Hudson Michael P, Armstrong Paul W, Ruzyllo Witold, Brum Jose, Cusmano Lisa, Krzeski Piotr, Lyon Robert, Quinones Miguel, Theroux Pierre, Sydlowski Diana, Kim Henry E, Garcia Mario J, Jaber Wael A, Weaver W Douglas
Henry Ford Heart and Vascular Institute, Detroit, Michigan 48202, USA.
J Am Coll Cardiol. 2006 Jul 4;48(1):15-20. doi: 10.1016/j.jacc.2006.02.055. Epub 2006 Jun 21.
We sought to determine whether matrix metalloproteinase (MMP) inhibitor, PG-116800, reduced left ventricular (LV) remodeling after myocardial infarction (MI).
PG-116800 is an oral MMP inhibitor with significant antiremodeling effects in animal models of MI and ischemic heart failure.
In an international, randomized, double-blind, placebo-controlled study, 253 patients with first ST-segment elevation MI and ejection fraction between 15% and 40% were enrolled 48+/- 24 h after MI and treated with placebo or PG-116800 for 90 days. Major efficacy end points were changes in LV volumes as determined by serial echocardiography, and clinical and safety outcomes were also collected.
In total, 203 patients (80%) completed 90 days of treatment and had evaluable baseline and 90-day echocardiograms. The proportion of patients with anterior MI (78% vs. 81%) and primary percutaneous coronary intervention (90% vs. 91%) along with baseline LV ejection fraction (35.5% vs. 36.8%) did not differ between PG-116800-treated and placebo-treated patients. There was no difference in the change in LV end-diastolic volume index from days 0 to 90 with PG-116800 versus placebo (5.09 +/- 1.45 ml/m(2) vs. 5.48 +/- 1.41 ml/m2, p = 0.42). Changes in LV diastolic volume, LV systolic volume, LV ejection fraction, sphericity index, plus rates of death or reinfarction were not significantly improved with PG-116800. PG-116800 was well tolerated; however, there was increased incidence of arthralgia and joint stiffness without significant increase in overall musculoskeletal adverse events (21% vs. 15%, p = 0.33).
Matrix metalloproteinase inhibition with PG-116800 failed to reduce LV remodeling or improve clinical outcomes after MI.
我们试图确定基质金属蛋白酶(MMP)抑制剂PG - 116800是否能减轻心肌梗死(MI)后的左心室(LV)重构。
PG - 116800是一种口服MMP抑制剂,在MI和缺血性心力衰竭动物模型中具有显著的抗重构作用。
在一项国际、随机、双盲、安慰剂对照研究中,253例首次发生ST段抬高型MI且射血分数在15%至40%之间的患者在MI后48±24小时入组,接受安慰剂或PG - 116800治疗90天。主要疗效终点是通过连续超声心动图测定的LV容积变化,同时收集临床和安全性结果。
总共203例患者(80%)完成了90天的治疗,并拥有可评估的基线和90天超声心动图。接受PG - 116800治疗的患者与接受安慰剂治疗的患者相比,前壁MI患者比例(78%对81%)、直接经皮冠状动脉介入治疗比例(90%对91%)以及基线LV射血分数(35.5%对36.8%)并无差异。从第0天到第90天,PG - 116800与安慰剂相比,LV舒张末期容积指数的变化无差异(5.09±1.45 ml/m²对5.48±1.41 ml/m²,p = 0.42)。PG - 116800并未显著改善LV舒张容积、LV收缩容积、LV射血分数、球形指数以及死亡或再梗死率。PG - 116800耐受性良好;然而,关节痛和关节僵硬的发生率增加,而总体肌肉骨骼不良事件无显著增加(21%对15%,p = 0.33)。
PG - 116800抑制基质金属蛋白酶未能减轻MI后的LV重构或改善临床结局。
