Dyslipidemia Clinical Trial
Official title:
Comparison of the Effect Noted in The Apo/Apo-1 Ratio Using Rosuvastatin and Atorvastatin in Patients With acUte Coronary Syndrome CENTAURUS Study
This is a 3-month, randomized, parallel-group study with 2 periods, comparing the efficacy and the safety of rosuvastatin 20 mg versus atorvastatin 80 mg in patients with an acute coronary syndrome (ACS).
Patients with ACS (acute coronary syndrome) constitute a high-risk population with unstable
coronary disease (CHD) that differs from stable CHD primarily in short term prognosis
(prediction of outcome). The 1-year rate of death or non-fatal MI (myocardial infarction or
heart attack) was 13% in patients with ACS in a recent controlled study (FRISC II 1999),
compared with less than 2% in patients with stable CHD (SAPAT 1992). Thus, despite
substantial progress in the treatment of ACS with antiplatelet and anti-thrombotic
medications (blood thinners), additional therapies are needed to reduce the additional risk
associated with unstable CHD. Current guidelines (NCEP 2001) recommend that patients
admitted with a major coronary event (MI or ACS) should be considered for treatment with a
statin on discharge from the hospital.
Cited advantages of this approach are patient motivation to start therapy at that time and
prevention of a "treatment gap" due to inconsistent outpatient follow-up. A previously
randomized controlled study of statin therapy in ACS patients (MIRACL study), showed that
aggressive cholesterol lowering with atorvastatin 80 mg between 24 and 96 hours after
hospital admission in patients with ACS resulted in reduced incidence of recurrent CHD
events at 16 weeks. However, the study excluded patients who underwent revascularization
(PCI). Thus the study enrolled only a subset of the ACS population.
There is also emerging data from clinical studies supporting the anti-inflammatory actions
of statins. One recent randomized controlled study demonstrated that statins decrease the
levels of CRP, considered to be a marker of intra-arterial inflammation and a predictor of
recurrent adverse cardiovascular events. The relative levels of various lipid measurements,
such as LDL-C, triglycerides and HDL-C probably influence the inflammatory and thrombotic
(blood clotting) properties, but the exact relationship is not clear. The anti-inflammatory
and antithrombotic properties of different statins are likely related to their impact on the
lipid profile and their different pleiotropic properties (producing more than one genetic
effect).
The present study is designed to compare the effects of rosuvastatin 20 mg versus
atorvastatin 80 mg started at maximum 6 days after an ACS to lipid profile (blood
cholesterol). Additionally, the hypothesis of beneficial effect on inflammatory markers
compared with statins started later will be tested.
c) Summary of study design:
This is a 3-month, randomized, parallel-group study with 2 periods, comparing the efficacy
and the safety of rosuvastatin 20 mg versus atorvastatin 80 mg in patients with an acute
coronary syndrome (ACS).
- The study comprises a 1st double blind, placebo controlled, period that starts at the
admission of the patient for an ACS (clinical symptoms less than 24 hours) until
hospital discharge (or a maximum timeline of 6 days).
- The 2nd double blind, double dummy, period starts at Day 0 (i.e. from the hospital
discharge or at a maximum of 6 days after admission) and will last 3 months. After
validation of eligibility criteria (including a 1st local assessment of CK, creatinine,
ALT and an ECG) and the planning of a PCI between 24 hours and 4 days after admission,
patients will be randomized into 3 groups:
1. early started rosuvastatin 20 mg from admission until the end of the study (group
1 - early rosuvastatin 20 mg),
2. placebo from admission until Day O (i.e. until hospital discharge or for a maximum
of 6 days) followed by rosuvastatin 20 mg until the end of the study (group 2 -
late rosuvastatin 20 mg),
3. placebo from admission until Day O (i.e. until hospital discharge or for a maximum
of 6 days) followed by atorvastatin 80 mg until the end of the study (group 3 -
atorvastatin 80 mg).
;
Allocation: Randomized, Endpoint Classification: Safety/Efficacy Study, Intervention Model: Parallel Assignment, Masking: Double Blind (Subject, Caregiver, Investigator, Outcomes Assessor), Primary Purpose: Treatment
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