Peripheral Vascular Diseases Clinical Trial
Official title:
Effects of Remote Ischemic Preconditioning on Restenosis Post Lower Limb Revascularization Angioplasty: A Pilot Randomized Control Trial
The investigators will established relation between restenosis and inflammatory response to shearing stress caused by angioplasty suggest that any mechanism that affect inflammatory response can consequently affect the restenosis rate. There is accumulated evidence that remote ischemic precondition has modifying suppressive effect on inflammatory response and the investigators hypothesized that RIPC may lead to reduction in post angioplasty restenosis rate.
Rationale:
The father of interventional radiology Charles Dotter (1920-1985) performed the first
percutaneous transluminal angioplasty in university of Oregon hospital on Laura Shaw in 16th
of January 1964. She presented with typical rest pain and foot gangrene on left leg and her
angiogram show distal superficial femoral artery focal stenosis. He saved her leg and she was
walking for the next 3 years of her life using his experimental dilating catheter Later in
1977 Zurich witnessed the first coronary angioplasty by German cardiologist Andreas Gruentzig
(1939-1985) using same technique .
The angioplasty utilized gradually in the next years after Dotter to provide less invasive
option for the growing number of peripheral vascular disease patients estimated to be in the
range of 3% to 10%, increasing to 15% to 20% in persons over 70 years. Early diagnosis
remains difficult because patients tends to be asymptomatic up to 50% or more of vessel
narrowing. the strong association between prevalence of peripheral vascular disease and age
increase the demand with world population ageing specially in western Europe and USA. The
lower extremity revascularization USA statistics in year 2000 was 40/100,000 and increasing.
Restenosis or the gradual narrowing of the re vascularized vessel remains one of the main
problems usually it occurs within 6 months of angioplasty . Restenosis percentages varies
between 12% up to 63 % in different studies largely depends on the lesion type and site with
below knee interventions being more liable for restenosis.
The restenosis phenomena can be explained by the physiological response to the trauma caused
by the balloon when inflated to compress the atheroma. Many factors can influence the process
e.g. patient , procedure and vessel condition before intervention.it can be considered as
hypertrophic wound healing from the interaction between monocyte-derived macrophages , T
cells and arterial wall .the inflammatory response lead to Neointimal Hyperplasia the
terminology uses to describe the proliferation and migration of vascular smooth muscle cells
. Elevated inflammatory and coagulation factors markers levels after angioplasty has been
suggested as predictors for the possibility of restenosis . The inflammatory theory was more
supported when using immunosuppressive drugs like Sirolimus shows positive effects on
reducing restenosis rate.
Ischemic precondition introduced first as mechanism to reduced subsequent myocardium injury
after applying intermittent periods of sub-lethal ischemia . Subsequently the concept
examined on other body organs . The mechanisms through which remote ischemic preconditioning
(RIPC) work was the subject for many studies suggesting neural, humoral and anti-Inflammatory
pathways . Animal studies suggest powerful anti-inflammatory effect for RIPC . other studies
shows endothelial protections by decrease formation of reactive oxygen species (ROS) and
upregulates endothelial nitric oxide (eNOS) synthase which responsible for most of
vasculature Nitric Oxide a very important protective molecule in reperfusion and shearing
stress injuries . In human studies Ischaemic, preconditioning show endothelial protective
effect and altered Neutrophils function including reduced adhesion, exocytosis, phagocytosis,
and modified cytokine secretion. . In one study, RIPC stimulates modified leukocyte
inflammatory gene expression in correlations with the first and second windows of the RIPC,
which is 1-2 hours and 12-24 respectively.
Sampling Frame the peripheral vascular disease patients with medical profiles, which match
trial criteria who are waiting for or admitted from emergency department for lower limb
revascularization angioplasty in Galway university hospital, will be identified. Recruitment
will be stopped at 10 months of 16 months of the trial period.
Trial Design Patients who need revascularization angioplasty classically had history of
symptomatic peripheral vascular disease usually assessed in OPD using ABI and send for duplex
ultrasound scan after which some get CT angiogram or Magnetic Resonance Angiography (MRA).
Furthermore, intra operative images are the common practice. the investigators will be
recruiting from this group in accordance with trial protocol.
The target number will be 40 patients divided into 2 groups. All groups candidates will
undergo base line assessment which include history, examination, duplex, ABI and blood sample
for inflammatory and coagulation markers.
The candidates will randomly allocated to:
Randomisation Age and DM are associated with many comorbidities. Randomization will be
stratified for these two confounders using Minimpy computer software.
All trial candidates will have unique numbers to identify them and conceal their identity.
Patients files will be locked in trial office with one-person access and each candidate will
get their numbers in sequential way according to their allocation.
Projected recruitment. Galway University hospital provides vascular services for a population
of approximately 750000 served by the West-North West Hospitals Group. The patients for the
trial will be actively recruited from out patient's clinics, in patients and theatre booking
database. Information about the trial will be given to all vascular team including criteria
for selection and exclusion. Those who qualified will be counselled by the trial team and
consented if the agree to join. The target of 40 patients should be achievable within the
recruitment window.
Patient recruitment & consent Eligible candidates will get all the information about the
trial in written and verbal explanation for all the steps. Patients who are willing to take
part will asked to provide written informed consent. Three copies of the consent form will be
signed: one for the patient, one for the patient's clinical notes file and a one copy for the
patient's trial folder.
Data collection Demographic and clinical data of eligible candidates who agree to participate
will be collected. The candidates will be assign a trial number identifier after informed
consent is signed and no personal information will be available on the data entry sheets. The
original data-entry preform will be retained together with a copy of the consent form in the
trial office with other trial documents in the trial office in CSI building. The code key for
the trial numbers will be limited to the Chief Investigator. Encrypted back up copy will be
prepared at the end of each data entry and will be kept looked separately. All data will be
retained in the care of the principal investigator for a period of five years from the
closure of the trial.
Statistical analysis A trial team member blinded to trial allocation will perform the
statistical analysis with respect to the primary and secondary outcomes. This is a pilot
study the results will be used to identify if there is a need for larger trial.
Trial monitoring Day-to-day management of the trial will be the responsibility of the trial
manager, supervised by the principal investigator. A meeting will be held every two weeks
between the trial manager and the principal investigator to monitor recruitment, data
collection etc.
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