Busse William, Koenig Steven M, Oppenheimer John, Sahn Steven A, Yancey Steven W, Reilly Donna, Edwards Lisa D, Dorinsky Paul M
University of Wisconsin, Medical School, Madison 53792, USA.
J Allergy Clin Immunol. 2003 Jan;111(1):57-65. doi: 10.1067/mai.2003.38.
Concurrent use of an inhaled corticosteroid (ICS) and an inhaled long-acting beta2-agonist provides better overall asthma control than the use of higher doses of ICS alone.
The purpose of this investigation was to determine whether fluticasone propionate (FP) combined with salmeterol in the Diskus device can be used to reduce the dose of ICS in patients currently stable on medium-dose ICS while maintaining asthma control.
This was a randomized, double-blind, parallel-group, 12- to 24-week trial consisting of a 3-part run-in period. The run-in period was designed to first establish FP 250 microg administered twice a day (bid) via Diskus as the minimum effective dose. During run-in period 1, patients received FP 220 microg bid or the equivalent for 10 to 14 days. Controlled patients moved to run-in period 2 (5-28 days), which assessed asthma stability on FP 100 microg bid administered via Diskus. Only patients who became unstable on FP 100 microg bid were eligible to enter run-in period 3 (26-30 days), during which they were placed on FP 250 microg bid and those regaining asthma control were eligible for randomization. The primary efficacy endpoint was the proportion of patients who remained in the study with no evidence of worsening asthma. Secondary efficacy measures included FEV1, morning peak expiratory flow, percent of symptom-free days, and daily albuterol use.
Only 5% of patients treated with FP100/salmeterol withdrew because of worsening asthma in the first 12 weeks; this compared with 7% in the FP250 group. All patients from a subset of sites continued in the study for an additional 12 weeks; only an additional 1% of patients treated with either FP100/salmeterol or FP250 withdrew because of worsening asthma. Secondary efficacy measures confirmed primary efficacy results.
In patients requiring FP250 bid for asthma stability, FP100/salmeterol bid was steroid-sparing, allowing a 60% reduction in the FP dose while maintaining overall asthma control.
与单独使用高剂量吸入性糖皮质激素(ICS)相比,联合使用吸入性糖皮质激素(ICS)和吸入性长效β2受体激动剂能更好地全面控制哮喘。
本研究旨在确定碟式吸入器中丙酸氟替卡松(FP)与沙美特罗联合使用是否可用于减少目前使用中等剂量ICS病情稳定的患者的ICS剂量,同时维持哮喘控制。
这是一项随机、双盲、平行组、为期12至24周的试验,包括一个为期3部分的导入期。导入期旨在首先确定通过碟式吸入器每天两次(bid)给予250微克FP作为最小有效剂量。在导入期1,患者接受bid 220微克FP或等效药物治疗10至14天。病情得到控制的患者进入导入期2(5至28天),评估通过碟式吸入器bid给予100微克FP时哮喘的稳定性。只有在bid给予100微克FP时病情变得不稳定的患者才有资格进入导入期3(26至30天),在此期间他们接受bid 250微克FP治疗,那些哮喘得到控制的患者有资格进行随机分组。主要疗效终点是留在研究中且无哮喘恶化迹象的患者比例。次要疗效指标包括第1秒用力呼气容积(FEV1)、早晨呼气峰值流速、无症状天数百分比和每日沙丁胺醇使用量。
在最初的12周内,接受FP100/沙美特罗治疗的患者中只有5%因哮喘恶化而退出;而FP250组为7%。来自部分研究点的所有患者继续进行了另外12周的研究;接受FP100/沙美特罗或FP250治疗的患者中只有另外1%因哮喘恶化而退出。次要疗效指标证实了主要疗效结果。
对于需要bid给予250微克FP以维持哮喘稳定的患者,bid给予100微克FP/沙美特罗可减少激素用量,在维持哮喘总体控制的同时使FP剂量降低60%。
Zotero 插件