Ongtengco I, Morales D, Sanderson J, Lu Z-R, Beilin L J, Burke V, Puddey I B, Tanomsup S, Dayi H, Rahardjo P, Zambahari Dato R, Chen C-Y, Soenarta A A, Buranakitjaroen P, Tan C, Soon T K, Wu D-J
St Luke's Medical Center, Quezon City, Philippines.
J Hum Hypertens. 2002 Nov;16(11):805-13. doi: 10.1038/sj.jhh.1001485.
Suboptimal management of hypertension is often a result of poor patient compliance in the form of missed doses of their antihypertensive medication. This multicentre, randomised, double-blind, parallel-group trial was designed to compare the persistence of the antihypertensive efficacy of the amlodipine and nifedipine gastrointestinal therapeutic system (GITS) after two 'missed doses', and also to compare the drugs' overall efficacy and safety in Asian patients with mild-to-moderate essential hypertension. Following a 2-week placebo run-in period, 222 patients were randomised to receive either amlodipine (5 mg daily, increased after 6 weeks if necessary to 10 mg daily, n=109) or nifedipine GITS (30 mg daily, increased after 6 weeks if necessary to 60 mg daily; n=113) for 12 weeks. A placebo was then substituted for further 2 days with continuous ambulatory blood pressure (BP) monitoring. The increases in the last 9 h of mean ambulatory BP on day 2 after treatment withdrawal were significantly less with amlodipine than with nifedipine GITS: 4.4+/-7.0 vs 11.2+/-11.3 mmHg for systolic BP (P<or=0.0001) and 2.4+/-6.3 vs 6.0+/-6.0 mmHg for diastolic BP (P<or=0.0002). Significant differences between the two drugs in mean 24-h ambulatory BP levels were already evident on day 1 after withdrawal, even though there were no significant differences on the final day of treatment. No differences in safety parameters were observed, and neither drug caused any serious or severe treatment-related adverse events. In conclusion, amlodipine provides greater protection than nifedipine GITS against loss of BP control following missed doses.
高血压管理欠佳往往是患者未按规定服用抗高血压药物导致依从性差的结果。这项多中心、随机、双盲、平行组试验旨在比较氨氯地平和硝苯地平胃肠道治疗系统(GITS)在两次“漏服剂量”后抗高血压疗效的持续性,同时比较这两种药物在亚洲轻至中度原发性高血压患者中的总体疗效和安全性。在为期2周的安慰剂导入期后,222例患者被随机分为接受氨氯地平(每日5 mg,必要时6周后增至每日10 mg,n = 109)或硝苯地平GITS(每日30 mg,必要时6周后增至每日60 mg;n = 113)治疗12周。然后用安慰剂替代治疗2天,并进行动态血压监测。停药后第2天,氨氯地平组平均动态血压在最后9小时的升高显著低于硝苯地平GITS组:收缩压为4.4±7.0 vs 11.2±11.3 mmHg(P≤0.0001),舒张压为2.4±6.3 vs 6.0±6.0 mmHg(P≤0.0002)。停药后第1天,两种药物在24小时平均动态血压水平上的显著差异就已显现,尽管在治疗最后一天没有显著差异。未观察到安全性参数有差异,两种药物均未引起任何严重或重度治疗相关不良事件。总之,与硝苯地平GITS相比,氨氯地平在漏服剂量后对血压控制丧失的保护作用更强。
