This double-blind, double-dummy drug, international trial included patients aged 19 to 80 years who presented with an accelerating pattern of prolonged (>20 minutes) or recurrent angina, either at rest or during minimal exertion within the preceding 48 hours, in association with positive cardiac biomarkers (troponin or creatinine kinase MB isoenzyme), with at least one coronary stenosis that required PCI. Although not mandated, a strategy of early invasive management (within 24 hours of hospital admission) was the standard of care at all participating centers for patients who presented with an acute coronary syndrome (ACS) and elevated cardiac biomarkers. All patients were treated with 325 to 500 mg of aspirin and 600 mg of clopidogrel before study drug administration. A total of 1721 NSTEMI patients were randomized to abciximab plus UFH (n=861) or bivalirudin (n=860) immediately before PCI. Baseline characteristics were well balanced between groups. The mean age of patients was 67.5 years, over 20% were female, almost one-third had diabetes mellitus, and there was a nearly 50-50 split between patients with 1- to 2-vessel coronary artery disease compared with 3-vessel disease. One in 5 patients had a prior MI, one-third had a prior PCI, 10% had prior coronary artery bypass, and the mean left ventricular ejection fraction (LVEF) was 51%, suggesting that these patients were representative of moderate- to high-risk ACS patients who are seen in routine clinical practice. The primary endpoint occurred in 10.9% of the patients in the abciximab group and in 11.0% in the bivalirudin group (relative risk [RR] with abciximab/UFH, 0.99; 95% CI, 0.74 to 1.32; p=0.94). The secondary endpoint occurred in 12.8% of the patients in the abciximab group and in 13.4% in the bivalirudin group (RR, 0.96; 95% CI, 0.74 to 1.25; p=0.76). Major bleeding occurred in 4.6% of the patients in the abciximab group (n=40) versus 2.6% in the bivalirudin group (n=22; RR, 1.84; 95% CI, 1.10 to 3.07; p=0.02) [Kastrati et al. N Engl J Med 2011]. In patients with NSTEMI who are treated with an early invasive strategy, many studies have been performed to define the optimal antithrombotic therapy to be used as adjunct to PCI. Prior to the ISAR-REACT 4 trial, the ACUITY trial also studied patients with NSTEMI [Stone GW. NEJM 2006] and demonstrated similar 30-day rates of net clinical benefit (ischemic plus bleeding outcomes) in patients who were treated with either bivalirudin alone (10.1%), GPIIb/IIIa inhibitor/bivalirudin (11.8%), or a GPIIb/IIIa inhibitor/UFH strategy (11.7%), with significantly lower rates of major bleeding (3.0%, 5.3%, and 5.7% respectively). Despite these impressive results, the ACUITY trial failed to sway many interventional
cardiologists, particularly in the United States, to implement these results and start using bivalirudin more frequently in NSTEMI because of concerns of potential bias that could have been introduced in the open-label design of ACUITY. Now, ISAR-REACT 4 has reported virtually the same results as ACUITY in patients with NSTEMI who have been treated with an early invasive approach in a rigorously conducted double-blind trial, which is reassuring and strengthens the evidence of efficacy and safety for treating patients with ACS who undergo PCI with bivalirudin instead of the previous standard of a GPIIb/IIIa inhibitor and UFH. According to Prof. Kastrati, it appears that bivalirudin merits use in MI patients (including either patients with STEMI, based on the HORIZONS AMI trial [Stone NEJM 2008;358:2218-30], or NSTEMI) but not in stable patients or in those with unstable angina without troponin elevations. He estimated that STEMI and NSTEMI patients together make up about one-third of all those who undergo PCI. “The other two-thirds may just as well receive heparin, as there is no benefit of using bivalirudin, and it is much more expensive,” he said.
CETP Inhibitor Evacetrapib Reduces LDL-C and Raises HDL-C Levels
Written by Rita Buckley
Stephen J. Nicholls, MBBS, PhD, Cleveland Clinic Heart & Vascular Institute, Cleveland, Ohio, USA, presented results from a Phase 2 randomized controlled trial of the novel cholesteryl ester transfer protein (CETP) inhibitor evacetrapib. Compared with placebo or statin monotherapy, evacetrapib with or without a statin increased highdensity lipoprotein cholesterol (HDL-C) and decreased low-density lipoprotein cholesterol (LDL-C) levels in patients with dyslipidemia [Effects of the CETP Inhibitor Evacetrapib Administered as Monotherapy or with Statins on HDL and LDL Cholesterol Trial; NCT01105975]. Several CETP inhibitors are currently undergoing clinical evaluation. However, their effects in combination with the most commonly used statins have not been fully characterized. The purpose of this randomized, doubleblind, multicenter, dose-ranging study was to examine the biochemical effects, safety, and tolerability of evacetrapib as monotherapy and in combination with statins in patients with hypercholesterolemia or low HDL-C levels. The co-primary endpoints were percentage changes from baseline in HDL-C and LDL-C after 12 weeks of treatment.
Peer-Reviewed Highlights from the American Heart Association Scientific Sessions 2011
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Table of Contents for the Digital Edition of MD Conference Express AHA 2011