Wiysonge Charles Shey, Bradley Hazel A, Volmink Jimmy, Mayosi Bongani M, Mbewu Anthony, Opie Lionel H
Institute of Infectious Disease and Molecular Medicine & Division of Medical Microbiology, University of Cape Town, Anzio Road, Observatory, South Africa, 7925.
Cochrane Database Syst Rev. 2012 Aug 15(8):CD002003. doi: 10.1002/14651858.CD002003.pub3.
This review is an update of the Cochrane Review published in 2007, which assessed the role of beta-blockade as first-line therapy for hypertension.
To quantify the effectiveness and safety of beta-blockers on morbidity and mortality endpoints in adults with hypertension.
In December 2011 we searched the Cochrane Central Register of Controlled Trials, Medline, Embase, and reference lists of previous reviews; for eligible studies published since the previous search we conducted in May 2006.
Randomised controlled trials (RCTs) of at least one year duration, which assessed the effects of beta-blockers compared to placebo or other drugs, as first-line therapy for hypertension, on mortality and morbidity in adults.
We selected studies and extracted data in duplicate. We expressed study results as risk ratios (RR) with 95% confidence intervals (CI) and combined them using the fixed-effects or random-effects method, as appropriate.
We included 13 RCTs which compared beta-blockers to placebo (4 trials, N=23,613), diuretics (5 trials, N=18,241), calcium-channel blockers (CCBs: 4 trials, N=44,825), and renin-angiotensin system (RAS) inhibitors (3 trials, N=10,828). Three-quarters of the 40,245 participants on beta-blockers used atenolol. Most studies had a high risk of bias; resulting from various limitations in study design, conduct, and data analysis.Total mortality was not significantly different between beta-blockers and placebo (RR 0.99, 95%CI 0.88 to 1.11; I(2)=0%), diuretics or RAS inhibitors, but was higher for beta-blockers compared to CCBs (RR 1.07, 95%CI 1.00 to 1.14; I(2)=2%). Total cardiovascular disease (CVD) was lower for beta-blockers compared to placebo (RR 0.88, 95%CI 0.79 to 0.97; I(2)=21%). This is primarily a reflection of the significant decrease in stroke (RR 0.80, 95%CI 0.66 to 0.96; I(2)=0%), since there was no significant difference in coronary heart disease (CHD) between beta-blockers and placebo. There was no significant difference in withdrawals from assigned treatment due to adverse events between beta-blockers and placebo (RR 1.12, 95%CI 0.82 to 1.54; I(2)=66%).The effect of beta-blockers on CVD was significantly worse than that of CCBs (RR 1.18, 95%CI 1.08-1.29; I(2)=0%), but was not different from that of diuretics or RAS inhibitors. In addition, there was an increase in stroke in beta-blockers compared to CCBs (RR 1.24, 95%CI 1.11-1.40; I(2)=0%) and RAS inhibitors (RR 1.30, 95%CI 1.11 to 1.53; I(2)=29%). However, CHD was not significantly different between beta-blockers and diuretics, CCBs or RAS inhibitors. Participants on beta-blockers were more likely to discontinue treatment due to adverse events than those on RAS inhibitors (RR 1.41, 95% CI 1.29 to 1.54; I(2)=12%), but there was no significant difference with diuretics or CCBs.
AUTHORS' CONCLUSIONS: Initiating treatment of hypertension with beta-blockers leads to modest reductions in cardiovascular disease and no significant effects on mortality. These effects of beta-blockers are inferior to those of other antihypertensive drugs. The GRADE quality of this evidence is low, implying that the true effect of beta-blockers may be substantially different from the estimate of effects found in this review. Further research should be of high quality and should explore whether there are differences between different sub-types of beta-blockers or whether beta-blockers have differential effects on younger and elderly patients.
本综述是2007年发表的Cochrane综述的更新版,该综述评估了β受体阻滞剂作为高血压一线治疗的作用。
量化β受体阻滞剂对高血压成年患者发病和死亡终点的有效性和安全性。
2011年12月,我们检索了Cochrane对照试验中央注册库、Medline、Embase以及以往综述的参考文献列表;对于自2006年5月上次检索以来发表的符合条件的研究进行检索。
至少为期一年的随机对照试验(RCT),该试验评估了β受体阻滞剂与安慰剂或其他药物相比,作为高血压一线治疗对成年人死亡率和发病率的影响。
我们选择研究并进行重复数据提取。我们将研究结果表示为具有95%置信区间(CI)的风险比(RR),并根据情况使用固定效应或随机效应方法进行合并。
我们纳入了13项RCT,这些试验将β受体阻滞剂与安慰剂(4项试验,N = 23,613)、利尿剂(5项试验,N = 18,241)、钙通道阻滞剂(CCB:4项试验,N = 44,825)以及肾素 - 血管紧张素系统(RAS)抑制剂(3项试验,N = 10,828)进行了比较。使用β受体阻滞剂的40,245名参与者中有四分之三使用阿替洛尔。大多数研究存在较高的偏倚风险;这是由研究设计、实施和数据分析中的各种局限性导致的。β受体阻滞剂与安慰剂(RR 0.99,95%CI 0.88至1.11;I² = 0%)、利尿剂或RAS抑制剂相比,总死亡率无显著差异,但与CCB相比,β受体阻滞剂的总死亡率更高(RR 1.07,95%CI 1.00至1.14;I² = 2%)。与安慰剂相比,β受体阻滞剂的总心血管疾病(CVD)发生率较低(RR 0.88,95%CI 0.79至0.97;I² = 21%)。这主要反映在中风显著减少(RR 0.80,95%CI 0.66至0.96;I² = 0%),因为β受体阻滞剂与安慰剂之间的冠心病(CHD)无显著差异。β受体阻滞剂与安慰剂因不良事件退出指定治疗的情况无显著差异(RR 1.12,95%CI 0.82至1.54;I² = 66%)。β受体阻滞剂对CVD的影响明显比CCB差(RR 1.18,95%CI 1.08 - 1.29;I² = 0%),但与利尿剂或RAS抑制剂无差异。此外,与CCB(RR 1.24,95%CI 1.11 - 1.40;I² = 0%)和RAS抑制剂(RR 1.30,95%CI 1.11至1.53;I² = 29%)相比,β受体阻滞剂组中风增加。然而,β受体阻滞剂与利尿剂、CCB或RAS抑制剂之间的CHD无显著差异。使用β受体阻滞剂的参与者因不良事件停药的可能性比使用RAS抑制剂的参与者更高(RR 1.41,95%CI 1.29至1.54;I² = 12%),但与利尿剂或CCB无显著差异。
用β受体阻滞剂启动高血压治疗可适度降低心血管疾病风险,但对死亡率无显著影响。这些β受体阻滞剂的效果不如其他抗高血压药物。该证据的GRADE质量较低,这意味着β受体阻滞剂的真实效果可能与本综述中发现的效果估计值有很大差异。进一步的研究应该是高质量的,并且应该探索不同亚型的β受体阻滞剂之间是否存在差异,或者β受体阻滞剂对年轻和老年患者是否有不同的影响。
