1 Lung Health Center, University of Alabama at Birmingham and Birmingham VA Medical Center, Birmingham, Alabama.
2 Institute of Health and Wellbeing, University of Glasgow, Glasgow, United Kingdom.
Ann Am Thorac Soc. 2018 May;15(5):608-614. doi: 10.1513/AnnalsATS.201708-626OC.
Cardiovascular disease is a common comorbidity in patients with chronic obstructive pulmonary disease. Although β-blockers can be used safely in patients with chronic obstructive pulmonary disease, concerns remain regarding safety and efficacy interactions in patients using concomitant inhaled long-acting β-agonists.
To compare the differential effects of long-acting β-agonist or inhaled corticosteroid use on clinical outcomes in patients with heightened cardiovascular risk treated and not treated with β-blockers.
We examined data from 16,485 participants in the SUMMIT study (Study to Understand Mortality and Morbidity in COPD) who were randomized to once-daily inhaled fluticasone furoate, vilanterol, fluticasone furoate/vilanterol combination, or placebo and examined the associations between treatment allocation and lung function, chronic obstructive pulmonary disease exacerbations, cardiovascular events, and all-cause mortality, stratified by baseline β-blocker therapy.
Baseline β-blocker therapy was used by 31% (n = 5,159) of SUMMIT participants. There was no evidence of an interaction between baseline β-blocker therapy and the association between inhaled treatments and forced expiratory volume in 1 second at 3 months (P = 0.27), 6 months (P = 0.14), or 12 months (P = 0.33). The placebo-adjusted mean differences in post-bronchodilator forced expiratory volume in 1 second at 3 months in the vilanterol-alone group were 58 ml (95% confidence interval, 38-78) in those receiving baseline β-blocker therapy and 51 ml (95% confidence interval, 38-65) in those not receiving baseline β-blocker therapy. The placebo-adjusted mean differences in post-bronchodilator forced expiratory volume in 1 second at 3 months in the combination fluticasone furoate/vilanterol group were 85 ml (95% confidence interval, 65-105) in those receiving baseline β-blocker therapy and 68 ml (95% confidence interval, 54-82) in those not receiving baseline β-blocker therapy. Overall, there was no evidence of interaction by randomized treatment, including vilanterol alone or in combination with fluticasone furoate, for chronic obstructive pulmonary disease exacerbations (P = 0.18), cardiovascular composite events (P = 0.33), and all-cause mortality (P = 0.41).
There is no evidence to suggest that baseline β-blocker therapy reduces the respiratory benefits or increases the cardiovascular risk of inhaled long-acting β-agonists in patients with chronic obstructive pulmonary disease and heightened cardiovascular risk. Clinical trial registered with www.clinicaltrials.gov (NCT01313676).
心血管疾病是慢性阻塞性肺疾病患者常见的合并症。虽然β受体阻滞剂可安全用于慢性阻塞性肺疾病患者,但对于同时使用吸入长效β激动剂的患者,安全性和疗效之间的相互作用仍存在担忧。
比较长效β激动剂或吸入皮质激素在伴有高心血管风险的患者中的使用对接受和不接受β受体阻滞剂治疗的患者的临床结局的差异影响。
我们对 SUMMIT 研究(评估慢性阻塞性肺疾病死亡率和发病率的研究)的 16485 名参与者的数据进行了检查,这些参与者被随机分配接受每日一次吸入糠酸氟替卡松、维兰特罗、糠酸氟替卡松/维兰特罗联合治疗或安慰剂,并根据基线β受体阻滞剂治疗情况,对治疗分配与肺功能、慢性阻塞性肺疾病加重、心血管事件和全因死亡率之间的关系进行了研究。
基线时,31%(n=5159)的 SUMMIT 参与者接受了β受体阻滞剂治疗。在 3 个月(P=0.27)、6 个月(P=0.14)和 12 个月(P=0.33)时,基线β受体阻滞剂治疗与吸入治疗与 1 秒用力呼气量之间的相关性之间没有证据表明存在交互作用。在接受基线β受体阻滞剂治疗的维兰特罗单药组中,支气管扩张剂后 1 秒用力呼气量在 3 个月时的安慰剂校正平均差异为 58ml(95%置信区间,38-78),而在未接受基线β受体阻滞剂治疗的患者中为 51ml(95%置信区间,38-65)。在接受基线β受体阻滞剂治疗的糠酸氟替卡松/维兰特罗联合组中,支气管扩张剂后 1 秒用力呼气量在 3 个月时的安慰剂校正平均差异为 85ml(95%置信区间,65-105),而在未接受基线β受体阻滞剂治疗的患者中为 68ml(95%置信区间,54-82)。总体而言,包括维兰特罗单药或与糠酸氟替卡松联合治疗在内的随机治疗均无交互作用的证据,用于慢性阻塞性肺疾病加重(P=0.18)、心血管复合事件(P=0.33)和全因死亡率(P=0.41)。
没有证据表明基线β受体阻滞剂治疗会降低伴有高心血管风险的慢性阻塞性肺疾病患者吸入长效β激动剂的呼吸获益或增加心血管风险。临床试验在 www.clinicaltrials.gov 注册(NCT01313676)。