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Oxidative phosphorylation and lacunar stroke

Version 4 2024-03-12, 15:32
Version 3 2023-10-29, 11:55
journal contribution
posted on 2024-03-12, 15:32 authored by Matthew Traylor, Christopher D. Anderson, Robert Hurford, Stephen BevanStephen Bevan, Hugh S. Markus

OBJECTIVE:We 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).METHODS:In 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.RESULTS:There 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).CONCLUSIONS:Our 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

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

ISSN

0028-3878

eISSN

1526-632X

Date Submitted

2017-07-13

Date Accepted

2015-09-08

Date of First Publication

2015-12-16

Date of Final Publication

2016-01-12

Date Document First Uploaded

2017-07-13

ePrints ID

27839

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