Myocardial Infarction Clinical Trial
Official title:
Assessment of the Effects of Aggressive Atorvastatin Therapy on Myocardial Deformation Characteristics, Vascular Rigidity, 24 Hour ECG Monitoring Parameters and Quality of Life in Patients With STEMI
The primary goal
• To assess the effect of atorvastatin in patients treated since the first 24-96 hours of the
disease on the parameters of global and regional myocardial deformation in the infarcted area
and the structural and functional properties of arteries at day 7, at 12, 24, 36 and 48 weeks
of treatment;
The secondary goals. To evaluate the effect of treatment:
- on the parameters of the global and regional myocardial deformation in the intact area
on day 7, on 12, 24, 36 and 48 weeks of treatment;
- on the parameters of the global and regional myocardial deformation depending on the
degree of coronary blood flow restoration by thrombolysis in myocardial infarction
(TIMI)
- on systolic and diastolic left ventricular function in the presence of initial
impairments, or absence of the negative dynamics of these parameters in case of normal
baseline values;
- on the clinical diagnostic criteria for the development or progression of heart failure;
- the dynamics of the duration and extent of myocardial ischemia according to the daily
ECG monitoring on day 7, at 12, 24, 36 and 48 weeks of treatment;
- the appearance of new prognostically significant cardiac arrhythmias
- on the pulse wave velocity
- the thickness of the intima-media complex (IMT); 200 patients are planned to be include
in a randomized, single-center, open, prospective, controlled clinical trial, the
enrollment will be held at the Department of "Therapy" of Medical Institute of Penza
State University.
Definition of the study group:
The patients with STEMI (myocardial infarction with ST-segment elevation) will be included in
the study
- Group 1 STEMI - 100 patients receiving atorvastatin 80 mg / day for 48 weeks;
- Group 2 STEMI - 100 patients receiving atorvastatin 20 mg / day for 48 weeks Planned
number of patients: Pre-Screening - 300 subjects; screening and randomization - 200
subjects.
Patients will be randomized by random number generation to include in the group 1 or 2. All
included patients will be on the standard basis therapy of the coronary artery disease,
according to the national recommendation.
1. Hypotheses:
1. Atorvastatin therapy directly results in improved deformation characteristics of
hibernating myocardium due to its pleiotropic effects on endothelial dysfunction and
atherosclerotic plaque stability, as well as stimulation of angiogenesis in ischemic
zones of myocardium.
2. Long-term atorvastatin therapy improves the morphofunctional properties of large
arteries and decreases the severity of endothelial dysfunction in patients with a
history of myocardial infarction.
3. Atorvastatin causes an anti-ischemic effect, if used for a long time. 2.1. Primary
objective To evaluate the effect of atorvastatin, when started between 24 and 96 hours
after disease onset, on the parameters of global and regional myocardial deformation in
the zone of infarction, as well as morphofunctional properties of arteries, on Day 7 and
Weeks 12, 24, 36 and 48 of the treatment; 2.2. Secondary objectives. To evaluate:
- the effect of treatment on the parameters of global and regional myocardial
deformation in the zone of intact myocardium on Day 7 and Weeks 12, 24, 36 and 48
of the treatment;
- the effect of treatment on the parameters of global and regional myocardial
deformation depending on TIMI blood flow grade;
- the effect of treatment on systolic and diastolic function of the left ventricle in
patients with impaired left ventricular function at baseline, as well as the
ability of this treatment to prevent deterioration of left ventricular function in
patients with normal left ventricular function at baseline;
- the effect of treatment on heart failure development and progression as assessed
using the corresponding clinical diagnostic criteria;
- the effect of treatment on duration and time course of myocardial ischemia using 24
hour ECG monitoring on Day 7 and Weeks 12, 24, 36 and 48 of treatment;
- the effect of treatment on the appearance of new prognostically significant
disorders of cardiac rhythm;
- the effect of treatment on pulse wave velocity and cardio-ankle vascular index
(CAVI);
- the effect of treatment on intima-media thickness (IMT);
- the effect of treatment on the results of automated quantitative vascular
elasticity measurements, pulse wave and pulse pressure;
- the effect of treatment on endothelial function using the reactive hyperemia test;
- the effect of treatment on the time course of blood chemistry parameters (i.e.,
total cholesterol, HDL, LDL, triglycerides, creatinine, C-reactive protein (CRP),
alanine transaminase (ALT), aspartate transaminase (AST) and creatinkinase (CK);
- the safety of treatment;
- the effect of treatment on patient's well-being and quality of life;
- patient compliance with the therapy. 2.3. Scientific novelty of the study It is
planned to study, for the first time, the effect of long-term aggressive statin
therapy on the functional status of myocardium in the zone of ischemia, lesion and
necrosis in patients with STEMI using the two-dimensional strain procedure.
It is planned, for the first time, to comprehensively study the effect of aggressive statin
therapy on the status of vasculature, with measuring multiple parameters characterizing the
morphofunctional status of elastic and muscular arteries in patients with documented coronary
heart disease (CHD).
2.4. Clinical significance of study results. If the proposed hypotheses are confirmed after
the primary endpoints described in Section 3 have been reached, new convincing evidence
supporting the use of long-term aggressive treatment with Atorvastatin starting from the
early stages of myocardial infarction will be obtained. Obviously, the clinical benefits will
include the improved prognosis and decreased risk of repeated vascular events. Favorable
effects of this therapy on the morphofunctional status of arterial vasculature will play an
important role in the treatment of these patients. Positive results of this study can form
the basis for planning and conducting larger studies on pleiotropic effects of Atorvastatin
in patients with a history of myocardial infarction.
3. Primary endpoints
1. Statistically significant differences in spatial and velocity parameters of myocardial
deformation in the zone of previous STEMI as compared to controls.
2. Statistically significant differences in spatial and velocity parameters of myocardial
deformation in the intact zone after STEMI as compared to controls.
3. Statistically significant differences in intima-media thickness (IMT) according to echo
tracking data as compared to controls.
4. Statistically significant differences in carotid-femoral pulse wave velocity and CAVI as
compared to controls.
4. Planning and conducting the study. It is planned to include 200 patients in this
randomized, open-label, single-center, prospective, controlled clinical study; these patients
will be recruited at the Department of Therapy of the Penza State University Medical
Institute.
4.1. Allocation to study groups:
Patients with STEMI will be included in this study:
Group 1: 100 patients with STEMI to receive atorvastatin at a dose of 80 mg per day for 48
weeks; Group 2: 100 patients with STEMI to receive atorvastatin at a dose of 20 mg per day
for 48 weeks.
4.2. Planned number of patients: Prescreening - 300 patients; screening and randomization -
200 patients.
4.3. Study design. Patients will be randomized using sealed envelopes numbered with
increasing serial numbers from 1 to 200; each envelope will contain information about patient
inclusion into Group 1 or Group 2. Information about treatment schedule and dosing regimen
will be provided separately.
4.3.1. Treatment regimen, dose titration strategy and combination treatment principles
Patients meeting the inclusion criteria and not meeting the exclusion criteria will be
included in the study.
Group A patients will start the treatment between 24 and 96 hours after the onset of STEMI:
• Atorvastatin at a dose of 80 mg per day.
Group K patients will start the treatment between 24 and 96 hours after the onset of STEMI:
• Atorvastatin at a dose of 20 mg per day.
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