Chrysant S G, Cohen M
Oklahoma Cardiovascular and Hypertension Center, University of Oklahoma, Oklahoma City 73132-4904, USA.
J Clin Pharmacol. 1995 Mar;35(3):239-43. doi: 10.1002/j.1552-4604.1995.tb04053.x.
The safety and efficacy, as measured by peak/trough blood pressure reduction, of a new, once-daily, controlled-release formulation of isradipine (isradipine-CR, ICR) were evaluated in patients with mild to moderate essential hypertension during a nine-week trial. After a 3-week placebo washout period, patients with a sitting diastolic blood pressure between 100 and 114 mm Hg were randomized to either 1 of 4 ICR treatment groups or placebo. Of 402 randomized patients, 384 completed the study (placebo = 77, ICR-5 mg = 76, ICR 10 mg = 76, ICR-15 mg = 78, and ICR-20 mg = 77). Peak and trough post-dose blood pressure responses and heart rates were monitored for both the sitting and upright positions. Blood chemistries, urinalyses, complete blood counts, and electrocardiograms were done during the study. Both sitting and upright blood pressure decreased with the 5-(P < .05), 10-, 15-, and 20-mg (P < .001) once-daily ICR doses. The peak blood pressure reduction for all ICR doses occurred at 8 to 10 hours post-dose. Maximum peak/trough blood pressure response, achieved with the 10-mg dose, was similar with that of 15 and 20 mg of ICR. No serious clinical or metabolic side effect were noted, except ankle edema, which was dose dependent but did not require discontinuation of treatment.(ABSTRACT TRUNCATED AT 250 WORDS)
在一项为期9周的试验中,对一种新型的、每日一次的控释伊拉地平制剂(伊拉地平控释片,ICR)在轻至中度原发性高血压患者中的安全性和有效性(通过峰/谷血压降低来衡量)进行了评估。在为期3周的安慰剂洗脱期后,坐位舒张压在100至114 mmHg之间的患者被随机分配至4个ICR治疗组之一或安慰剂组。在402名随机分组的患者中,384名完成了研究(安慰剂组 = 77名,ICR-5 mg组 = 76名,ICR 10 mg组 = 76名,ICR-15 mg组 = 78名,ICR-20 mg组 = 77名)。监测了坐位和立位给药后的峰血压和谷血压反应以及心率。在研究期间进行了血液化学检查、尿液分析、全血细胞计数和心电图检查。每日一次的ICR剂量为5 mg(P < .05)、10 mg、15 mg和20 mg时,坐位和立位血压均下降(P < .001)。所有ICR剂量的峰血压降低均在给药后8至10小时出现。10 mg剂量达到的最大峰/谷血压反应与15 mg和20 mg的ICR相似。除踝部水肿外,未观察到严重的临床或代谢副作用,踝部水肿虽与剂量有关,但无需停药。(摘要截断于250字)
