在健康正常受试者无限制钠摄入期间,血管紧张素受体阻滞剂对动态血浆肾素活性的影响。
Effects of angiotensin receptor blockers on ambulatory plasma Renin activity in healthy, normal subjects during unrestricted sodium intake.
作者信息
Jones Michael R, Sealey Jean E, Laragh John H
机构信息
Phase IV Research, Daiichi Sankyo, Inc., Parsippany, New Jersey 07054, USA.
出版信息
Am J Hypertens. 2007 Aug;20(8):907-16. doi: 10.1016/j.amjhyper.2007.04.009.
BACKGROUND
Plasma renin activity (PRA), measured under controlled conditions, is a marker of the degree and persistence of renin-angiotensin system blockade.
METHODS
Two similarly designed five-way crossover studies evaluated angiotensin II type 1 (AT1) receptor blockade-induced changes in PRA in quietly seated, ambulatory volunteers who were ingesting uncontrolled diets. At weekly intervals, PRA was measured during the 24 h after administration of placebo, olmesartan medoxomil (20 or 40 mg), or valsartan (80 or 160 mg) (Study CS866-445), or placebo, olmesartan medoxomil (40 mg), valsartan (160 or 320 mg), or irbesartan (300 mg) (Study CS866-448). The primary end point was change in PRA relative to placebo from predose to 24 h postdose (DeltaPRA24).
RESULTS
In the 20 subjects who completed each study, there was a direct relationship between baseline PRA and DeltaPRA24 for all doses. Subjects with low PRA (<0.65 ng/mL/h) exhibited very low absolute increases in PRA. The DeltaPRA(24) increased significantly with olmesartan medoxomil 20 mg (P<.01) and 40 mg (P<.001) and valsartan 160 mg (P<.05) but not with valsartan 80 mg. In the second study (in which baseline PRA was lower), DeltaPRA24 increased with olmesartan medoxomil 40 mg (P<.0001), valsartan 320 mg (P<.01), and irbesartan 300 mg (P<.01) but not with valsartan 160 mg. The DeltaPRA24 was greatest with olmesartan medoxomil 40 mg and was dose-related for olmesartan medoxomil but not for valsartan.
CONCLUSIONS
The greater DeltaPRA24 with olmesartan medoxomil 40 mg indicates a more prolonged AT1 receptor blockade than with valsartan 80, 160, or 320 mg or irbesartan 300 mg. A routine, clinic ambulatory PRA level can be used as a biochemical marker of the persistence and degree of AT1 receptor blockade in subjects without suppressed PRA levels.
背景
在可控条件下测量的血浆肾素活性(PRA)是肾素-血管紧张素系统阻断程度和持续性的标志物。
方法
两项设计相似的五交叉研究评估了在安静就坐、饮食不受控制的门诊志愿者中,1型血管紧张素II(AT1)受体阻断剂引起的PRA变化。每周一次,在给予安慰剂、奥美沙坦酯(20或40mg)或缬沙坦(80或160mg)后24小时内测量PRA(研究CS866-445),或在给予安慰剂、奥美沙坦酯(40mg)、缬沙坦(160或320mg)或厄贝沙坦(300mg)后24小时内测量PRA(研究CS866-448)。主要终点是从给药前到给药后24小时PRA相对于安慰剂的变化(DeltaPRA24)。
结果
在完成每项研究的20名受试者中,所有剂量的基线PRA与DeltaPRA24之间存在直接关系。PRA低(<0.65ng/mL/h)的受试者PRA的绝对增加非常低。DeltaPRA(24)在奥美沙坦酯20mg(P<0.01)和40mg(P<0.001)以及缬沙坦160mg(P<0.05)时显著增加,但在缬沙坦80mg时未增加。在第二项研究(其中基线PRA较低)中,DeltaPRA24在奥美沙坦酯40mg(P<0.0001)、缬沙坦320mg(P<0.01)和厄贝沙坦300mg(P<0.01)时增加,但在缬沙坦160mg时未增加。DeltaPRA24在奥美沙坦酯40mg时最大,且与奥美沙坦酯剂量相关,但与缬沙坦无关。
结论
奥美沙坦酯40mg时DeltaPRA24更大,表明其AT1受体阻断作用比缬沙坦80、160或320mg或厄贝沙坦300mg更持久。在PRA水平未受抑制的受试者中,常规门诊PRA水平可作为AT1受体阻断持续性和程度的生化标志物。
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