对正常男性志愿者口服特异性血管紧张素II受体拮抗剂DuP 753。抑制对外源性血管紧张素I和II的升压反应。

Oral administration of DuP 753, a specific angiotensin II receptor antagonist, to normal male volunteers. Inhibition of pressor response to exogenous angiotensin I and II.

作者信息

Christen Y, Waeber B, Nussberger J, Porchet M, Borland R M, Lee R J, Maggon K, Shum L, Timmermans P B, Brunner H R

机构信息

Hypertension Division, University Hospital, Lausanne, Switzerland.

出版信息

Circulation. 1991 Apr;83(4):1333-42. doi: 10.1161/01.cir.83.4.1333.

DOI:10.1161/01.cir.83.4.1333

PMID:2013151

Abstract

BACKGROUND

The purpose of the present study was to assess the inhibitory effect of DuP 753, an orally active angiotensin II receptor antagonist, on the pressor action of exogenous angiotensin I and II in healthy male volunteers.

METHODS AND RESULTS

In the first study (single-dose study), eight volunteers were included in a 2-day protocol repeated four times at 1-week intervals. In each phase, a different dose of drug (2.5, 5, 10, 20, or 40 mg) or placebo was given. The peak systolic blood pressure response to a test-dose of angiotensin I was determined serially before and after oral administration of DuP 753 by continuously monitoring finger blood pressure using a photoplethysmographic method. DuP 753 reduced the systolic blood pressure response to angiotensin I in a dose-dependent fashion. Three, 6, and 13 hours after the 40-mg dose, blood pressure response decreased to 31 +/- 5%, 37 +/- 6%, and 45 +/- 3% of the control values (mean +/- SEM, n = 7), respectively. In the second study, 29 volunteers were treated for 8 days with either a placebo or DuP 753 (5, 10, 20, or 40 mg p.o. q.d.) and challenged on the first, fourth, and eighth days with bolus injections of angiotensin II. Again, the inhibitory effect on the systolic blood pressure response to angiotensin II was clearly dose dependent. Six hours after 40 mg DuP 753, the systolic blood pressure response to the test-dose of angiotensin II was reduced to 37 +/- 7%, 40 +/- 4%, and 38 +/- 6% of baseline values (mean +/- SEM, n = 6) on days 1, 4, and 8, respectively. With this latter dose, there was still a blocking effect detectable 24 hours after the drug. Similar to angiotensin converting enzyme and renin inhibitors, DuP 753 induced a dose-dependent increase in plasma renin that was more pronounced on the eighth than on the first day of drug administration. In these normal volunteers, no consistent clinically significant side effects were observed. There was no evidence for an agonist effect.

CONCLUSIONS

DuP 753 appears to be a well-tolerated, orally active, potent, and long-lasting antagonist of angiotensin II in men.

摘要

背景

本研究的目的是评估口服活性血管紧张素II受体拮抗剂DuP 753对健康男性志愿者中外源性血管紧张素I和II升压作用的抑制效果。

方法与结果

在第一项研究（单剂量研究）中，8名志愿者参与了一项为期2天的方案，该方案以1周的间隔重复进行4次。在每个阶段，给予不同剂量的药物（2.5、5、10、20或40毫克）或安慰剂。通过使用光电容积描记法连续监测手指血压，在口服DuP 753之前和之后依次测定对血管紧张素I试验剂量的收缩压峰值反应。DuP 753以剂量依赖性方式降低了对血管紧张素I的收缩压反应。在40毫克剂量后的3、6和13小时，血压反应分别降至对照值的31±5%、37±6%和45±3%（平均值±标准误，n = 7）。在第二项研究中，29名志愿者用安慰剂或DuP 753（5、10、20或40毫克口服，每日一次）治疗8天，并在第1、4和8天用血管紧张素II推注进行激发试验。同样，对血管紧张素II收缩压反应的抑制作用明显呈剂量依赖性。在40毫克DuP 753给药6小时后，在第1、4和8天，对血管紧张素II试验剂量的收缩压反应分别降至基线值的37±7%、40±4%和38±6%（平均值±标准误，n = 6）。使用后一剂量时，在药物给药24小时后仍可检测到阻断作用。与血管紧张素转换酶和肾素抑制剂类似，DuP 753诱导血浆肾素呈剂量依赖性增加，在给药的第8天比第1天更明显。在这些正常志愿者中，未观察到一致的具有临床意义的副作用。没有证据表明存在激动剂效应。