塞来昔布对使用ACE抑制剂的高血压患者动态血压的影响

W. White, J. Kent, Addison A. Taylor, K. Verburg, J. Lefkowith, A. Whelton
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引用次数: 154

摘要

非选择性非甾体类抗炎药已被证明可以降低ACE抑制剂的降压效果,使收缩压(BP)平均升高5至10毫米汞柱。目前对广泛用于治疗关节炎的特异性环氧合酶-2 (COX-2)抑制剂知之甚少。本研究的目的是比较塞来昔布与安慰剂对ACE抑制剂治疗的高血压患者24小时血压水平的影响。这是一项随机、双盲、安慰剂对照、平行组临床试验,涉及178名患有原发性高血压的男性和女性(平均年龄53岁),接受赖诺普利单药治疗和控制(每天10 - 40毫克)。基线血压值通过24小时动态记录获得。患者接受塞来昔布200mg,每日两次(骨关节炎推荐剂量的两倍)(n=91)或安慰剂(n=87)治疗4周,并评估24小时血压、体重和临床实验室参数的变化。塞来昔布组24小时收缩压和舒张压较基线的平均变化为2.6/1.5±0.9/0.6 mm Hg,安慰剂组为1.0/0.3±1/0.6 mm Hg(收缩压P =0.34,舒张压P =0.45)。塞来昔布和安慰剂组24小时血压升高至少5、10、15或20毫米汞柱的患者比例也相似。两组患者的体重、血清肌酐或钾均未发生变化。因此,这些数据表明,大剂量塞来昔布对ACE抑制剂赖诺普利的降压作用没有显著影响。在ACE抑制剂治疗的患者中,安慰剂减去24小时血压(1.6/1.2 mm Hg)的变化小于非选择性非甾体类抗炎药的报道。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Effects of Celecoxib on Ambulatory Blood Pressure in Hypertensive Patients on ACE Inhibitors
Nonselective nonsteroidal anti-inflammatory agents have been shown to attenuate the antihypertensive efficacy of ACE inhibitors with average increases in systolic blood pressure (BP) of 5 to 10 mm Hg. Less is known about the specific cyclooxygenase-2 (COX-2) inhibitors now widely used for the treatment of arthritis. The objective of this study was to determine the effects of celecoxib compared with placebo on 24-hour BP levels in ACE inhibitor-treated patients with hypertension. This was a randomized, double-blind, placebo-controlled, parallel-group clinical trial involving 178 men and women (mean age, 53 years) with essential hypertension who were treated and controlled with lisinopril monotherapy (10 to 40 mg daily). Baseline BP values were obtained using 24-hour ambulatory recordings. Patients received either celecoxib, 200 mg twice daily (twice the recommended dose for osteoarthritis) (n=91), or placebo (n=87) for 4 weeks, and changes in the 24-hour BP, body weight, and clinical laboratory parameters were assessed. Mean changes from baseline in the 24-hour systolic and diastolic BP were 2.6/1.5±0.9/0.6 mm Hg on celecoxib versus 1.0/0.3±1/0.6 mm Hg on placebo (P =0.34 for systolic BP;P =0.45 for diastolic BP). The proportion of patients whose 24-hour BP increased by at least 5, 10, 15, or 20 mm Hg were also similar on celecoxib and placebo. No changes in body weight, serum creatinine, or potassium occurred in either group. Thus, these data demonstrate that high doses of celecoxib have no significant effect on the antihypertensive effect of the ACE inhibitor lisinopril. The placebo-subtracted changes observed in 24-hour BP (1.6/1.2 mm Hg) are less than what has been reported for nonselective nonsteroidal anti-inflammatory agents in ACE inhibitor-treated patients.
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