新型血管紧张素II受体拮抗剂TCV 116的开放性临床研究。

Open clinical studies on a new angiotensin II receptor antagonist, TCV 116.

作者信息

Ogihara T, Arakawa K, Iimura O, Abe K, Saruta T, Ishii M, Hiwada K, Fujishima M, Fukiyama K

机构信息

Department of Geriatric Medicine, Osaka University Medical School, Japan.

出版信息

J Hypertens Suppl. 1994 Nov;12(9):S35-8.

PMID:7884583

Abstract

OBJECTIVES

The goals of these preliminary studies were to evaluate the effects of a new angiotensin II receptor antagonist, TCV 116, on the daytime blood pressure profile in hospital inpatients with essential hypertension, and to evaluate the clinical efficacy and safety of this agent in outpatients with essential hypertension.

SUBJECTS

In study 1, daytime blood pressure changes were studied in 28 inpatients with mild to moderate essential hypertension (systolic blood pressure > or = 150 mmHg, diastolic blood pressure > or = 90 mmHg). In study 2, 55 outpatients with essential hypertension (systolic blood pressure > or = 160 mmHg, diastolic blood pressure > or = 95 mmHg) were enrolled in a dose-finding study.

METHODS

In study 1, after a 1-week placebo run-in period, blood pressure and the pulse rate were measured every 2 h except at night. TCV 116 monotherapy was started at 1 mg/day and increased stepwise at 3- to 5-day intervals to 2, 4 and 8 mg/day until a predetermined reduction in blood pressure was achieved. The daytime profiles of blood pressure and the pulse rate were again monitored at the end of the treatment period. In study 2, after a 4-week placebo run-in period, TCV 116 alone was administered for 2 weeks at 1 mg/day. The dose was then increased to 2 mg/day and stepwise at 2-week intervals to 4 and 8 mg/day until a predetermined reduction in blood pressure was achieved. The total treatment period was 8-12 weeks.

RESULTS

In study 1, a sufficient reduction in blood pressure was achieved in 19 of 28 patients (68%), with blood pressure significantly reduced at all measurement points, compared with the placebo run-in period. No differences were seen in the pulse rate. The only adverse reaction reported was a rash in one patient. In study 2, a sufficient reduction in blood pressure was achieved in 42 out of 55 patients (76%). The cumulative efficacy rate increased dose-dependently (15% at 1 mg/day, 38% at 2 mg/day, 60% at 4 mg/day and 76% at 8 mg/day). No differences were seen in the pulse rate. Adverse reactions were reported in three out of 55 patients (5.5%). No dry cough was reported by any of the patients.

CONCLUSIONS

TCV 116, an angiotensin II receptor antagonist, has potential as an antihypertensive agent. A dose of 4-8 mg once per day appears to be appropriate for the treatment of patients with mild to moderate essential hypertension.

摘要

目的

这些初步研究的目标是评估新型血管紧张素II受体拮抗剂TCV 116对原发性高血压住院患者日间血压曲线的影响，并评估该药物在原发性高血压门诊患者中的临床疗效和安全性。

受试者

在研究1中，对28例轻度至中度原发性高血压患者（收缩压≥150 mmHg，舒张压≥90 mmHg）的日间血压变化进行了研究。在研究2中，55例原发性高血压门诊患者（收缩压≥160 mmHg，舒张压≥95 mmHg）被纳入剂量探索研究。

方法

在研究1中，经过1周的安慰剂导入期后，除夜间外每2小时测量一次血压和脉搏率。TCV 116单药治疗从1 mg/天开始，每隔3至5天逐步增加至2、4和8 mg/天，直至血压达到预定降幅。在治疗期结束时再次监测血压和脉搏率的日间曲线。在研究2中，经过4周的安慰剂导入期后，单独给予TCV 116，1 mg/天，持续2周。然后剂量增加至2 mg/天，每隔2周逐步增加至4和8 mg/天，直至血压达到预定降幅。总治疗期为8至12周。

结果

在研究1中，28例患者中有19例（68%）血压得到充分降低，与安慰剂导入期相比，所有测量点的血压均显著降低。脉搏率未见差异。报告的唯一不良反应是1例患者出现皮疹。在研究2中，55例患者中有42例（76%）血压得到充分降低。累积有效率呈剂量依赖性增加（1 mg/天时为15%，2 mg/天时为38%，4 mg/天时为60%，8 mg/天时为76%）。脉搏率未见差异。55例患者中有3例（5.5%）报告了不良反应。所有患者均未报告干咳。