Clincosm LogoSign in Get a demo

XILO-FIST, the Effect of Allopurinol on the Brain Heart and Blood Pressure After Stroke

Sponsor
NHS Greater Glasgow and Clyde (Other)
Overall Status
Completed
CT.gov ID
NCT02122718
Collaborator
University of Glasgow (Other)
464
Enrollment
21
Locations
2
Arms
81.1
Duration (Months)
22.1
Patients Per Site
0.3
Patients Per Site Per Month

Study Details

Study Description

Brief Summary

Recurrent stroke and cognitive decline are common after ischaemic stroke. Allopurinol, a drug usually used to treat gout, has been shown to reduce heart ischaemia, heart size, and arterial stiffness and to relax brain blood vessels and may reduce the blood pressure. All of these properties may be associated with a lower risk of second stroke and cognitive decline. We now aim to explore whether allopurinol will reduce further damage to the brain (called white matter hyper-intensities) after stroke and also whether it reduces heart size and blood pressure after stroke.

We will conduct a multi-centre randomised, double-blind placebo controlled study to investigate whether two years allopurinol 300 mg twice per day (BD) improves these 3 outcomes, which are inextricably linked to risk of recurrence and cognitive decline after ischaemic stroke.

Condition or Disease Intervention/Treatment Phase
Phase 4

Detailed Description

New strategies are needed to improve long-term outcomes after ischaemic stroke or transient ischaemic attack (TIA). Approximately 13% of participants suffered recurrent stroke in recent secondary preventative trials , 40% of patients with TIA experience recurrent cardiovascular (CV) events during long-term follow up and there is an additional substantial burden from incident post-stroke dementia (~ 10% after first stroke and higher still after recurrent events) , cognitive decline (over 30%) and decline in physical function. Improving these outcomes is a recognised priority area for stroke research (as identified by stroke survivors through the recent James Lind Alliance priority setting workshops ).

Such adverse outcomes are particularly common in those with brain white matter hyper-intensities (WMH) on brain magnetic resonance imaging (MRI) . WMH are seen in as many as 90% of patients with ischaemic stroke , , are at least moderately severe in 50%6 and such 'severe' WMH are associated with substantially higher stroke recurrence rates (43% in one study)6, death and increased cognitive and physical decline. The burden of WMH increases during longitudinal follow up and this is associated with increased incident stroke, dementia and cognitive decline5. In the longitudinal population based Rotterdam scan study, 39% of elderly participants had WMH progression (over a mean period of 3.4 years) , as did 50% in the recent PROFeSS MRI sub-study (over 2 years)7 and 74% (over 3 years) in the Leukoariosis and Disability study (LADIS) .Similarly, silent brain infarction (SBI) is also associated with recurrent stroke and 14% developed incident infarcts on brain MRI in the Rotterdam scan study9. Thus, treatments that reduce WMH progression and incident silent brain infarction could have potentially profound effects on a variety of outcomes after stroke including cognition, functional outcome and recurrent stroke.

The pathological basis for WMH development and progression is poorly understood. Post mortem studies show presence of varied pathologies including demyelination, infarction, arteriosclerosis and breakdown of the blood-brain barrier. Key risk factors for development and progression of WMH are age, arterial hypertension and previous stroke9 and associations with other cardiovascular risk factors and left ventricular hypertrophy (LVH) have been demonstrated . Blood pressure (BP) lowering reduces WMH progression, as demonstrated by the PROGRESS MRI sub-study . In the PROFeSS MRI sub-study WMH progression was unaffected by the angiotensin receptor blocker telmisartan7 but unlike PROGRESS, there was no significant difference in BP between groups. In addition, WMH are less clearly related to hypertension in older patients with established cardiovascular disease meaning that novel strategies which reduce WMH progression and SBI would be particularly promising in this group.

The association between WMH and LVH is of particular interest; it appears independent of arterial BP , and may be mediated by aortic stiffness . There are additional potential mechanisms for this association (e.g., LVH is the strongest predictor of left atrial appendage thrombi, stronger than any left atrial parameter) . Regression of LVH is associated with reduced risk of stroke. In a recent meta-analysis of 14 studies in 12,809 patients, LVH regression was independently associated with a 25% reduction in future strokes, whereas the composite endpoint of CV events/mortality was only 15% lower . Similar findings were seen in the LIFE echo sub-study which utilised measures of left ventricular mass (LVM) . LVH regression is thus a promising therapeutic target in devising new ways to prevent strokes, especially if the same treatment were found to reduce WMH.

Study Design

Study Type:
Interventional
Actual Enrollment :
464 participants
Allocation:
Randomized
Intervention Model:
Parallel Assignment
Masking:
Quadruple (Participant, Care Provider, Investigator, Outcomes Assessor)
Primary Purpose:
Treatment
Official Title:
Xanthine Oxidase Inhibition for Improvement of Long-term Outcomes Following Ischaemic Stroke and Transient Ischaemic Attack
Study Start Date :
May 1, 2014
Actual Primary Completion Date :
Feb 1, 2021
Actual Study Completion Date :
Feb 1, 2021

Arms and Interventions

Arm Intervention/Treatment
Experimental: Allopurinol

Drug: Allopurinol
Placebo Comparator: Placebo

Drug: Placebo

Outcome Measures

Primary Outcome Measures

  1. White matter hyper-intensities (WMH) progression rate over 2 years, defined using the Rotterdam Progression Score [2 years]

Secondary Outcome Measures

  1. change in mean day-time systolic BP at 1 month [1 month]

  2. change in mean day-time diastolic BP at 1 month [1 month]

  3. Schmidt's Progression Score [2 years]

  4. Fazekas score [2 years]

  5. Scheltens scale score [2 years]

  6. New brain infarction on MRI [2 years]

  7. Rotterdam Progression Score with those who die / become too frail to undergo MRI being assigned the highest score [2 years]

  8. Montreal Cognitive Assessment (MoCA) score [2 years]

  9. Incident dementia [2 years]

  10. change in mean day-time systolic BP at 2 years [2 years]

  11. change in mean day-time diastolic BP at 2 years [2 years]

  12. blood pressure variability [2 years]

  13. Quality of life (EQ-5D, Stroke Specific Quality of Life Scale (SS-QOL)) [2 years]

  14. Recurrent stroke [2 years]

  15. Recurrent myocardial infarction (MI), stroke or cardiac death [2 years]

  16. Mortality [2 years]

  17. Incident atrial fibrillation [2 years]

  18. Clinic blood pressure [2 years]

Other Outcome Measures

  1. Cardiac sub-study: Change in measured Left ventricular mass (LVM) at 2 years [2 years]

  2. Cardiac sub-study: change in ejection fraction [2 years]

  3. Cardiac Sub-study: change in end diastolic volume [2 years]

  4. Cardiac sub-study: change in end systolic volume [2 years]

  5. Cardiac Sub-study: change in stroke volume [2 years]

  6. Cardiac sub-study: change in left atrial diameter [2 years]

Eligibility Criteria

Criteria

Ages Eligible for Study:
50 Years and Older
Sexes Eligible for Study:
All
Accepts Healthy Volunteers:
No
Inclusion Criteria:

  • Ischaemic Stroke/ Ischaemic lesion on brain imaging in relevant anatomical territory in patients with transient ischaemic attack.

  • Age greater than 50 years. -- Consent within one month of stroke.

Exclusion Criteria:

  • Modified Rankin scale score of 5 (at end of the possible enrolment window of one month after stroke).

  • Diagnosis of dementia (defined as a documented diagnosis or a screening Informant Questionnaire for Cognitive Decline in the Elderly (IQCODE) score of 3.6 or more).

  • Cognitive impairment deemed sufficient to compromise capacity to consent or to comply with the protocol (in the opinion of the local investigator).

  • Dependent on daily help from others for basic or instrumental activities of daily living prior to stroke (defined as assistance needed with toileting, walking or dressing).

  • Significant co-morbidity or frailty likely to cause death within 24 months or likely to make adherence to study protocol difficult for participant (in the opinion of the local investigator).

  • Contra-indication to or indication for administration of allopurinol (as detailed in Summary of Product Characteristics on the XILO-FIST web portal and in trial master file).

  • Concurrent azathioprine, 6-mercaptopurine therapy, other cytotoxic therapies, cyclosporin, theophylline and didanosine.

  • Significant hepatic impairment (defined as serum bilirubin, Aspartate Aminotransferase (AST) or Alanine transaminase (ALT) greater than three times upper limit of normal (ULN)).

  • Estimated Glomerular Filtration Rate < 30 mls/min

  • Contraindication to MRI scanning.

  • Women who are pregnant or breastfeeding.

  • Women of childbearing potential who are unable or unwilling to use contraception.

  • Prisoners.

  • Active participation in another Clinical Trial of Investigational Medicinal Product (CTIMP) or device trial or participation within the past month.

Contacts and Locations

Locations

Site City State Country Postal Code
1 Altnagelvin Campus Londonderry County Derry United Kingdom BT47 6SB
2 Broomfield Hospital Chelmsford Essex United Kingdom CM1 7ET
3 Southend University Hospital Westcliff-on-Sea Essex United Kingdom SS0 0RY
4 Darent Valley Hospital Dartford Kent United Kingdom DA2 8DA
5 The Royal London Hospital Whitechapel London United Kingdom E1 1BB
6 Northumbria NHS Trust Ashington Northumberland United Kingdom NE63 9JJ
7 Royal United Hospital Bath Somerset United Kingdom BA1 3NG
8 Royal Stoke University Hosptial Stoke-on-Trent Staffordshire United Kingdom ST4 6QG
9 NHS Grampian Aberdeen United Kingdom AB25 2ZD
10 NHS Lanarkshire Airdrie United Kingdom ML6 0JS
11 NHS Tayside Dundee United Kingdom DD1 9SY
12 South West Acute Hospital Enniskillen United Kingdom BT74 6DN
13 NHS Greater Glagsow and Clyde Glasgow United Kingdom G11 6NT
14 Leeds Teaching Hospitals NHS Trust Leeds United Kingdom LS1 3EX
15 Barnet Hospital London United Kingdom EN5 3DJ
16 Guys and St Thomas NHS Foundation Trust London United Kingdom SE1 7EH
17 UCL Stroke Research Centre London United Kingdom WC1B 5EH
18 Luton and Dunstable University Hosptial Luton United Kingdom LU4 0DZ
19 Newcastle UPon Tyne Hospitals NHS Trust Newcastle United Kingdom NE2 4AB
20 Nottingham University Nottingham United Kingdom NG5 1PB
21 City Hospital Sunderland NHS Foundation Trust Sunderland United Kingdom SR4 7TP

Sponsors and Collaborators

  • NHS Greater Glasgow and Clyde
  • University of Glasgow

Investigators

  • Principal Investigator: Jesse Dawson, University of Glasgow

Study Documents (Full-Text)

None provided.

More Information

Publications

None provided.
Responsible Party:
NHS Greater Glasgow and Clyde
ClinicalTrials.gov Identifier:
NCT02122718
Other Study ID Numbers:
  • GN12MT494
  • TSA BHF 2013/01
First Posted:
Apr 24, 2014
Last Update Posted:
Nov 12, 2021
Last Verified:
Nov 1, 2021
Additional relevant MeSH terms:
Stroke
Ischemic Stroke
Ischemia
Allopurinol

Study Results

No Results Posted as of Nov 12, 2021