Oklahoma Cardiovascular and Hypertension Center and University of Oklahoma School of Medicine, Oklahoma City, Oklahoma, USA.
Clin Drug Investig. 2010;30(7):473-82. doi: 10.2165/11536560-000000000-00000.
One of the reasons for suboptimal blood pressure (BP) control in patients with hypertension is poor adherence to treatment, which may be caused by treatment-emergent adverse events. Therefore, it is crucial for an antihypertensive agent to provide a high level of efficacy without compromising tolerability.
To evaluate the safety and tolerability of a titrate-to-goal, olmesartan medoxomil-based therapy in patients with stage 1 hypertension (seated systolic BP [SeSBP] of 140-159 mmHg or seated diastolic BP [SeDBP] of 90-99 mmHg).
This was a pre-specified analysis of data from a randomized, double-blind, placebo-controlled, multicentre (29 sites) clinical study conducted from January to October 2007 in the US. Male and female patients (n = 130) aged >or=18 years with stage 1 hypertension were included in the analysis. Patients were treated with either placebo or an olmesartan medoxomil-based titration regimen, which comprised treatment with olmesartan medoxomil plus hydrochlorothiazide (HCTZ) as required to achieve a target BP of <120/80 mmHg. The current analysis focused on the safety of olmesartan medoxomil in patients with stage 1 hypertension, particularly in terms of discontinuation rates and the incidence of dizziness and orthostatic hypotension. Safety and tolerability were assessed throughout the study. The primary efficacy outcome was the least-squares (LS) mean change from baseline in SeSBP after 12 weeks' double-blind treatment. Additional efficacy variables included LS mean change from baseline in SeDBP at 12 weeks and the proportions of patients achieving BP goals at study end and at each titration step.
In patients with stage 1 hypertension, the olmesartan medoxomil-based regimen was generally well tolerated at all titration steps, and discontinuation due to adverse events was similar between olmesartan medoxomil and placebo. Treatment-emergent adverse events occurred in 16.1% up to 27.6% of olmesartan medoxomil recipients and between 8.3% and 24.3% of placebo recipients, across treatment regimens; a slight increase in the incidence of treatment-emergent adverse events was observed with olmesartan medoxomil/HCTZ versus olmesartan medoxomil alone (<or=27.6% vs <or=19.3%). In addition, one or more drug-related events were reported in up to 10.3% of olmesartan medoxomil recipients and up to 5.7% of placebo recipients. Gastrointestinal disorders (<or=10.0%), nervous system disorders (<or=10.3%), and infections/infestations (<or=7.1%) were the most commonly reported treatment-emergent adverse events in the olmesartan medoxomil treatment group. The most common nervous system disorders in the olmesartan medoxomil treatment group were dizziness (<or=6.9%) and headache (<or=5.4%). Orthostatic hypotension was not reported. The LS mean differences between olmesartan medoxomil and placebo for change from baseline in SeSBP (-22.0 mmHg; 95% confidence interval [CI] -26.9, -17.3) and SeDBP (-12.2 mmHg; 95% CI -14.9, -9.4; both p < 0.0001) significantly favoured olmesartan medoxomil at week 12 with last observation carried forward. At study end, a BP goal of <140/90 mmHg was achieved by 81.0% of patients in the olmesartan medoxomil group versus 43.1% of patients in the placebo group (p < 0.0001).
Olmesartan medoxomil-based therapy was well tolerated in this study among patients with stage 1 hypertension and demonstrated a placebo-like safety and tolerability profile. This regimen was also effective in terms of BP lowering and enabling patients to achieve BP goals without an adverse effect on tolerability.
高血压患者血压控制不理想的原因之一是治疗依从性差,这可能是由治疗中出现的不良反应引起的。因此,降压药物的疗效要高,同时又要保证耐受性良好。
评估依那普利为基础的个体化降压治疗方案治疗 1 期高血压(坐位收缩压[SeSBP]为 140-159mmHg 或坐位舒张压[SeDBP]为 90-99mmHg)的安全性和耐受性。
这是一项在美国 29 个中心(2007 年 1 月至 10 月)进行的随机、双盲、安慰剂对照、多中心临床研究的预设分析。纳入的分析对象为年龄≥18 岁的 1 期高血压男性和女性患者(n=130)。患者接受安慰剂或依那普利为基础的滴定方案治疗,根据需要联合应用奥美沙坦酯氢氯噻嗪,以达到<120/80mmHg 的目标血压。当前分析主要关注奥美沙坦酯在 1 期高血压患者中的安全性,特别是停药率以及头晕和体位性低血压的发生率。在整个研究过程中评估安全性和耐受性。主要疗效指标是 12 周双盲治疗后 SeSBP 的最小二乘(LS)均数变化。其他疗效变量包括 12 周时 SeDBP 的 LS 均数变化以及治疗结束和每个滴定步骤时达到血压目标的患者比例。
在 1 期高血压患者中,奥美沙坦酯基础方案在所有滴定阶段均具有良好的耐受性,奥美沙坦酯和安慰剂组因不良事件导致停药的比例相似。奥美沙坦酯组和安慰剂组分别有 16.1%至 27.6%和 8.3%至 24.3%的患者出现治疗中出现的不良事件,在奥美沙坦酯/氢氯噻嗪治疗组中,治疗中出现的不良事件发生率略有增加(<或=27.6% vs <或=19.3%)。此外,奥美沙坦酯组和安慰剂组分别有 10.3%和 5.7%的患者报告有 1 种或多种与药物相关的事件。最常见的治疗中出现的不良事件是胃肠道疾病(<或=10.0%)、神经系统疾病(<或=10.3%)和感染/寄生虫病(<或=7.1%)。奥美沙坦酯治疗组最常见的神经系统疾病是头晕(<或=6.9%)和头痛(<或=5.4%)。未报告体位性低血压。奥美沙坦酯组和安慰剂组在 SeSBP(-22.0mmHg;95%置信区间[CI] -26.9,-17.3)和 SeDBP(-12.2mmHg;95%CI -14.9,-9.4;均 p<0.0001)的最小二乘(LS)均值差异均有利于奥美沙坦酯,在第 12 周时进行最后一次观测结转。在研究结束时,奥美沙坦酯组有 81.0%的患者血压目标<140/90mmHg,而安慰剂组有 43.1%的患者血压目标<140/90mmHg(p<0.0001)。
在这项 1 期高血压患者的研究中,奥美沙坦酯为基础的治疗方案具有良好的耐受性,表现出与安慰剂相似的安全性和耐受性特征。该方案在降低血压和使患者达到血压目标方面也很有效,同时不影响耐受性。
