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血浆肾素及口服活性肾素抑制剂阿利吉仑在临床高血压中的降压作用。

Plasma renin and the antihypertensive effect of the orally active renin inhibitor aliskiren in clinical hypertension.

作者信息

Nussberger J, Gradman A H, Schmieder R E, Lins R L, Chiang Y, Prescott M F

机构信息

Department of Internal Medicine, CHUV, Lausanne, Switzerland.

出版信息

Int J Clin Pract. 2007 Sep;61(9):1461-8. doi: 10.1111/j.1742-1241.2007.01473.x. Epub 2007 Jun 22.

DOI:10.1111/j.1742-1241.2007.01473.x
PMID:17590217
Abstract

BACKGROUND

Aliskiren is the first in a new class of orally effective renin inhibitors for the treatment of hypertension.

METHODS

In 569 patients with mild-to-moderate hypertension, blood pressure (BP), plasma renin activity (PRA) and plasma renin concentration (PRC) were measured before and after 8 weeks of double-blind treatment with once-daily oral doses of aliskiren (150, 300 or 600 mg), irbesartan 150 mg or placebo.

RESULTS

Aliskiren 150, 300 and 600 mg and irbesartan 150 mg significantly reduced mean cuff sitting systolic BP (SBP) from baseline (p < 0.001 vs. placebo). Aliskiren 150, 300 and 600 mg significantly reduced geometric mean PRA by 69%, 71% and 75% from baseline respectively (p < 0.05 vs. placebo). Irbesartan 150 mg significantly increased PRA by 109% (p < 0.05 vs. placebo). Aliskiren dose-dependently increased PRC from baseline by 157%, 246% and 497%, at 150, 300 and 600 mg respectively, compared with a 9% decrease with placebo (p < 0.05). PRC increased significantly more with aliskiren 300 and 600 mg compared with irbesartan 150 mg (105%; p < 0.05). Regression analysis showed no significant correlations between baseline PRA and changes in SBP in any of the treatment groups, but interestingly, the slopes of the regression lines between changes in SBP and log-transformed baseline PRA were +2.0 for placebo and -1.5, -1.8 and -2.3 for aliskiren 150, 300 and 600 mg respectively. The slope for irbesartan 150 mg (-1.4) was similar to that for aliskiren 150 mg.

CONCLUSIONS

Aliskiren reduces SBP and PRA and increases PRC dose-dependently. In contrast, irbesartan reduces SBP but increases both PRC and PRA. As PRA is a measurement of angiotensin I-generating capacity, PRA can be used for measuring the ability of an antihypertensive agent to prevent the generation or action of Ang II, either directly (renin inhibitors, beta-blockers, central alpha(2)-agonists) or indirectly (AT(1)-receptor blockers, ACE inhibitors).

摘要

背景

阿利吉仑是用于治疗高血压的新型口服有效肾素抑制剂中的首个药物。

方法

在569例轻至中度高血压患者中,于每日口服一次阿利吉仑(150、300或600毫克)、厄贝沙坦150毫克或安慰剂进行双盲治疗8周前后,测量血压(BP)、血浆肾素活性(PRA)和血浆肾素浓度(PRC)。

结果

阿利吉仑150、300和600毫克以及厄贝沙坦150毫克与基线相比均显著降低了平均袖带坐位收缩压(SBP)(与安慰剂相比,p < 0.001)。阿利吉仑150、300和600毫克分别使几何平均PRA较基线水平显著降低69%、71%和75%(与安慰剂相比,p < 0.05)。厄贝沙坦150毫克使PRA显著升高109%(与安慰剂相比,p < 0.05)。与安慰剂降低9%相比,阿利吉仑150、300和600毫克分别使PRC较基线水平剂量依赖性升高157%、246%和497%(p < 0.05)。与厄贝沙坦150毫克(升高105%;p < 0.05)相比,阿利吉仑300和600毫克使PRC升高更为显著。回归分析显示,在任何治疗组中,基线PRA与SBP变化之间均无显著相关性,但有趣的是,SBP变化与对数转换后的基线PRA之间的回归线斜率,安慰剂组为 +2.0,阿利吉仑150、300和600毫克组分别为 -1.5、-1.8和 -2.3。厄贝沙坦150毫克组的斜率(-1.4)与阿利吉仑150毫克组相似。

结论

阿利吉仑可降低SBP和PRA,并使PRC呈剂量依赖性升高。相比之下,厄贝沙坦可降低SBP,但会使PRC和PRA均升高。由于PRA是血管紧张素I生成能力的一种测量指标,PRA可用于衡量抗高血压药物直接(肾素抑制剂、β受体阻滞剂、中枢α₂激动剂)或间接(AT₁受体阻滞剂、ACE抑制剂)预防血管紧张素II生成或作用的能力。

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