系列:糖尿病药物的心血管结局试验。

IF 0.4 Q4 ENDOCRINOLOGY & METABOLISM British Journal of Diabetes Pub Date : 2022-12-21 DOI:10.15277/bjd.2022.387
M. Fisher
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引用次数: 0

摘要

LEADER是一项具有里程碑意义的心血管结局试验,使用GLP-1受体激动剂利拉鲁肽,该试验显示主要不良心血管事件(MACE,心血管死亡、非致死性心肌梗死和非致死性卒中的组合)的显著降低,主要原因是心血管死亡的减少,并伴随着全因死亡率的显著降低。不久之后,每周服用一次西马鲁肽的SUSTAIN-6试验显示MACE的非劣效性,MACE的象征性降低是由于非致命性卒中风险的降低。此后,又发表了6项使用GLP-1受体激动剂的心血管试验,在研究设计和结果上存在重大差异。已经进行了四次试验,每周一次配方。每周一次使用艾塞那肽的EXSCEL试验显示MACE非劣效性,但不是优势性,全因死亡率降低,这是一个探索性结果。阿比鲁肽的Harmony Outcomes试验显示,由于致死性或非致死性心肌梗死的减少,MACE显著降低。使用杜拉鲁肽的REWIND也显示出MACE的显著降低,这一次是由于中风的减少。使用efpeglenatide的amplude - o试验显示MACE显著降低,但作为次要终点,MACE的单个成分均未显著降低,与其他试验相比,心力衰竭事件也显著减少。第五项试验是口服西马鲁肽制剂的PIONEER 6试验,该试验显示MACE的非劣效性,但不是优势,心血管死亡和全因死亡率(次要结局)降低。最后,FREEDOM-CVO与皮下迷你泵艾塞那肽显示MACE和MACE合并住院治疗不稳定心绞痛的非劣效性。在一些试验中发现蛋白尿减少,但对eGFR或终末期肾病没有明确的影响。GLP-1受体激动剂心血管结局试验的荟萃分析显示,MACE、心血管死亡、致死性或非致死性卒中、致死性或非致死性心肌梗死和全因死亡率显著降低。目前尚不清楚为什么NICE关于成人T2DM管理的最新指南没有承认这些基于证据的心血管益处。
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Series: Cardiovascular outcome trials for diabetes drugs.
LEADER was a landmark cardiovascular outcome trial with the GLP-1 receptor agonist liraglutide, which demonstrated significant reductions in major adverse cardiovascular events (MACE, a composite of cardiovascular death, non-fatal myocardial infarction and non-fatal stroke), driven by a reduction in cardiovascular deaths and accompanied by a significant reduction in all-cause mortality. Shortly afterwards, the SUSTAIN-6 trial with once-weekly semaglutide demonstrated non-inferiority for MACE, with a nominal reduction in MACE that was driven by a reduction in the risk of non-fatal strokes. Since then, a further six cardiovascular trials have been published with GLP-1 receptor agonists, with major differences in study design and outcomes. Four trials have been performed with once-weekly formulations. The EXSCEL trial with once-weekly exenatide showed non-inferiority for MACE, but not superiority, with a reduction in all-cause mortality which was an exploratory outcome. The Harmony Outcomes trial with albiglutide demonstrated significant reductions in MACE, driven by reductions in fatal or non-fatal myocardial infarction. REWIND, with dulaglutide, also demonstrated significant reductions in MACE, this time driven by reductions in strokes. The AMPLITUDE-O trial with efpeglenatide showed significant reductions in MACE, but none of the individual components of MACE was significantly reduced as a secondary endpoint, and in contrast to other trials there was also a significant reduction in heart failure events. The fifth trial was the PIONEER 6 trial with the oral formulation of semaglutide, and this showed non-inferiority for MACE, but not superiority, with reductions in cardiovascular deaths and all-cause mortality which were secondary outcomes. Finally, FREEDOM-CVO with a subcutaneous mini-pump of exenatide showed non-inferiority for MACE and MACE plus hospitalisation for unstable angina. A reduction in albuminuria was seen in several of these trials, but there was no definite effect on eGFR or end-stage renal disease. Meta-analysis of the cardiovascular outcome trials with GLP-1 receptor agonists has demonstrated significant reductions in MACE, cardiovascular death, fatal or non-fatal stroke, fatal or non-fatal myocardial infarction, and all-cause mortality. It remains unclear why updated guidance from NICE on the management of T2DM in adults fails to acknowledge these evidence-based cardiovascular benefits.
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来源期刊
British Journal of Diabetes
British Journal of Diabetes ENDOCRINOLOGY & METABOLISM-
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16.70%
发文量
15
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