Respiratory Medicines Development Centre, GlaxoSmithKline, Uxbridge, UK.
Clin Ther. 2012 Aug;34(8):1683-95. doi: 10.1016/j.clinthera.2012.06.024. Epub 2012 Jul 13.
Fluticasone furoate (FF) is an inhaled corticosteroid that is structurally and functionally distinct from fluticasone propionate and is under development as a once-daily therapy for asthma.
The objective of this study was to estimate the treatment differences (with 95% CI) in efficacy and safety profile between FF administered once daily in the morning and evening via Rotadisk Diskhaler (see text) in patients with persistent asthma. No hypothesis testing was performed for this comparison.
This was a randomized, double-blind, double-dummy, placebo-controlled, parallel-group study. Patients (ages 16-55 years; peak expiratory flow [PEF] 50%-90% predicted) were randomized to receive 1 of 3 doses of FF Rotadisk or placebo daily for 4 weeks. The sponsor, GlaxoSmithKline, designed the study and selected the study sites. The primary end point was change from baseline in daily trough (pretreatment, prebronchodilator) PEF during the treatment period with FF Rotadisk 100 μg once daily in the morning compared with 100 μg once daily in the evening. Other end points included change from baseline in forced expiratory volume in 1 second, asthma symptom score, adverse events (AEs), 24-hour urinary cortisol excretion, and FF pharmacokinetics.
Five hundred and seventy-five patients (mean age 36.6 years, 56.9% female) formed the intent-to-treat population and were randomly allocated to FF Rotadisk 100 μg once daily in the morning (n = 144), FF Rotadisk 100 μg once daily in the evening (n = 146), FF Rotadisk 250 μg once daily in the evening (n = 142), or placebo (n = 143). Of these patients, 526 (91.5%) completed the study. A smaller proportion of patients in the placebo group (86.7%) than in the active treatment groups completed the study. Mean difference in PEF change from baseline with FF Rotadisk 100 μg once daily in the morning relative to evening was +13.4 L/min (95% CI, 2.3-24.4). However, morning trough values might have been affected by higher placebo response after morning dosing (18.8 vs 8.8 L/min). Trough PEF improved relative to placebo (P ≤ 0.005), with little difference between FF Rotadisk 100 μg morning (19 L/min) and evening (16 L/min) dosing, as with other efficacy measures. Frequencies of all-cause AEs were similar with FF Rotadisk (32%-39%, 2 serious AEs) and placebo (37%, 1 serious AE). No serious AEs were deemed by the investigator to be related to study treatment. Twenty-four-hour urinary cortisol increased from baseline in all groups, but the increase was significantly lower with FF Rotadisk 250 μg group than placebo.
FF Rotadisk administered once daily in the morning or evening was well tolerated and associated with improvements in lung function and asthma symptoms compared with placebo. Improvements seen for FF Rotadisk 100 μg appear to be comparable for morning and evening dosing. Clinical.trials.govNCT01499446.
糠酸氟替卡松(FF)是一种结构和功能上与丙酸氟替卡松不同的吸入性皮质类固醇,正在开发为每日一次治疗哮喘的药物。
本研究旨在评估每日一次早晨和晚上使用 Rotadisk Diskhaler 给药的 FF 在持续性哮喘患者中的疗效和安全性特征的治疗差异(95%CI)。对于这种比较,没有进行假设检验。
这是一项随机、双盲、双模拟、安慰剂对照、平行组研究。患者(年龄 16-55 岁;峰流速[PEF]50%-90%预计值)随机接受 3 种剂量的 FF Rotadisk 或安慰剂,每天一次,持续 4 周。赞助商葛兰素史克设计了这项研究并选择了研究地点。主要终点是与早晨每日一次 100μg FF Rotadisk 相比,每日一次 100μg 晚上使用 FF Rotadisk 治疗期间每日清晨(治疗前,未经支气管扩张剂治疗)PEF 的变化。其他终点包括用力呼气量在 1 秒内的变化、哮喘症状评分、不良事件(AE)、24 小时尿皮质醇排泄和 FF 药代动力学。
575 名患者(平均年龄 36.6 岁,56.9%为女性)构成意向治疗人群,并随机分配至 FF Rotadisk 100μg 每日一次早晨(n=144)、FF Rotadisk 100μg 每日一次晚上(n=146)、FF Rotadisk 250μg 每日一次晚上(n=142)或安慰剂(n=143)。这些患者中有 526 名(91.5%)完成了研究。与活性治疗组相比,安慰剂组完成研究的患者比例较小(86.7%)。与晚上相比,早晨使用 FF Rotadisk 100μg 时 PEF 从基线的平均变化差异为+13.4L/min(95%CI,2.3-24.4)。然而,早晨剂量后安慰剂反应较高可能影响了早晨的低谷值(18.8 与 8.8L/min)。与安慰剂相比,PEF 改善(P≤0.005),FF Rotadisk 100μg 早晨(19L/min)和晚上(16L/min)剂量之间差异较小,其他疗效指标也是如此。FF Rotadisk(32%-39%,2 例严重 AE)和安慰剂(37%,1 例严重 AE)的所有原因 AE 发生率相似。没有严重 AE 被研究者认为与研究治疗有关。所有组的 24 小时尿皮质醇均从基线升高,但与安慰剂相比,FF Rotadisk 250μg 组的升高明显较低。
与安慰剂相比,每日一次早晨或晚上使用 FF Rotadisk 耐受性良好,并与肺功能和哮喘症状的改善相关。FF Rotadisk 100μg 的改善似乎与早晨和晚上给药相当。Clinical.trials.gov NCT01499446。
