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Adverse effects of incretin-based therapies on major cardiovascular and arrhythmia events: meta-analysis of randomized trials

机译:肠降血糖素疗法对主要心血管和心律失常事件的不良影响:随机试验的荟萃分析

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摘要

Recent cardiovascular outcome trials of incretin-based therapies (IBT) in type 2 diabetes have not demonstrated either benefit or harm in terms of major adverse cardiovascular events (MACE). Earlier meta-analyses showed conflicting results but were limited in methodology. We aimed to perform an updated meta-analysis of all available incretin therapies on the incidence of MACE plus arrhythmia and heart failure.MethodsWe identified studies published through November 2014 by searching electronic databases and reference lists. We included RCTs in which the intervention group received incretin-based therapies and the control group received placebo or standard treatment; enrolled >100 participants in each group; interventions lasted >24 weeks; and reported data on one or more primary major adverse cardiovascular events endpoints plus terms for arrhythmia and heart failure. We used the Peto method for each CV event for individual IBT treatment.ResultsIn this meta-analysis of 100 RCTs involving 54,758 incretin-based therapies users and 48,175 controls, exenatide was associated with increased risk of arrhythmia (OR 2.83; 95% CI, 1.06–7.57); saxagliptin was associated with an increased risk of heart failure (OR 1.23; 95% CI, 1.03–1.46), and sitagliptin was associated with a significantly decreased risk of all cause death compared to active controls (OR 0.39, 95% CI 0.18–0.82).ConclusionsIn type 2 diabetes, exenatide may increase the risk of arrhythmia, and sitagliptin may reduce the risk of all cause death; however, the subgroup of patients most likely to experience harm or benefit is unclear.
机译:最近关于2型糖尿病的肠降血糖素疗法(IBT)的心血管结局试验尚未显示出主要不良心血管事件(MACE)的益处或危害。较早的荟萃分析显示出矛盾的结果,但方法学上受到限制。我们旨在对MACE加心律失常和心力衰竭的发生率的所有可用降血糖素疗法进行最新的荟萃分析。方法我们通过搜索电子数据库和参考文献清单确定了截至2014年11月发表的研究。我们纳入了RCT,其中干预组接受基于肠降血糖素的疗法,对照组接受安慰剂或标准疗法。每组招募> 100名参与者;干预持续超过24周;并报告了有关一个或多个主要主要不良心血管事件终点的数据,以及心律失常和心力衰竭的相关术语。我们对每个IB治疗的CV事件使用Peto方法进行分析。结果在100项RCT的荟萃分析中,涉及54,758种基于降钙素的疗法使用者和48,175名对照,艾塞那肽与心律失常的风险增加相关(OR 2.83; 95%CI,1.06 –7.57);沙格列汀与心力衰竭的风险增加相关(OR 1.23; 95%CI,1.03-1.46),西格列汀与活动对照组相比,所有原因死亡的风险均显着降低(OR 0.39,95%CI 0.18-0.82)结论:在2型糖尿病中,艾塞那肽可能会增加心律不齐的风险,西他列汀可能会降低所有原因导致的死亡;然而,尚不清楚最有可能遭受伤害或受益的患者亚组。

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