Abstract
A 48-hour course of intravenous unfractionated heparin (UFH) is the standard of treatment in conjunction with fibrin-specific thrombolysis in ST-elevation myocardial infarction (STEMI). In recent trials, the efficacy and safety of in-hospital administration of subcutaneous low-molecular-weight heparins (LMWH), previously proven effective in non-ST-elevation acute coronary syndromes, have been investigated in the setting of STEMI. The aim of this review was to evaluate the available evidence supporting the use of LMWH in STEMI.Overall, about 27,000 patients treated with various thrombolytic regimens, were included in 12 open-label randomized clinical trials, where dalteparin, reviparin or enoxaparin were administered. While acknowledging the wide variability in study dimensions, designs and end-points, a higher efficacy of LMWH was observed overall as compared to placebo, and also to UFH (mainly as regards the occurrence of reinfarction). As regards safety, bleedings were more frequent than placebo and comparable to UFH in LMWH groups, with the exception of the pre-hospital ASSENT-3 PLUS trial, where in elderly patients, enoxaparin had an incidence of intracranial hemorrhage twice higher than UFH. In a recent double-blind, randomized, mega-trial including over 20,000 patients, the superior efficacy on in-hospital and 30-day adverse cardiac events (namely reinfarction), and comparable safety on intracranial bleedings, of enoxaparin compared to UFH, was shown.In conclusion, in-hospital subcutaneous administration of dalteparin, reviparin and enoxaparin, as an adjunct to various thrombolytics in STEMI, appears feasible and at least as effective and safe as 48-hour intravenous treatment with UFH. In accordance with the available strongest evidence, an initial intravenous bolus of enoxaparin followed by twice daily subcutaneous administration for about 1 week should be the preferred regimen, and should be strongly considered instead of intravenous UFH. Along with its easiness of use, not requiring laboratory monitoring, subcutaneous administration of LMWH following STEMI treated with thrombolysis allows extended antithrombotic treatment, while permitting early mobilization (and rehabilitation) of patients.
Highlights
Rapid and complete dissolution of the occlusive coronary thrombus is the objective of thrombolytic treatment in acute ST-elevation myocardial infarction (STEMI)
low-molecular-weight heparins (LMWH) have increased bioavailability and dose-dependant clearance, which make the anticoagulant response more predictable and routine laboratory monitoring unnecessary. Because of these potential advantages, LMWH have been evaluated in recent years as an adjunct to thrombolysis in STEMI, and are currently recommended as an acceptable alternative to unfractionated heparin (UFH) (Class IIb recommendation), provided that patients are less than 75 years of age and significant renal dysfunction is absent [3, 4]
Highly different in design, thrombolytic agent and LMWH used, these trials generally show a favourable effect of dalteparin, reviparin and enoxaparin on the clinical efficacy end-points, in comparison to placebo [5, 6, 8, 9, 14], and to UFH [15, 11,12,13, 15, 16] (Table 1)
Summary
Rapid and complete dissolution of the occlusive coronary thrombus is the objective of thrombolytic treatment in acute ST-elevation myocardial infarction (STEMI). The ASSENT PLUS trial [7] compared dalteparin with UFH as an adjunct to alteplase in 1639 patients, aiming at evaluating TIMI 3 flow grade at 4-7 days (primary end-point). Evaluation at 30 days by a blinded Clinical Events Committee of the clinical efficacy end-points showed significantly less death/reinfarction with enoxaparin, when administered with full-dose tenecteplase This was mainly due to the reduction in reinfarction, which could be observed when pooling all enoxaparin vs all UFH patients. The primary end-point was the IRA patency rate at 510 days, while secondary end-points were ST-segment resolution at 90’ and 180’ and occurrence of combined death, reinfarction, recurrent angina and major bleedings at 30 days. 30-day mortality was comparable in both groups and neither significant difference in the incidence of major or minor hemorrhage was observed
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