has been a game changer," says Stephanie Debette, Professor of Epidemiology and Neurologist at University of Bordeaux and Bordeaux University Hospital, leading a research team at INSERM Center U1219, and another leader of the study.

Stroke is the second most common cause of both death and disability-adjusted life-years worldwide, but its molecular mechanisms remain poorly understood, which makes developing new treatments challenging. This study provides extensive novel insight on the biology and pathways leading to stroke.

Stroke can originate from alterations in various parts of the vasculature including large arteries, small arteries, the heart, and the venous system and the researchers found genetic risk factors implicated in each of these mechanisms. They showed that some genetic risk factors contribute to specific mechanisms and others to stroke susceptibility at large. They further found shared genetic influences between stroke caused by vessel occlusion (the most common cause of stroke) and stroke caused by rupture of a blood vessel (the most catastrophic cause of stroke), often thought to have opposite mechanisms.

When the researchers took a closer look on the genomic areas pinpointed in the study, they noticed that several of them overlap with genomic areas known to be implicated in related vascular conditions such as atrial fibrillation, coronary artery disease, venous thrombosis, or vascular risk factors, especially elevated blood pressure, and less so hyperlipidemia.

By adding data on gene expression, protein expression, and other characteristics in multiple cell types and tissues compiled by their co-investigators the researchers obtained first insights into the specific genes, molecular pathways, and cell and tissue types through which the new genetic risk factors cause stroke.

The researchers further found that the genes they identified are enriched in drug targets for antithrombotic therapy, used to re-open occluded blood vessels in patients with acute stroke or to prevent vascular events including stroke. These findings illustrate the potential of genetics for drug discovery says Bradford B. Worrall, MD, a researcher from the University of Virginia School of Medicine and co-author of the study.

The genetic findings represent a first step towards developing personalized, evidence-based treatments for this very complex disease, he said, adding that they provide evidence for several novel biological pathways involved in stroke that may lead to the discovery of novel drug targets.

###

Original publication:

Multi-ancestry genome-wide association study of 520,000 subjects identifies 32 loci associated with stroke and stroke subtypes (2018). Rainer Malik, Ganesh Chauhan, Matthew Traylor, Muralidharan Sargurupremraj et al. Nature Genetics. doi: http://dx.doi.org/10.1038/s41588-018-0058-3.

More information:

Professor Martin Dichgans
Institute for Stroke and Dementia Research
Klinikum der Universität München. Ludwig-Maximilians-University (LMU), Munich, Germany
Feodor-Lynen-Straße 17, D-81377 München
T: 49-0-89-4400 – 46019
E-Mail: [email protected]

Professor Stephanie Debette
INSERM U1219 Bordeaux Population Health Research Center,
University of Bordeaux, Bordeaux, France
Department of Neurology, Institute for Neurodegenerative Disease,
Bordeaux University Hospital, Bordeaux, France.
T: 33-0-5-47-30-42-74
E-mail: [email protected]

Media Contact

Josh Barney
[email protected]
434-906-8864

http://www.healthsystem.virginia.edu/home.html

Original Source

http://newsroom.uvahealth.com/2018/03/12/large-scale-genetic-study-provides-new-insight-causes-stroke/ http://dx.doi.org/10.1038/s41588-018-0058-3

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