Barnes N C, Pujet J C
London Chest Hospital, Department of Respiratory Medicine, UK.
Thorax. 1997 Jun;52(6):523-7. doi: 10.1136/thx.52.6.523.
Leukotriene receptor antagonists have been shown to protect against bronchoconstriction induced by antigens, exercise, and cold air. There are relatively few clinical studies reported in patients with asthma. The present study is the first clinical evaluation of pranlukast (SB 205312, ONO-1078) outside Japan in patients with asthma.
A randomised, double blind, placebo controlled, parallel group, multicentre four week study of the safety and tolerability of oral pranlukast, 225 or 337.5 mg twice daily, was performed in patients with mild to moderate asthma. Preliminary efficacy data were obtained; the main efficacy variables evaluated were forced expiratory volume in one second (FEV1) and morning domiciliary (home) peak expiratory flow rates (PEFR). Clinic PEFR and daytime and night-time asthma symptom scores were also recorded.
Compared with the placebo group the improvement in morning home PEFR was statistically significant at all time points for patients receiving pranlukast 337.5 mg twice daily and at weeks 1 and 2 for those treated with pranlukast in a dose of 225 mg twice daily. Mean morning home PEFR increased by 10.8 to 18.61/min (95% CI 0.2 to 29.3 l/min) in patients treated with pranlukast compared with a slight deterioration in those given placebo. FEV1 significantly increased within one hour after the first dose of pranlukast compared with baseline and this increase was maintained for eight hours. Improvements in trough FEV1-that is, at the end of the dosing interval-were statistically significant for the group treated with pranlukast 225 mg twice daily compared with placebo at week 4. Mean increases in FEV1 ranged from 210 ml to 340 ml (95% CI 60 to 500 ml) at trough in the pranlukast group. Patients treated with pranlukast also showed improvements in summary symptom and night-time asthma scores. Pranlukast was well tolerated, and no drug related changes in haematological and biochemical variables were observed.
Pranlukast, an oral leukotriene receptor antagonist, is well tolerated and is effective for the treatment of asthma. It increased FEV1 within one hour of dosing, improved patient summary symptom and night-time asthma scores, and reduced the use of rescue bronchodilators, thus providing further evidence of a role for leukotrienes in the pathogenesis of asthma.
白三烯受体拮抗剂已被证明可预防由抗原、运动和冷空气诱发的支气管收缩。在哮喘患者中报道的临床研究相对较少。本研究是在日本境外对哮喘患者进行的普仑司特(SB 205312,ONO - 1078)的首次临床评估。
对轻度至中度哮喘患者进行了一项随机、双盲、安慰剂对照、平行组、多中心为期四周的研究,以评估每日两次口服225或337.5毫克普仑司特的安全性和耐受性。获得了初步疗效数据;评估的主要疗效变量为一秒用力呼气容积(FEV1)和早晨在家中的呼气峰值流速(PEFR)。还记录了门诊PEFR以及白天和夜间哮喘症状评分。
与安慰剂组相比,每日两次服用337.5毫克普仑司特的患者在所有时间点早晨在家中的PEFR改善均具有统计学意义,每日两次服用225毫克普仑司特的患者在第1周和第2周时也有改善。与给予安慰剂的患者略有恶化相比,服用普仑司特的患者早晨在家中的平均PEFR增加了10.8至18.6升/分钟(95%可信区间0.2至29.3升/分钟)。与基线相比,首次服用普仑司特后1小时内FEV1显著增加,且这种增加持续了8小时。与安慰剂相比,在第4周时,每日两次服用225毫克普仑司特的组在给药间隔结束时(即谷值FEV1)的改善具有统计学意义。普仑司特组谷值时FEV1的平均增加范围为210毫升至340毫升(95%可信区间60至500毫升)。接受普仑司特治疗的患者在总体症状和夜间哮喘评分方面也有改善。普仑司特耐受性良好,未观察到血液学和生化变量与药物相关的变化。
口服白三烯受体拮抗剂普仑司特耐受性良好且对哮喘治疗有效。它在给药后1小时内增加FEV1,改善患者总体症状和夜间哮喘评分,并减少急救支气管扩张剂的使用,从而为白三烯在哮喘发病机制中的作用提供了进一步证据。