Clinical Trial Details
— Status: Completed
Administrative data
| NCT number |
NCT00789542 |
| Other study ID # |
2008/W/NEU/12 |
| Secondary ID |
ISRCTN93529999 |
| Status |
Completed |
| Phase |
Phase 3
|
| First received |
|
| Last updated |
|
| Start date |
December 2008 |
| Est. completion date |
March 2013 |
Study information
| Verified date |
December 2014 |
| Source |
University of Edinburgh |
| Contact |
n/a |
| Is FDA regulated |
No |
| Health authority |
|
| Study type |
Interventional
|
Clinical Trial Summary
Strokes occur when blood flow to part of the brain is interrupted. Patients are often
bedbound for several days or weeks although if they survive, most will make some recovery.
The lack of mobility encourages blood clots to form in the legs - so called deep venous
thrombosis or DVT. About 10% of patients will develop these. Pieces of this clot may break
off and can be carried by the bloodstream to the lungs. These clots, called pulmonary emboli,
can stop the heart and can cause patients with stroke to die suddenly. A treatment which
reduces the risk of DVT after surgery is intermittent pneumatic compression (IPC). Inflatable
sleeves wrapped around the legs inflate at intervals squeezing blood up the legs, increasing
the blood flow, and decreasing the likelihood of clots forming - at least that is the
theory!. Although this sounds uncomfortable, most people actually quite like the sensation!
There have been some small randomised trials of IPC in stroke patients, particularly those
with intracerebral bleeding. However, these studies although encouraging have not provided
enough information to persuade clinicians to use this treatment routinely in stroke units.
The proposed study will include 2000 patients who have had a stroke and who have been
admitted to a stroke unit.
Patients who cannot walk independently, and who are at greatest risk of DVT will be invited
to join the study. If they agree they will be randomly allocated to having routine care plus
IPC or just routine care. Patient in both groups will have routine ultrasound scans on their
legs to detect DVTs. The study will establish whether IPC reduces the risk of DVT. This
result could improve the outcome of many thousands of patients each year.
Description:
Design: Multicentre randomised controlled trial with observer blinded assessment of the
primary outcome.
Setting: Stroke units in the UK. Identification of eligible patients, consent, recruitment,
delivery and monitoring of allocated treatment will occur within the unit. Screening
compression doppler ultrasounds will occur in the radiology department or vascular laboratory
mainly during hospital admission although in the minority of patients who are discharged from
hospital they may have these tests as an outpatient. Six month follow up will occur in their
place of residence via a postal or telephone questionnaire.
Target population: Patients (16 years or over) admitted to hospital with an acute stroke who
are immobile and therefore at significant risk of developing a deep venous thrombosis.
Health technologies being assessed: The trial will compare the outcomes of patients receiving
Routine care plus Intermittent Pneumatic Compression (IPC) vs. Routine care and avoiding IPC.
Patients allocated to IPC will be fitted with thigh length IPC sleeves although if these are
not well tolerated, for instance because of heavy soiling due to faecal incontinence, below
knee sleeves can be substituted. Ideally IPC will be worn both day and night for 30 days from
randomisation OR until a second screening doppler ultrasound (if after 30 days). Routine care
is likely to include general measures to reduce risk of DVT including, adequate hydration,
routine use of aspirin in patients with ischaemic stroke and early mobilisation. It may also
include routine use of graduated compression stockings (GCS) if these are shown to be
effective in the ongoing CLOTS Trials 1 & 2. Participating centres will be asked to ensure
that the standard care specific to their institution is applied equally rigorously to
patients in the trial irrespective of their treatment allocation. Collaborators will be
permitted to use these interventions where they feel this is clinically justified - we will
monitor use of antithrombotics and GCS to ensure it is balanced in the two treatment arms.
Measurement of costs and outcomes: The primary outcome will be the "presence of definite or
probable symptomatic or asymptomatic DVT in the veins behind the knee or in the thigh
detected on either of two screening compression Doppler ultrasound scans (performed at about
7-10 days and 25 - 30 days as part of the research) or contrast venography or MRI(only if
clinically indicated) within 30 days of randomisation". This is regarded as a clinically
important outcome, acceptable to patients and staff and has been shown to be practical to
collect in the vast majority of patients in the ongoing CLOTS Trials 1 & 2. Secondary
outcomes measured in hospital and collected at hospital discharge by reviewing the casenotes
will include: death within 30 days; Presence of definite or probable DVT in the popliteal or
femoral veins detected on a screening Compression Doppler ultrasound scan which had not been
suspected clinically before the scan,Definite (i.e. excluding probable DVTs) symptomatic or
asymptomatic DVT in the popliteal or femoral veins detected on either a Compression Doppler
ultrasound scan or contrast venography or MRI direct thrombus imaging within 30 days of
randomisation; Any definite or probable symptomatic or asymptomatic DVT (i.e. including DVTs
which only involve the calf veins); Confirmed fatal or non-fatal PE; Adherence to allocated
treatment.
Others secondary outcomes measured by either postal or telephone questionnaire at six months
will include: death from any cause, place of residence, post discharge DVT, PE, post DVT
syndrome, disability, and health related quality of life. These will be supplemented by
follow-up for survival via GPs.
Sample size: We plan to recruit about 2000 patients. The Trial will have > 90% power (alpha
0.05) to identify an absolute reduction of risk of our primary outcome of 4% (10% to 6%). The
frequency of our primary outcome is estimated from the ongoing CLOTS Trials 1 & 2 which use
the same entry criteria and methods of follow up. The estimated effect size (odds reduction =
43%) is based on the treatment effects in the systematic review of previous stroke trials
(odds reduction = 48%) attenuated by the delays in applying the treatment due to trial
recruitment and realistic estimates of adherence to the allocated treatment. If the event
rate in both treatment groups combined is lower than expected the Trial Steering Committee
may decide to increase the recruitment target. We aim to enrol at least 1500 patient on Days
0-2 after stroke onset. This will provide greater than 80% power to detect a reduction in
proximal DVT from 10% to 6% in patients enrolled on Days 0-2. If the proportion enrolled
after Day 2 exceeds 25% of the total then the Trial Steering Committee will consider raising
the overall target beyond 2000 to ensure that at least 1500 are recruited on Days 0-2. This
should help ensure that we do not miss a real treatment effect because of delays in
recruitment. If the trial shows that IPC is effective in reducing the risk of DVT after
stroke it is likely that IPC treatment will be started earlier than in the trial.
Flow from patients perspective
1. Approach by clinical staff who will give verbal and written information about trial
2. Completion of consent form
3. Informed of treatment allocation
4. Start of treatment - application of intermittent pneumatic compression in half of
patients. This involves nursing staff measuring the patients thigh diameter, fitting the
correct size of sleeves and checking the patients legs three times per day to ensure
there are no problems with the skin developing.
5. At 7-10 days after recruitment the patient goes to X Ray department to have a screening
Doppler ultrasound of both legs. The IPC is removed prior to them leaving the ward and
replaced on their return.
6. At 25-30 days after recruitment the patients go to X Ray department to have a second
screening Doppler ultrasound of both legs. If already discharged from hospital this may
involve an outpatient appointment. Patient transport is provided if this is required.
7. At 30 days the IPC (if allocated) is finally removed unless it has been removed earlier
for a specific reason (see protocol)
8. At about 6 months after recruitment the patient will receive a short postal
questionnaire to find out their current functional status, whether they have had any
clots since hospital discharge and what blood thinning medication they might be taking.