Stroke Clinical Trial
Official title:
An Investigator-Sponsored,Double Blind,Placebo-controlled,Randomised,Multi-centre Study to Assess the Effects of Very Early Use of Rosuvastatin in Preventing Recurrence of Ischemic Stroke
It is anticipated that 548 subjects will be recruited from approximately 27 centres in South
Korea.
This is an investigator-sponsored, double-blind, placebo-controlled, randomized,
multi-centre study to assess the effects of rosuvastatin 20 mg compared to placebo in acute
ischemic stroke patients, with the first dose within 18 hours after baseline MRI and
continued treatment for 14 days.
Subjects will be male or female, over 20 years, with diagnosis of acute ischemic stroke with
baseline MRI, and who are either statin-naïve or untreated with statin for the previous 3
months.
The objective would be to compare the recurrence rate of ischemic stroke by comparing the
imaging parameters during 14 days of treatment and clinical improvement as defined by
percent improvement based on NIHSS scores measurements at baseline, 5 days and 14 days of
treatment.
Statins have action mechanisms that may work nicely in preventing recurrence during acute
stage of infarction!
First, statins have antithrombotic effects and lower thrombogenicity. Statins prolong time
to arterial thrombosis in endothelial injury model, inhibit P-selectin expression and
platelet aggregation, reduce platelet PAR-1 thrombin receptor, and reduce tissue factor
levels in plasma, its expression on monocyte surface, and atherosclerotic plaques. Second,
statins enhance thrombolysis. They reduce PAI-1, increase t-PA activity and reduce
fibrinogen level. Combined treatment of statins and t-PA in rats reduces the infarct size
and downregulates expression of tissue factor, ICAM-1, vWF, and MMP-9. In addition, t-PA
induced toxicity is reversed by statins.
Third, statins have anti-inflammatory actions that can stabilize and even regress plaques.
Statins reduce the number of T-lymphocytes within plaques, inhibit migration and activation
of monocyte/macrophage system, and reduce matrix metalloproteinase activity that play a
critical role in plaque rupture. Rosuvastatin 40 mg could regress coronary atheroma burden
at 2 years, and reduce progression of carotid intima-media thickness.
Benefits of statins in stroke patients are partially proven!
First, statins are well known to be effective in primary prevention of stroke. Second,
statins were effective in secondary prevention of stroke. A high dose of statin
(atorvastatin 80 mg) reduced recurrent stroke in patients with recent TIA or ischemic stroke
when it was administrated 1-6 months after stroke onset. However, it is uncertain whether
statins are effective during the first month after stroke. Third, outcomes are better in
patients under statin treatment at the moment of stroke. Patients pretreated with statins
showed better survival, less severe neurologic deficits, and improved outcomes when they
were treated with thrombolysis.
However, it is unknown whether statin treatment in stroke patients is effective when it is
administrated during the acute stage.
Based on strong supportive evidence in human and experimental animals which support
theoretical superiority of rosuvastatin, this study will test a hypothesis that a high dose
of rosuvastatin is effective in preventing recurrence during the first month after onset in
ischemic stroke patients and should be given to all patients from their onset.
;
Allocation: Randomized, Endpoint Classification: Efficacy Study, Intervention Model: Parallel Assignment, Masking: Double Blind (Subject, Caregiver, Investigator, Outcomes Assessor), Primary Purpose: Treatment
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