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Oxidative phosphorylation and lacunar stroke: genome-wide enrichment analysis of common variants

Version 4 2024-03-12, 14:32
Version 3 2023-10-29, 11:01
journal contribution
posted on 2024-03-12, 14:32 authored by Matthew Traylor, Christopher D. Anderson, Robert Hurford, Stephen BevanStephen Bevan, Hugh S. Markus

OBJECTIVEWe investigated whether oxidative phosphorylation (OXPHOS) abnormalities were associated with lacunar stroke, hypothesizing that these would be more strongly associated in patients with multiple lacunar infarcts and leukoaraiosis (LA).METHODSIn 1,012 MRI-confirmed lacunar stroke cases and 964 age-matched controls recruited from general practice surgeries, we investigated associations between common genetic variants within the OXPHOS pathway and lacunar stroke using a permutation-based enrichment approach. Cases were phenotyped using MRI into those with multiple infarcts or LA (MLI/LA) and those with isolated lacunar infarcts (ILI) based on the number of subcortical infarcts and degree of LA, using the Fazekas grading. Using gene-level association statistics, we tested for enrichment of genes in the OXPHOS pathway with all lacunar stroke and the 2 subtypes.RESULTSThere was a specific association with strong evidence of enrichment in the top 1% of genes in the MLI/LA (subtype p = 0.0017) but not in the ILI subtype (p = 1). Genes in the top percentile for the all lacunar stroke analysis were not significantly enriched (p = 0.07).CONCLUSIONSOur results implicate the OXPHOS pathway in the pathogenesis of lacunar stroke, and show the association is specific to patients with the MLI/LA subtype. They show that MRI-based subtyping of lacunar stroke can provide insights into disease pathophysiology, and imply that different radiologic subtypes of lacunar stroke subtypes have distinct underlying pathophysiologic processes.

History

School affiliated with

  • Department of Life Sciences (Research Outputs)

Publication Title

Neurology

Volume

86

Issue

2

Pages/Article Number

141-145

Publisher

merican Academy of Neurology (AAN) / Lippincott, Williams & Wilkins

ISSN

0028-3878

eISSN

1526-632X

Date Submitted

2016-07-28

Date Accepted

2016-09-08

Date of First Publication

2015-12-16

Date of Final Publication

2016-01-12

Date Document First Uploaded

2016-07-28

ePrints ID

23608

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