Department of Medicine, Division of Cardiology, University of Iceland, Reykjavik, Iceland.
J Renin Angiotensin Aldosterone Syst. 2009 Sep;10(3):157-67. doi: 10.1177/1470320309342407. Epub 2009 Jul 17.
This subgroup analysis assessed the effects of treatment based on the direct renin inhibitor, aliskiren, or the angiotensin-converting enzyme inhibitor, ramipril, on plasma renin activity (PRA), plasma renin concentration (PRC) and other biomarkers in a 26-week randomised, double-blind trial. Changes in PRA and PRC after stopping treatment were also assessed.
After placebo run-in, 842 patients (mean sitting diastolic blood pressure (BP) 95-109 mmHg) were randomised to aliskiren 150 mg or ramipril 5 mg. Dose titration and hydrochlorothiazide addition were allowed after Week 6 and 12, respectively, for inadequate BP control. Patients completing active treatment were re-randomised to current regimen or placebo during a 4-week posttreatment phase.
BP reductions were independent of baseline PRA at Week 12, were greater with aliskiren- than ramipril-based therapy at Week 26 (17.9/13.3 vs. 15.2/12.0 mmHg, p<0.05) and persisted for longer after stopping aliskiren. Aliskiren-based therapy reduced geometric mean PRA (-63%, p<0.05; n=103), while ramipril-based therapy increased PRA (+143%, p<0.05; n=100) at Week 26; PRC increased in both groups (aliskiren: +224% [n=33], ramipril: +145% [n=39], both p<0.05). Four weeks after stopping aliskiren-based therapy, PRA remained 52% below pre-treatment baseline; PRA returned to baseline 2 weeks after stopping ramipril-based therapy.
Aliskiren-based therapy produced sustained BP and PRA reductions over 26 weeks; ramipril-based therapy lowered BP and increased PRA. PRA reductions persisted 4 weeks after stopping aliskiren, suggesting an inhibitory effect beyond the elimination half-life of the drug.
本亚组分析评估了基于直接肾素抑制剂阿利西利或血管紧张素转换酶抑制剂雷米普利的治疗对血浆肾素活性(PRA)、血浆肾素浓度(PRC)和 26 周随机、双盲试验中其他生物标志物的影响。还评估了停止治疗后 PRA 和 PRC 的变化。
在安慰剂导入期后,842 名患者(平均坐位舒张压(BP)95-109mmHg)被随机分配至阿利西利 150mg 或雷米普利 5mg。分别在第 6 周和第 12 周后允许剂量滴定和添加氢氯噻嗪,以控制血压不足。完成积极治疗的患者在治疗后 4 周的治疗阶段被重新随机分配至当前方案或安慰剂。
血压降低与第 12 周的基线 PRA 无关,第 26 周时阿利西利治疗组的降低大于雷米普利治疗组(17.9/13.3 对 15.2/12.0mmHg,p<0.05),且在停止阿利西利后持续时间更长。阿利西利治疗组降低了几何均数 PRA(-63%,p<0.05;n=103),而雷米普利治疗组增加了 PRA(+143%,p<0.05;n=100),第 26 周;两组 PRC 均增加(阿利西利:+224%[n=33],雷米普利:+145%[n=39],均 p<0.05)。停止阿利西利治疗后 4 周,PRA 仍较治疗前基线低 52%;停止雷米普利治疗后 2 周,PRA 恢复至基线。
阿利西利治疗 26 周可持续降低血压和 PRA;雷米普利治疗可降低血压并增加 PRA。停止阿利西利后 4 周,PRA 持续下降,提示药物消除半衰期后仍存在抑制作用。
