坎地沙坦酯与氯沙坦的药代动力学-药效学相互作用

Azizi M, Chatellier G, Guyene T T, Ménard J

Broussais Hospital Clinical Investigation Center, INSERM, and Assistance Publique des Hôpitaux de Paris, France.

J Hypertens. 1999 Apr;17(4):561-8. doi: 10.1097/00004872-199917040-00015.

BACKGROUND

The variability of the blood pressure response to blockade of the angiotensin II type 1 receptor is influenced by renin status and pharmacokinetics and pharmacokinetic-pharmacodynamic interactions.

OBJECTIVE

To compare the pharmacokinetic-pharmacodynamic interactions of two doses of an ester prodrug of a noncompetitive angiotensin II type 1 receptor antagonist, candesartan cilexetil, at 8 and 16 mg, with those of the reference angiotenisn II type 1 receptor blocker, losartan, at the standard dose (50 mg), in a human model that controls renin status.

DESIGN AND METHODS

In a double-blind placebo-controlled crossover study, we compared the effects on renin and mean blood pressure over 24 h of single oral doses of candesartan cilexetil at 8 and 16 mg and losartan at 50 mg in 16 sodium-depleted normotensive subjects.

RESULTS

The area under the curve (0-24 h) for plasma active renin did not differ significantly between 8 mg candesartan cilexetil and 50 mg losartan, but was significantly higher for 16 than for 8 mg candesartan cilexetil or for 50 mg losartan. The area under the curve (0-24 h) for the fall in mean blood pressure with 16 mg candesartan cilexetil (-197 +/- 96 mmHg/h) was significantly greater than that for placebo (-112 +/- 81 mmHg/h; P< 0.05) but the difference was not statistically significant compared with either 8 mg candesartan cilexetil (-158 +/- 95 mmHg/h) or 50 mg losartan (-144 +/- 66 mmHg/h). The area under the curve (0-24 h) for the fall in mean blood pressure did not significantly differ between 8 mg candesartan cilexetil, 50 mg losartan and placebo. The area under the curve (0-24 h) for plasma active renin was significantly correlated to that for plasma levels of the active metabolite of losartan, EXP 3174 (r = 0.65, n = 16, P< 0.01). No such correlation was detected for each single dose of candesartan cilexetil but a dose-response relationship was present when both doses were combined.

CONCLUSIONS

The pharmacodynamic effects of a single oral dose of 16 mg candesartan cilexetil are greater than those of 50 mg losartan and 8 mg candesartan cilexetil. The variability in the pharmacokinetic-pharmacodynamic interaction is less pronounced for candesartan than for EXP 3174, which could result in reduced variability of the blood pressure effects in patients.

背景

血管紧张素II 1型受体阻断后血压反应的变异性受肾素状态、药代动力学以及药代动力学 - 药效学相互作用的影响。

目的

在一个控制肾素状态的人体模型中，比较两种剂量（8毫克和16毫克）的非竞争性血管紧张素II 1型受体拮抗剂坎地沙坦酯前药与标准剂量（50毫克）的参考血管紧张素II 1型受体阻滞剂氯沙坦的药代动力学 - 药效学相互作用。

设计与方法

在一项双盲安慰剂对照交叉研究中，我们比较了16名钠缺失的血压正常受试者单次口服8毫克和16毫克坎地沙坦酯前药以及50毫克氯沙坦后24小时内对肾素和平均血压的影响。

结果

8毫克坎地沙坦酯前药与50毫克氯沙坦相比，血浆活性肾素的曲线下面积（0 - 24小时）无显著差异，但16毫克坎地沙坦酯前药的该曲线下面积显著高于8毫克坎地沙坦酯前药或50毫克氯沙坦。16毫克坎地沙坦酯前药使平均血压下降的曲线下面积（0 - 24小时）（-197±96 mmHg/h）显著大于安慰剂组（-112±81 mmHg/h；P<0.05），但与8毫克坎地沙坦酯前药（-158±95 mmHg/h）或50毫克氯沙坦（-144±66 mmHg/h）相比，差异无统计学意义。8毫克坎地沙坦酯前药、50毫克氯沙坦和安慰剂使平均血压下降的曲线下面积（0 - 24小时）无显著差异。血浆活性肾素的曲线下面积（0 - 24小时）与氯沙坦活性代谢物EXP 3174的血浆水平曲线下面积显著相关（r = 0.65，n = 16，P<0.01）。对于每单剂量的坎地沙坦酯前药未检测到这种相关性，但当两种剂量合并时存在剂量 - 反应关系。