Omboni S, Zanchetti A
Istituto di Clinica Medical Generale e Terapia Medica, Ospedale Maggiore, Università di Milano, Italy.
J Hypertens. 1998 Dec;16(12 Pt 1):1831-8. doi: 10.1097/00004872-199816120-00017.
To evaluate the antihypertensive effect of lercanidipine once a day at three different doses (2.5, 5 and 10 mg) by clinic and ambulatory blood pressure.
After 3 weeks of a placebo run-in, 243 mild to moderate essential hypertensives (mean+/-SD age 51+/-8 years) were randomly allocated to lercanidipine at 2.5, 5 or 10 mg or a placebo for 4 weeks, in a double-blind parallel-group design. At the end of each period, supine clinic blood pressure (standard sphygmomanometry) and 24 h ambulatory blood pressure (Spacelabs 90207) were measured. The duration and homogeneity of the antihypertensive effect of the active drug compared with placebo over 24 h was evaluated by calculating the smoothness index, the ratio of the mean of the 24 hourly blood pressure changes to the corresponding SD. The higher the smoothness index, the greater and the smoother is the antihypertensive effect of a drug over the 24 h.
In 211 patients with valid clinic blood pressure data at the end of treatment, larger systolic/diastolic blood pressure reductions were found in the 5 mg (10+/-12/8+/-6 mmHg; P< 0.05 versus placebo, diastolic blood pressure only) and the 10 mg (12+/-11/9+/-7 mmHg; P < 0.05 versus placebo, both pressures) lercanidipine groups than in the placebo (5+/-11/4+/-8 mmHg) and 2.5 mg lercanidipine (7+/-12/6 +/-7 mmHg) groups. In 105 patients with complete 24 h ambulatory blood pressure recordings, there were significantly (P< 0.05 versus placebo) larger reductions in the 10 mg (9+/-7/7+/-5 mmHg) than the 2.5 mg (1+/-10/1+/-6 mmHg) and placebo (2+/-6/1+/-4 mmHg) groups. The reduction in 24 h blood pressure with 5 mg lercanidipine (6+/-7/4+/-5 mmHg) was significantly greater compared with placebo for diastolic pressure only, and when hourly average blood pressure changes were considered, this reduction did not extend to the final hours of the dosing interval. No significant changes in the clinic or 24 h heart rate were induced by placebo or lercanidipine. The smoothness index was significantly (P< 0.05) lower for 2.5 mg lercanidipine and placebo (0.2+/-0.5 and 0.3+/-0.7 for systolic and 0.1+/-0.4 and 0.2+/-0.7 for diastolic blood pressure) than for the 5 and 10 mg doses (0.7+/-1 and 1+/-0.7 for systolic and 0.7+/-1 and 1+/-0.9 for diastolic blood pressure).
At a dose of 10 mg, lercanidipine had a significant and durable antihypertensive effect over 24 h, but at 5 mg, the effect was less consistent and did not last 24 h. There was no clinically relevant reduction in clinic or ambulatory blood pressure with 2.5 mg lercanidipine, and the effect was superimposable on that of placebo.
通过诊所血压和动态血压评估不同剂量(2.5、5和10毫克)的乐卡地平每日一次的降压效果。
经过3周的安慰剂导入期后,243例轻度至中度原发性高血压患者(平均年龄51±8岁,标准差)被随机分配至2.5毫克、5毫克或10毫克乐卡地平组或安慰剂组,进行为期4周的双盲平行组设计研究。在每个阶段结束时,测量仰卧位诊所血压(标准血压计测量)和24小时动态血压(Spacelabs 90207)。通过计算平滑指数来评估活性药物与安慰剂相比在24小时内降压效果的持续时间和一致性,平滑指数为24小时每小时血压变化平均值与相应标准差的比值。平滑指数越高,药物在24小时内的降压效果越大且越平稳。
在治疗结束时具有有效诊所血压数据的211例患者中,5毫克(收缩压/舒张压降低10±12/8±6毫米汞柱;仅舒张压与安慰剂相比P<0.05)和10毫克(收缩压/舒张压降低12±11/9±7毫米汞柱;收缩压和舒张压与安慰剂相比P<0.05)乐卡地平组的收缩压/舒张压降低幅度大于安慰剂组(5±11/4±8毫米汞柱)和2.5毫克乐卡地平组(7±12/6±7毫米汞柱)。在105例有完整24小时动态血压记录的患者中,10毫克组(9±7/7±5毫米汞柱)的血压降低幅度显著大于2.5毫克组(1±10/1±6毫米汞柱)和安慰剂组(2±6/1±4毫米汞柱)(与安慰剂相比P<0.05)。5毫克乐卡地平组24小时血压降低幅度(6±7/4±5毫米汞柱)仅舒张压与安慰剂相比显著更大,且当考虑每小时平均血压变化时,这种降低在给药间隔的最后几小时并未持续。安慰剂或乐卡地平未引起诊所或24小时心率的显著变化。2.5毫克乐卡地平组和安慰剂组的平滑指数显著低于5毫克和10毫克剂量组(收缩压分别为0.2±0.5和0.3±0.7,舒张压分别为0.1±0.4和0.2±0.7;收缩压和舒张压5毫克和10毫克剂量组分别为0.7±1和1±0.7以及0.7±1和1±0.9)(P<0.05)。
10毫克剂量的乐卡地平在24小时内具有显著且持久的降压效果,但5毫克剂量时,效果不太稳定且不能持续24小时。2.5毫克乐卡地平在诊所或动态血压方面无临床相关的降低,其效果与安慰剂相当。
