首页> 外文期刊>European journal of heart failure: journal of the Working Group on Heart Failure of the European Society of Cardiology >Effect of bucindolol on heart failure outcomes and heart rate response in patients with reduced ejection fraction heart failure and atrial fibrillation
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Effect of bucindolol on heart failure outcomes and heart rate response in patients with reduced ejection fraction heart failure and atrial fibrillation

机译:布比多洛对射血分数降低的心力衰竭和心房纤颤患者心力衰竭结局和心率反应的影响

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AimsThere is little evidence of beta-blocker treatment benefit in patients with heart failure and reduced left ventricular ejection fraction (HFREF) and atrial fibrillation (AF). We investigated the effects of bucindolol in HFREF patients with AF enrolled in the Beta-blocker Evaluation of Survival Trial (BEST).Methods and resultsA post-hoc analysis of patients in BEST with and without AF was performed to estimate the effect of bucindolol on mortality and hospitalization. Patients were also evaluated for treatment effects on heart rate and the influence of beta1-adrenergic receptor position 389 (β1389) arginine (Arg) vs. glycine (Gly) genotypes. In the 303/2708 patients in AF, patients receiving bucindolol were more likely to achieve a resting heart rate ≤80 b.p.m. at 3 months (P 0.005) in the absence of treatment-limiting bradycardia. In AF patients and sinus rhythm (SR) patients who achieved a resting heart rate ≤80 b.p.m., there were beneficial treatment effects on cardiovascular mortality/cardiovascular hospitalization [hazard ratio (HR) 0.61, P = 0.025, and 0.79, P = 0.002]. Without achieving a resting heart rate ≤80 b.p.m., there were no treatment effects on events in either group. β1389-Arg/Arg AF patients had nominally significant reductions in all-cause mortality/HF hospitalization and cardiovascular mortality/hospitalization with bucindolol (HR 0.23, P = 0.037 and 0.28, P = 0.039), whereas Gly carriers did not. There was no evidence of diminished heart rate response in β1389-Arg homozygotes. ConclusionIn HFREF patients with AF, bucindolol was associated with reductions in composite HF endpoints in those who achieved a resting heart rate ≤80 b.p.m. and nominally in those with the β1389-Arg homozygous genotype.
机译:目的几乎没有证据表明,对于心力衰竭,左心室射血分数(HFREF)和心房颤动(AF)降低的患者,β受体阻滞剂的治疗获益。我们调查了bucindolol在HFREF房颤患者中的生存率,该研究纳入了Beta受体阻滞剂评估生存试验(BEST)。和住院。还评估了患者对心率的治疗效果以及β1-肾上腺素能受体389(β1389)精氨酸(Arg)与甘氨酸(Gly)基因型之间的关系。在303/2708的房颤患者中,接受布比多洛的患者静息心率≤80b.p.m。在不存在限制治疗性心动过缓的情况下,在3个月时(P <0.005)。在静息心率≤80 bpm的房颤患者和窦性心律(SR)患者中,对心血管死亡率/心血管住院治疗有有益的治疗效果[危险比(HR)0.61,P = 0.025和0.79,P = 0.002] 。没有达到静息心率≤80 b.p.m.,两组中的事件都没有治疗效果。 β1389-Arg/ Arg房颤患者的总因数死亡率/心衰住院率和心律失常/布比多洛的住院率明显降低(HR 0.23,P = 0.037和0.28,P = 0.039),而Gly携带者则没有。没有证据表明β1389-Arg纯合子的心率反应减弱。结论对于静息心率≤80 b.p.m的患者,HFREF合并AF的患者中,bucindolol与复合HF终点降低有关。在名义上具有β1389-Arg纯合基因型的人。

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