Bangalore Sripal, Messerli Franz H, Cohen Jerome D, Bacher Peter H, Sleight Peter, Mancia Giuseppe, Kowey Peter, Zhou Qian, Champion Annette, Pepine Carl J
Division of Cardiovascular Medicine, St. Luke's-Roosevelt Hospital Center, New York, NY 10025, USA.
Am Heart J. 2008 Aug;156(2):241-7. doi: 10.1016/j.ahj.2008.02.023.
In patients with prior myocardial infarction (MI), beta-blockers reduce mortality by 23% to 40%. However, despite this favorable effect, adverse effects limit compliance to this medication. The purpose of the study was to compare a beta-blocker-based strategy with a heart rate-lowering calcium antagonists-based strategy in patients with prior MI.
We evaluated 7,218 patients with prior MI enrolled in the INternational VErapamil SR-Trandolapril (INVEST) substudy randomized to verapamil-sustained release (SR)- or atenolol-based strategies. Primary outcome was time to first occurrence of death (all-cause), nonfatal MI, or nonfatal stroke. Secondary outcomes included death, total MI (fatal and nonfatal), and total stroke (fatal and nonfatal) considered separately.
During the 2.8 +/- 1.0 years of follow-up, patients assigned to the verapamil-SR-based and atenolol-based strategies had comparable blood pressure control, and the incidence of the primary outcome was equivalent. There was no difference between the 2 strategies for the outcomes of either death or total MI. However, more patients reported excellent/good well-being (82.3% vs 78.0%, P = .02) at 24 months with a trend toward less incidence of angina pectoris (12.0% vs 14.3%, adjusted P = .07), nonfatal stroke (1.4% vs 2.0%; P = .06), and total stroke (2.0% vs 2.5%, P = .18) in the verapamil-SR-based strategy group.
In hypertensive patients with prior MI, a verapamil-SR-based strategy was equivalent to a beta-blocker-based strategy for blood pressure control and prevention of cardiovascular events, with greater subjective feeling of well-being and a trend toward lower incidence of angina pectoris and stroke in the verapamil-SR-based group.
在既往有心肌梗死(MI)的患者中,β受体阻滞剂可使死亡率降低23%至40%。然而,尽管有这种有益作用,但不良反应限制了患者对该药物的依从性。本研究的目的是比较在既往有MI的患者中,基于β受体阻滞剂的治疗策略与基于降低心率的钙拮抗剂的治疗策略。
我们评估了7218例既往有MI且参加国际维拉帕米缓释片 - 群多普利(INVEST)子研究的患者,这些患者被随机分配至基于维拉帕米缓释片(SR)或阿替洛尔的治疗策略组。主要结局是首次发生死亡(全因)、非致死性MI或非致死性卒中的时间。次要结局包括分别考虑的死亡、总MI(致死性和非致死性)和总卒中(致死性和非致死性)。
在2.8±1.0年的随访期间,分配至基于维拉帕米缓释片和基于阿替洛尔治疗策略组的患者血压控制情况相当,主要结局的发生率相当。两种策略在死亡或总MI结局方面无差异。然而,在24个月时,更多患者报告基于维拉帕米缓释片策略组的健康状况为优/良(82.3%对78.0%,P = 0.02)且心绞痛发生率有降低趋势(12.0%对14.3%,校正P = 0.07)、非致死性卒中(1.4%对2.0%;P = 0.06)和总卒中(2.0%对2.5%,P = 0.18)。
在既往有MI的高血压患者中,基于维拉帕米缓释片的治疗策略在血压控制和预防心血管事件方面与基于β受体阻滞剂的治疗策略相当,基于维拉帕米缓释片组患者的主观幸福感更强,且心绞痛和卒中发生率有降低趋势。
