常规治疗的有症状的严重慢性心力衰竭患者的短期口服内皮素受体拮抗剂治疗

Short-term oral endothelin-receptor antagonist therapy in conventionally treated patients with symptomatic severe chronic heart failure.

作者信息

Sütsch G, Kiowski W, Yan X W, Hunziker P, Christen S, Strobel W, Kim J H, Rickenbacher P, Bertel O

机构信息

Divisions of Cardiology, Departments of Medicine, University Hospital Zürich, Switzerland.

出版信息

Circulation. 1998 Nov 24;98(21):2262-8. doi: 10.1161/01.cir.98.21.2262.

DOI:10.1161/01.cir.98.21.2262

PMID:9826312

Abstract

BACKGROUND

The vasoconstrictor peptide endothelin-1 (ET-1) is important for increased vascular tone in patients with chronic heart failure, but the effects of endothelin-receptor blockade in addition to conventional triple therapy are unknown.

METHODS AND RESULTS

Thirty-six men (mean age+/-SD, 55+/-8 years) with symptomatic heart failure (NYHA class III; left ventricular ejection fraction, 22.4+/-4.5%) despite treatment with diuretics, digoxin, and ACE inhibitors received, in a double-blind and randomized fashion, either additional oral bosentan (1.0 g BID; n=24) or placebo (n=12) over 2 weeks. Hemodynamic and hormonal (plasma ET-1, norepinephrine, renin activity, and angiotensin II) measurements were obtained before and repeatedly for 24 hours after administration of bosentan on days 1 and 14. Bosentan was discontinued in 1 patient with symptomatic hypotension, and 2 patients (bosentan group) declined hemodynamic investigations on day 14. Compared with placebo, bosentan on day 1 significantly decreased mean arterial pressure (difference from baseline over 12 hours [95% CIs], -13.9% [-16.0% to -11.7%]), pulmonary artery mean (-12.9% [-17. 4% to -8.3%]) and capillary wedge (-14.5% [-20.5% to -8.5%]) pressures, and right atrial pressure (-20.2% [-29.4% to -11.0%]). Cardiac output increased (15.1% [10.7% to 19.7%]), but heart rate was unchanged. Both systemic (-24.2% [-28.1% to -20.3%]) and pulmonary (-19.9% [-28.4% to -11.4%]) vascular resistance were reduced. After 2 weeks, cardiac output had further increased (by 15. 2% [10.8% to 19.6%]) and systemic (-9.3% [-12.3% to -6.4%]) and pulmonary (-9.7% [-16.3% to -3.1%]) vascular resistances further decreased compared with day 1. Heart rate remained unchanged. Plasma ET-1 levels increased after bosentan, but baseline levels of the other hormones were unchanged.

CONCLUSIONS

Additional short-term oral endothelin-receptor antagonist therapy improved systemic and pulmonary hemodynamics in heart failure patients who were symptomatic with standard triple-drug therapy. Further investigations are warranted to characterize the effects of long-term endothelin-receptor antagonist therapy on symptoms, morbidity, and mortality in such patients.

摘要

背景

血管收缩肽内皮素-1（ET-1）在慢性心力衰竭患者血管张力增加中起重要作用，但除传统三联疗法外，内皮素受体阻断的效果尚不清楚。

方法与结果

36名有症状心力衰竭（纽约心脏协会III级；左心室射血分数22.4±4.5%）的男性（平均年龄±标准差，55±8岁），尽管接受了利尿剂、地高辛和ACE抑制剂治疗，仍以双盲随机方式在2周内额外接受口服波生坦（1.0 g，每日两次；n = 24）或安慰剂（n = 12）治疗。在第1天和第14天服用波生坦前及给药后24小时内多次进行血流动力学和激素（血浆ET-1、去甲肾上腺素、肾素活性和血管紧张素II）测量。1例有症状性低血压患者停用波生坦，2例（波生坦组）患者在第14天拒绝进行血流动力学检查。与安慰剂相比，第1天波生坦显著降低平均动脉压（12小时内与基线的差值[95%可信区间]，-13.9%[-16.0%至-11.7%]）、肺动脉平均压（-12.9%[-17.4%至-8.3%]）和毛细血管楔压（-14.5%[-20.5%至-8.5%]）以及右心房压（-20.2%[-29.4%至-11.0%]）。心输出量增加（15.1%[10.7%至19.7%]），但心率未改变。全身血管阻力（-24.2%[-28.1%至-20.3%]）和肺血管阻力（-19.9%[-28.4%至-11.4%]）均降低。2周后，与第1天相比，心输出量进一步增加（15.2%[10.8%至19.6%]），全身血管阻力（-9.3%[-12.3%至-6.4%]）和肺血管阻力（-9.7%[-16.3%至-3.1%]）进一步降低。心率保持不变。服用波生坦后血浆ET-1水平升高，但其他激素的基线水平未改变。