Myocardial Infarction Clinical Trial
Official title:
A Randomized Comparison of Excimer LASER vs Manual Thrombus Aspiration for the Prevention of No-reflow During Primary Percutaneous Coronary Intervention of St-elevation Myocardial Infarction(LASER-AMI Study)
The occurrence of no-reflow phenomenon after recanalization of the infarct related artery in
acute myocardial infarction is described in up to 40% of cases. This event is associated
with a worse prognosis at follow up and an unfavourable left ventricular remodelling. Two
main pathogenetic mechanisms cause no-reflow: distal embolization, ischemia-reperfusion
injury and individual susceptibility. In such a context, Excimer Laser (EL) may play an
important role in order to reduce the rate of microvascular obstruction.
Thus, in this randomized study we will assess the effect of EL versus Manual Thrombus
Aspiration for ST elevation MI using ST segment resolution on standard 12 leads ECG as
primary endpoint of myocardial reperfusion.
Acute myocardial infarction (AMI) is the leading cause of death in developed countries. In
patients with AMI, prompt reopening of an occluded coronary artery is the main goal of
reperfusion therapies in order to restore normal blood flow to the myocardium, thus
preventing left ventricular (LV) adverse remodelling and occurrence of heart failure.
Primary percutaneous coronary intervention (PPCI) represents the pivotal step in the current
management of ST-segment elevation myocardial infarction (STEMI) (1). Yet, in a sizable
proportion of patients, PPCI achieves epicardial coronary artery reperfusion but not
myocardial reperfusion, a condition known as no-reflow (2), that increases the extent of
myocardial damage. The proportion of patients who get optimal myocardial reperfusion, among
those without cardiogenic shock undergoing PPCI, is about 35% (3). Thus, the prevalence of
no-reflow remains extremely high. Furthermore, a series of consistent data has clearly shown
that no-reflow has a strong negative impact on outcome, negating the potential benefit of
PPCI (4-10). Indeed, as compared to patients without no-reflow, patients with no-reflow
exhibit a higher prevalence of: 1) early post-infarction complications (arrhythmias,
pericardial effusion, cardiac tamponade, early congestive heart failure); 2) LV adverse
remodelling; 3) late re-hospitalizations for heart failure; 4) mortality. In man, no-reflow
is caused by the variable combination of four pathogenetic mechanisms: 1) distal
atherothrombotic embolization, 2) ischemic injury, 3) reperfusion injury, 4) susceptibility
of coronary microcirculation to injury (3). As a consequence, appropriately designed
strategies to prevent or to treat, at the right time, each of these components are expected
to reduce the final number of patients with no-reflow. Manual thrombus aspiration (MTA) has
been clearly shown to improve microvascular perfusion and survival in STEMI patients treated
by PPCI (9,10). Accordingly, in current guidelines of the European Society of Cardiology
(ESC), MTA is a 2a recommendation (1). Yet, complete ST-segment resolution (defined as >70%)
is obtained in only about 50% of patients (3,6), thus suggesting that microvascular
perfusion may be further improved. In such a context, Excimer laser (EL) may play an
important role in order to reduce the rate of microvascular obstruction. Coronary lasers are
devices emitting electromagnetic energy which, upon absorption within the atherosclerotic
plaque, can debulk the target tissue (11-12). Over the past decade, a second generation of
pulsed-wave lasers was introduced (13). These devices combine a brief pulse duration of
light emission with a long pause interval, thus ensuring prevention of thermal injury and
adverse effect on the arterial wall to be laser. The pulsed wave EL (308 nm, ultraviolet
wavelength, in the UVB region of the spectrum) is an FDA and EMEA approved device for
treatment of atherosclerotic coronary lesions considered "non ideal" for standard balloon
angioplasty (14-16). Furthermore, continuous saline flush of saline during laser advancement
has allowed to further reduce heat generation and tissue damage. Taken together device
improvement and technical advancement have allowed to lower procedural complication rate and
to confirm in published registries the safety of the EL assisted angioplasty (17-18). In the
setting of thrombotic lesion, EL has the potential to vaporize thrombotic and plaque
material, leading to particles smaller than the size of erythrocytes unlikely to plug the
microcirculation (19-20), and inhibits platelet aggregation, by inducing platelets stunning
(21). Furthermore, laser is able to debulk underlying thrombogenic plaque thus limiting its
thrombogenicity (22). EL has been used in the setting of STEMI within registries (23-26) and
in a small randomized trial vs balloon assisted PPCI (27), showing a very low rate of
myocardial no-reflow, as assessed by angiography (around 5%) and electrocardiography (around
35%). These studies, however, were limited by the small sample size and for most of them by
the non-randomized design. Thus, a randomized study of EL assisted PPCI has become necessary
in order to evaluate the efficacy of this mechanical strategy for STEMI patients. As
MTA-assisted PPCI is nowadays the recommended approach by current guidelines, the
effectiveness of EL-assisted PPCI should be evaluated against MTA-assisted PPCI. The goal of
this trial, which will be carried out in patients with STEMI undergoing PPCI, is to assess
the superiority of EL-assisted vs MTA-assisted PPCI, having as primary end-point the rate of
90-min ST segment resolution>70% and as secondary end-points the rate of angiographic
no-reflow, defined as TIMI flow3 and MBG >=2 (28), the evaluation of infarct size, as
assessed by the area under the curve of cardiac markers (29) and the rate of adverse
remodelling as assessed by echocardiography at 6 months follow-up
Description of LASER-AMI trial
Study design
LASER-AMI is a randomized, open-label, blind-examination (PROBE), active controlled,
multinational clinical trial. Patients undergoing PPCI will be randomly assigned to 1 of 2
interventional strategies of reperfusion: MTA-assisted PPCI alone or EL-assisted PPCI alone.
Study protocol and procedure
The informed consent will be signed before angiography. The randomization process will start
after the completion of diagnostic angiography and patients will be allocated to one of the
following two arms: MTA-assisted PPCI alone; or EL-assisted PPCI alone. A consecutively
numbered and sealed envelope will be opened to have knowledge of the randomization arm. Each
enrolling center will receive from the promoting center an exact number of numbered
envelopes to use for the randomization.
The interventional procedure will be carried out according to usual site's local protocol.
The choice of vascular access and stent type will be left to operator discretion. All
patients will receive aspirin per os (150-325 mg), clopidogrel (600 mg) or prasugrel or
ticagrelor in the emergency department. Anticoagulant therapy in the catheterization
laboratory will be left to the operator's choice according to recent ESC guidelines (1); GP
IIb/IIIa inhibitors will be considered for bailout therapy if there is angiographic evidence
of massive thrombus, slow or no-reflow or a thrombotic complication. After identification of
culprit vessel and crossing the lesion by the guidewire, vessel recanalization will start by
using either MTA or EL, according to randomization (see appendix 1 about advices for ELCA
use). The choice of the MTA devices will be left to each site's usual availability.
Complications related to either ELCA or MTA will be recorded (perforation, dissection) as
well as failure to restore antegrade flow and lack of crossing culprit stenosis. The use of
balloon after MTA or EL is left to operator discretion, even if direct stenting is
recommended. In all patients, after MTA or ELCA, intracoronary adenosine (120 µg as fast
bolus followed by 2 mg given in 33cc of saline in 2 minutes as slow bolus) will be
administered.
Vessel recanalization will be completed by coronary stenting. Postdilatation of the stent is
left to the operator's discretion, although stent overexpansion is not recommended in order
to reduce the risk for no-reflow.
Angiographic and electrocardiography analysis
Angiographic analysis will be performed off-line by the angio core lab (IsMeTT, Palermo,
Italy) and will include: quantitative coronary angiography (31), TIMI flow (32), corrected
TIMI frame count (33), MBG (34), combined evaluation of TIMI flow and MBG (27), thrombus
score (35), and Rentrop collateral grading (36). Angiographic no-reflow will be defined as a
final TIMI flow of < 2 or final TIMI flow 3 with a MBG 0/1 (3,27). These parameters will be
assessed according to validated methods (31-36).
At 90 minutes after the end of the procedure a 12 leads ECG will be recorded for the
analysis of ST-segment resolution as compared to admission ECG. Complete ST-segment
resolution will be defined as >70% of ST-segment as compared to baseline in both single lead
showing maximum ST-elevation on admission and on the sum of leads showing ST-elevation on
admission (37,38) Baseline ECG will be also assessed off-line for number of Q waves and
terminal distorsion of QRS (39).
ECG analysis will be performed offline by an ECG core lab (Clinica di Cardiologia, UNIVPM,
Ancona, Italy).
Echocardiographic protocol
At day 3 to 5 and at 6-month after the index procedure all patients will undergo
comprehensive 2D transthoracic echocardiography examination at rest. End-systolic (LVESV)
and end-diastolic volumes (LVEDV), LV ejection fraction (LVEF), presence and degree of
mitral insufficiency and wall motion score index (each segment scored from 1= normal/
hyperkinetic, to 4 = dyskinetic, in a 16 segment model of the left ventricle) will be
calculated following the recommendations of the American Society of Echocardiography (40).
LV volumes and ejection fraction will be measured by modified biplane Simpson's method, and
adjusted for body surface area. LV remodeling will be defined as an increase in
end-diastolic volume > 20% at 6 months after AMI as compared to in-hospital examination (7).
Serious Adverse Events
Serious adverse events will be recorded and defined as any untoward medical occurrence that
results in cardiac death, vascular death, death, re-infarction, target lesion
revascularization, target vessel revascularization, or stent thrombosis. They will be
communicated to the Safety Board within 24hours from their occurrence.
Blood sampling
Blood samples will be collected before the PCI and at 4, 8, 12, 24, 36, 48, and 72 h after
the procedure to measure creatine kinase-myocardial band (CK-MB) (mass), troponin-T (mass),
and hemoglobin levels.
Clinical follow-up
The incidence of cardiac death, myocardial infarction, target lesion revascularization and
heart failure requiring hospitalization will be assessed at 6 months by interview and
clinical check and at 1 year by telephone contact. In line with protocol, interviewers and
examiners will not know which drug was administrated at the time of procedure. The
accumulation of such end-points will be defined as major adverse cardiac events (MACEs).
Study end-point
The end-point of the study is the comparison of the rate of ST-segment resolution at 90
minutes post PPCI between patients randomized to MTA-assisted PPCI and EL-assisted PPCI.
Thus, the study will test whether EL-assisted PPCI is superior to MTA-assisted PPCI in
reducing of the incidence of electrocardiographic no-flow after performing PPCI.
Secondary endpoints are: a) angiographic no-reflow defined as a TIMI flow ≤2 or a TIMI flow
3 with a MBG 0/1; b) LVESV, LVEDV, LVEF, and WMSI assessed by in-hospital and 6 months
echocardiography; c) infarct size, defined as CK-MB and troponin-I area under the curve; d)
MACEs rate in the two groups at 6 and 1 year follow-up.
Power calculation
LASER-AMI is a randomized, open-label clinical trial, in which patients will be randomly
assigned to 1 of 2 interventional strategies (MTA-assisted PPCI; or EL-assisted PPCI). The
primary objective of LASER-AMI trial is to test the superiority of EL-assisted PPCI vs
MTA-assisted PPCI based on the rate of post-procedural STR>70% after PPCI. The study sample
size was powered to demonstrate a significant difference in the primary end point of rate
STR >70%, which was around 56% in a previous trial of PPCI with MTA only (10). Starting from
such figures and thus assuming an 76% event rate in the control group with an absolute 20%
decrease in the experimental group, we calculated that 194 patients (97 per group) had to be
enrolled to have an alpha error of 0.05 and a power of 0.80 in a prospective 1:1 randomized
study.
Statistical analysis
All analyses will be planned and conducted according to the intention-to-treat principle, as
this approach minimizes the risk of selection bias and alpha error. Continuous variables
(presented as mean ± standard deviation) will be compared by the Student t test for normally
distributed variables and by the Wilcoxon test for nonnormally distributed variables.
Chi-square tests will be used to compare discrete variables (reported as raw numbers [%]).
Odds ratios (OR) with 95% confidence intervals (CI) will be calculated to compare event
rates in the EL-assisted PPCI group versus those observed in the MTA-assisted PPCI group
(considered as the control group). A multivariable logistic regression analysis will be also
performed to further assess and confirm the independent predictive value of randomization to
EL-assisted PPCI for the achievement of STR>70% (cut-off for entry 0.05, cut-off for removal
0.10). Moreover, infarct size assessment will be perfomed, defined as CK-MB and troponin-I
area under the curve, calculated by the linear trapezoidal method (29). If baseline or 72-h
values are missing, the value will be set to 0, whereas missing intermediate values will be
substituted by linear interpolation. For patients dying in the first 72 h after enrollment,
the area under the curve will be set as the largest area under the curve recorded in the
study (29). Analyses will be carried out using SPSS for Windows 11.0 (SPSS Inc., Chicago,
Illinois). Statistical significance will be defined by two-tailed p < 0.05.
In addition, prespecified subgroup analyses by means of multiple logistic regression or
multiple linear regression, as appropriate, will be performed according to the following
variables: age class, sex, diabetes, anterior myocardial infarction, total ischemic time
cutoff, pre-infarction angina, baseline angiographic thrombus score, baseline TIMI flow,
number of diseased vessels.
;
Allocation: Randomized, Endpoint Classification: Efficacy Study, Intervention Model: Parallel Assignment, Masking: Double Blind (Subject, Caregiver, Outcomes Assessor), Primary Purpose: Treatment
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