No relevant cardiac, pharmacokinetic or safety interactions between roflumilast and inhaled formoterol in healthy subjects: an open-label, randomised, actively controlled study.

Christian de Mey, Nassr Nassr, Gezim Lahu
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Abstract

Background: Roflumilast is an oral, selective phosphodiesterase 4 inhibitor with anti-inflammatory effects in chronic obstructive pulmonary disease (COPD). The addition of roflumilast to long-acting bronchodilators improves lung function in patients with moderate-to-severe COPD. The present study investigated drug-drug interaction effects between inhaled formoterol and oral roflumilast.

Methods: This was a single-centre (investigational clinic), open, randomised, multiple-dose, parallel-group study. In Regimen A, healthy men were treated with roflumilast (500 μg tablet once daily; Day 2-18) and concomitant formoterol (24 μg twice daily; Day 12-18). In Regimen B, healthy men were treated with formoterol (24 μg twice daily; Day 2-18) and concomitant roflumilast (500 μg once daily; Day 9-18). Steady-state plasma pharmacokinetics of roflumilast, roflumilast N-oxide and/or formoterol (Cmax and AUC0-τ) as well as pharmacodynamics - blood pressure, transthoracic impedance cardiography (ZCG), 12-lead digital electrocardiography, peripheral blood eosinophils, and serum glucose and potassium concentrations - were evaluated through Day 1 (baseline), Day 8 (Regimen B: formoterol alone) or Day 11 (Regimen A: roflumilast alone), and Day 18 (Regimen A and B: roflumilast plus formoterol). Blood and urine samples were taken for safety assessment at screening, pharmacokinetic profiling days and Day 19. Adverse events were monitored throughout the study.

Results: Of the 27 subjects enrolled, 24 were evaluable (12 in each regimen). No relevant pharmacokinetic interactions occurred. Neither roflumilast nor formoterol were associated with significant changes in cardiovascular parameters as measured by ZCG, and these parameters were not affected during concomitant administration. Formoterol was associated with a slight increase in heart rate and a corresponding shortening of the QT interval, without changes in the heart rate-corrected QTc interval. There were small effects on the other pharmacodynamic assessments when roflumilast and formoterol were administered individually, but no interactions or safety concerns were seen after concomitant administration. No severe or serious adverse events were reported, and no adverse events led to premature study discontinuation.

Conclusions: No clinically relevant pharmacokinetic or pharmacodynamic interactions were found when oral roflumilast was administered concomitantly with inhaled formoterol, including no effect on cardiac repolarisation. Roflumilast was well tolerated.

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在健康受试者中,罗氟司特与吸入福莫特罗之间不存在相关的心脏、药代动力学或安全性相互作用:一项开放标签、随机、主动控制研究。
背景介绍罗氟司特是一种口服选择性磷酸二酯酶4抑制剂,对慢性阻塞性肺病(COPD)具有抗炎作用。在长效支气管扩张剂中添加罗氟司特可改善中重度慢性阻塞性肺病患者的肺功能。本研究调查了吸入福莫特罗和口服罗氟司特之间的药物相互作用效应:这是一项单中心(研究诊所)、开放、随机、多剂量、平行组研究。在方案 A 中,健康男性接受罗氟司特(500 微克片剂,每天一次;第 2-18 天)和福莫特罗(24 微克,每天两次;第 12-18 天)治疗。在方案 B 中,健康男性接受福莫特罗治疗(24 微克,每天两次;第 2-18 天),同时服用罗氟司特(500 微克,每天一次;第 9-18 天)。对罗氟司特、罗氟司特 N-氧化物和/或福莫特罗的稳态血浆药代动力学(Cmax 和 AUC0-τ)以及药效学--血压、经胸阻抗心电图 (ZCG)、12 导联数字心电图、外周血嗜酸性粒细胞以及血清葡萄糖和钾浓度--进行了评估,评估时间为第 1 天(基线)、第 8 天(方案 B.单用福莫特罗)或第 10 天(方案 B.单用福莫特罗):第 8 天(方案 B:单独使用福莫特罗)或第 11 天(方案 A:单独使用罗氟司特)以及第 18 天(方案 A 和 B:罗氟司特加福莫特罗)。在筛选、药代动力学分析日和第 19 天抽取血液和尿液样本进行安全性评估。在整个研究过程中对不良反应进行监测:结果:在 27 名受试者中,有 24 人接受了评估(每种方案各 12 人)。没有发生相关的药代动力学相互作用。根据 ZCG 测量,罗氟司特和福莫特罗均未引起心血管参数的显著变化,这些参数在同时用药期间也未受到影响。福莫特罗会导致心率轻微加快,QT 间期相应缩短,但心率校正后的 QTc 间期没有变化。罗氟司特和福莫特罗单独给药时对其他药效学评估的影响较小,但同时给药后未发现相互作用或安全问题。没有严重不良反应的报告,也没有导致研究提前终止的不良反应:结论:当口服罗氟司特与吸入福莫特罗同时给药时,没有发现与临床相关的药代动力学或药效学相互作用,包括对心脏复极化没有影响。罗氟司特的耐受性良好。
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