Xanthine oxidase inhibition and white matter hyperintensity progression following ischaemic stroke and transient ischaemic attack (XILO-FIST): a multicentre, double-blinded, randomised, placebo-controlled trialResearch in context

Jesse Dawson; Michele Robertson; David Alexander Dickie; Phillip Bath; Kirsten Forbes; Terence Quinn; Niall M. Broomfield; Krishna Dani; Alex Doney; Graeme Houston; Kennedy R. Lees; Keith W. Muir; Allan Struthers; Matthew Walters; Mark Barber; Ajay Bhalla; Alan Cameron; Alexander Dyker; Paul Guyler; Ahamad Hassan; Mark T. Kearney; Breffni Keegan; Sekaran Lakshmanan; Mary Joan Macleod; Marc Randall; Louise Shaw; Ganesh Subramanian; David Werring; Alex McConnachie

EClinicalMedicine (Mar 2023)

Xanthine oxidase inhibition and white matter hyperintensity progression following ischaemic stroke and transient ischaemic attack (XILO-FIST): a multicentre, double-blinded, randomised, placebo-controlled trialResearch in context

Jesse Dawson,
Michele Robertson,
David Alexander Dickie,
Phillip Bath,
Kirsten Forbes,
Terence Quinn,
Niall M. Broomfield,
Krishna Dani,
Alex Doney,
Graeme Houston,
Kennedy R. Lees,
Keith W. Muir,
Allan Struthers,
Matthew Walters,
Mark Barber,
Ajay Bhalla,
Alan Cameron,
Alexander Dyker,
Paul Guyler,
Ahamad Hassan,
Mark T. Kearney,
Breffni Keegan,
Sekaran Lakshmanan,
Mary Joan Macleod,
Marc Randall,
Louise Shaw,
Ganesh Subramanian,
David Werring,
Alex McConnachie

Affiliations

Jesse Dawson: School of Cardiovascular and Metabolic Health, College of Medical, Veterinary & Life Sciences, University of Glasgow, Queen Elizabeth University Hospital, Glasgow, G51 4TF, UK; Corresponding author.
Michele Robertson: Robertson Centre for Biostatistics, School of Health and Wellbeing, College of Medical, Veterinary & Life Sciences, University of Glasgow, Glasgow, G12 8QQ, UK
David Alexander Dickie: School of Cardiovascular and Metabolic Health, College of Medical, Veterinary & Life Sciences, University of Glasgow, Queen Elizabeth University Hospital, Glasgow, G51 4TF, UK; DD Analytics Cubed Ltd, 73 Union Street, Greenock, Scotland, PA16 8BG, UK
Phillip Bath: Stroke Trials Unit, Mental Health & Clinical Neuroscience, University of Nottingham, Nottingham, NG7 2UH, UK
Kirsten Forbes: Department of Neuroradiology, Institute of Neurological Sciences, Queen Elizabeth University Hospital, 1345 Govan Road, Glasgow, G51 4TF, UK
Terence Quinn: School of Cardiovascular and Metabolic Health, College of Medical, Veterinary & Life Sciences, University of Glasgow, Glasgow Royal Infirmary, Glasgow, UK
Niall M. Broomfield: Department of Clinical Psychology and Psychological Therapies, Norwich Medical School, University of East Anglia, NR4 7TJ, UK
Krishna Dani: Department of Neurology, Institute of Neurological Sciences Glasgow, Queen Elizabeth University Hospital, 1345 Govan Road, Glasgow, G51 4TF, UK
Alex Doney: Medicine Monitoring Unit (MEMO), School of Medicine, University of Dundee. Ninewells Hospital, Dundee, DD1 9SY, UK
Graeme Houston: Division of Imaging and Science Technology, School of Medicine, Ninewells Hospital, Dundee, DD1 9SY, UK
Kennedy R. Lees: School of Medicine, College of Medical, Veterinary & Life Sciences, University of Glasgow, Glasgow, G12 8QQ, UK
Keith W. Muir: School of Psychology and Neuroscience, College of Medical, Veterinary & Life Sciences, University of Glasgow, Queen Elizabeth University Hospital, Glasgow, G51 4TF, UK
Allan Struthers: Division of Molecular and Clinical Medicine, University of Dundee, UK
Matthew Walters: School of Medicine, College of Medical, Veterinary & Life Sciences, University of Glasgow, Glasgow, G12 8QQ, UK
Mark Barber: University Department of Stroke Care, University Hospital Monklands, Airdrie, ML6 OJS, UK
Ajay Bhalla: Department of Stroke, Ageing and Health, Guy's and St Thomas NHS Foundation Trust, St Thomas' Hospital, Lambeth Palace Rd, London, SE1 7EH, UK
Alan Cameron: School of Cardiovascular and Metabolic Health, College of Medical, Veterinary & Life Sciences, University of Glasgow, Queen Elizabeth University Hospital, Glasgow, G51 4TF, UK
Alexander Dyker: Wolfson Unit of Clinical Pharmacology, Royal Victoria Infirmary, Newcastle Upon Tyne, UK
Paul Guyler: Department of Stroke Medicine, Mid and South Essex University Hospitals Group, Southend University Hospital, Prittlewell Chase, Westcliff-on-Sea, Essex, SS0 0RY, UK
Ahamad Hassan: Department of Neurology, Leeds General Infirmary, Leeds, UK
Mark T. Kearney: Leeds Institute of Cardiovascular and Metabolic Medicine, The University of Leeds, Leeds, UK
Breffni Keegan: Department of Medicine, South West Acute Hospital, Enniskillen, BT74 6DN, UK
Sekaran Lakshmanan: Department of Stroke Medicine The Luton and Dunstable University Hospital, Bedfordshire, NHSFT, Lewsey Road, Luton, LU4 0DZ, UK
Mary Joan Macleod: Institute of Medical Sciences, University of Aberdeen, Aberdeen, UK
Marc Randall: Department of Neurology, Leeds Teaching Hospitals NHS Trust, Leeds, UK
Louise Shaw: Department of Stroke Medicine, Royal United Hospital, Combe Park, Bath, BA1 3NG, UK
Ganesh Subramanian: Department of Stroke Medicine, Nottingham University Hospitals, Nottingham, NG5 1PB, UK
David Werring: Stroke Research Centre, UCL Queen Square Institute of Neurology, London, UK; Comprehensive Stroke Service, National Hospital for Neurology and Neurosurgery, Queen Square, University College Hospitals NHS Foundation Trust, London, UK
Alex McConnachie: Robertson Centre for Biostatistics, School of Health and Wellbeing, College of Medical, Veterinary & Life Sciences, University of Glasgow, Glasgow, G12 8QQ, UK

Journal volume & issue: Vol. 57
p. 101863

Abstract

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Summary: Background: People who experience an ischaemic stroke are at risk of recurrent vascular events, progression of cerebrovascular disease, and cognitive decline. We assessed whether allopurinol, a xanthine oxidase inhibitor, reduced white matter hyperintensity (WMH) progression and blood pressure (BP) following ischaemic stroke or transient ischaemic attack (TIA). Methods: In this multicentre, prospective, randomised, double-blinded, placebo-controlled trial conducted in 22 stroke units in the United Kingdom, we randomly assigned participants within 30-days of ischaemic stroke or TIA to receive oral allopurinol 300 mg twice daily or placebo for 104 weeks. All participants had brain MRI performed at baseline and week 104 and ambulatory blood pressure monitoring at baseline, week 4 and week 104. The primary outcome was the WMH Rotterdam Progression Score (RPS) at week 104. Analyses were by intention to treat. Participants who received at least one dose of allopurinol or placebo were included in the safety analysis. This trial is registered with ClinicalTrials.gov, NCT02122718. Findings: Between 25th May 2015 and the 29th November 2018, 464 participants were enrolled (232 per group). A total of 372 (189 with placebo and 183 with allopurinol) attended for week 104 MRI and were included in analysis of the primary outcome. The RPS at week 104 was 1.3 (SD 1.8) with allopurinol and 1.5 (SD 1.9) with placebo (between group difference −0.17, 95% CI −0.52 to 0.17, p = 0.33). Serious adverse events were reported in 73 (32%) participants with allopurinol and in 64 (28%) with placebo. There was one potentially treatment related death in the allopurinol group. Interpretation: Allopurinol use did not reduce WMH progression in people with recent ischaemic stroke or TIA and is unlikely to reduce the risk of stroke in unselected people. Funding: The British Heart Foundation and the UK Stroke Association.

Published in EClinicalMedicine

ISSN: 2589-5370 (Online)
Publisher: Elsevier
Country of publisher: United Kingdom
LCC subjects: Medicine: Medicine (General)
Website: https://www.thelancet.com/journals/eclinm/home

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