Asthma and Allergy Research Group, Medical Research Institute, University of Dundee, Ninewells Hospital and Medical School, , Dundee, UK.
Heart. 2014 Feb;100(3):219-23. doi: 10.1136/heartjnl-2013-304769. Epub 2013 Nov 7.
Despite their benefits in the treatment of cardiovascular disease, β-blockers are seldom used to treat asthmatics. We assessed the safety and tolerability of acute dosing with esmolol and propranolol in patients with asthma.
Post-hoc analysis of a double blind, randomised, placebo controlled trial of β-blocker use in asthma.
Mild-to-moderate asthmatics on inhaled corticosteroids.
Each participant underwent a 6-8 week dose titration of oral propranolol. A subgroup received an intravenous bolus dose of esmolol (0.5 mg/kg). Measurements were recorded pre- and post-esmolol and first dose exposure to 10 mg, 20 mg, and 80 mg of propranolol. Tiotropium was given concurrently with propranolol. Bronchoconstriction was reflected as a fall in forced expiratory volume in 1 s (FEV1) or increase in total airway resistance at 5 Hz (R5).
12 patients completed the trial. There were no adverse effects on FEV1% or R5% following intravenous esmolol. There were significant reductions at 2 min post-esmolol in heart rate (-4.7 beats/min (bpm), 95% CI -7.9 to -1.3 bpm; p=0.002) and systolic blood pressure (-5.9 mm Hg, 95% CI -11.4 to -0.4 mm Hg; p=0.03). No bronchoconstriction was seen during up titration following the first dose of 10 mg, 20 mg or 80 mg of propranolol in the presence of tiotropium. No difference in the asthma control questionnaire at 80 mg propranolol was seen versus placebo in the presence of tiotropium.
Intravenous esmolol was administered without any adverse effects on pulmonary function in selected, stable, mild-to-moderate asthmatics controlled on inhaled corticosteroids. Tiotropium prevented propranolol induced bronchoconstriction after acute dosing during up-titration to 80 mg with no adverse impact on asthma control.
尽管β受体阻滞剂在心血管疾病治疗中有诸多益处,但在哮喘患者的治疗中却很少使用。我们评估了艾司洛尔和普萘洛尔在哮喘患者中的急性给药的安全性和耐受性。
对β受体阻滞剂在哮喘中的使用进行双盲、随机、安慰剂对照试验的事后分析。
吸入皮质激素的轻度至中度哮喘患者。
每位参与者接受口服普萘洛尔的 6-8 周剂量滴定。亚组接受艾司洛尔静脉推注(0.5mg/kg)。在艾司洛尔给药前和给药后以及首次暴露于 10mg、20mg 和 80mg 普萘洛尔时进行测量。同时给予噻托溴铵和普萘洛尔。支气管收缩反映为用力呼气量第一秒(FEV1)下降或 5Hz 总气道阻力(R5)增加。
12 名患者完成了试验。静脉注射艾司洛尔后,FEV1%或 R5%无不良反应。艾司洛尔给药后 2 分钟,心率显著下降(-4.7 次/分钟(bpm),95%置信区间-7.9 至-1.3bpm;p=0.002),收缩压下降(-5.9mmHg,95%置信区间-11.4 至-0.4mmHg;p=0.03)。在噻托溴铵存在的情况下,首次给予 10mg、20mg 或 80mg 普萘洛尔后进行上调滴定期间,未见支气管收缩。在噻托溴铵存在的情况下,80mg 普萘洛尔与安慰剂相比,哮喘控制问卷无差异。
在吸入皮质激素控制的、稳定的轻度至中度哮喘患者中,静脉内给予艾司洛尔不会对肺功能产生任何不良反应。在增加至 80mg 剂量的过程中,噻托溴铵可防止急性给药后普萘洛尔引起的支气管收缩,且对哮喘控制无不良影响。
