2型糖尿病患者长效注射和口服胰高血糖素样肽1受体激动剂的心血管和肾脏预后和死亡率：随机试验的系统评价和荟萃分析

IF 16.6

Diabetes care Pub Date : 2025-05-01 DOI:10.2337/dc25-0241

Matthew M Y Lee, Naveed Sattar, Rodica Pop-Busui, John Deanfield, Scott S Emerson, Silvio E Inzucchi, Johannes F E Mann, Nikolaus Marx, Sharon L Mulvagh, Neil R Poulter, Sunil V Badve, Richard E Pratley, Vlado Perkovic, John B Buse, Darren K McGuire

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引用次数: 0

摘要

背景：胰高血糖素样肽1受体激动剂（GLP-1RA）可降低2型糖尿病（T2D）患者主要不良心血管事件（MACE）的发生率，尽管其益处是否延伸到皮下和口服制剂仍不清楚。目的：在这些荟萃分析中，包括来自Semaglutide cardiOvascular oUtcomes试验（SOUL）（口服Semaglutide）和用Semaglutide Once Weekly （FLOW）试验评估肾功能的新数据，我们检查了长效（定义为具有足以提供24小时活性的药代动力学）GLP-1RA在T2D中心血管（CV）和肾脏的益处和风险。数据来源：对PubMed进行了系统评价（至2025年2月7日）。研究选择：纳入≥500例T2D患者GLP-1RA的随机安慰剂对照CV和肾脏结局试验。数据提取：使用随机效应模型来估计MACE的风险比（HR）、其组成、全因死亡率、心力衰竭住院（HHF）、复合肾脏结局（肾衰竭[肾脏替代治疗或持续估计肾小球滤过率[eGFR]）。数据综合：在10项试验（n = 71,351）中，长效GLP-1RA使MACE的发病率降低14% (HR 0.86 [95% CI 0.81, 0.90]；I2 = 27.6%)， HHF下降14% (0.86 [0.79,0.93]；I2 = 2.1%)，肾脏综合预后降低17% (0.83 [0.75,0.92]；I2 = 20.4%)，全因死亡率降低12% (0.88 [0.82,0.93]；I2 = 17.5%)。所有MACE成分均一致降低14%。GLP-1RA给药途径（皮下给药与口服给药）无显著异质性。严重低血糖、视网膜病变或胰腺事件的风险没有增加。局限性：试验水平的荟萃分析排除了详细的亚组分析，并可能引入生态偏倚。结论：作为一个整体，长效GLP-1RA（包括注射和口服制剂）可降低T2D患者MACE、HHF和肾脏事件的发生率以及全因死亡率。

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Cardiovascular and Kidney Outcomes and Mortality With Long-Acting Injectable and Oral Glucagon-Like Peptide 1 Receptor Agonists in Individuals With Type 2 Diabetes: A Systematic Review and Meta-analysis of Randomized Trials.

Background: Glucagon-like peptide 1 receptor agonists (GLP-1RA) reduce the incidence of major adverse cardiovascular events (MACE) in type 2 diabetes (T2D), although whether benefits extend to both subcutaneous and oral formulations remains unclear.

Purpose: In these meta-analyses, including new data from the Semaglutide cardiOvascular oUtcomes triaL (SOUL) (oral semaglutide) and Evaluate Renal Function with Semaglutide Once Weekly (FLOW) trial, we examined cardiovascular (CV) and kidney benefits and risks of long-acting (defined as having pharmacokinetics sufficient to provide 24-h activity) GLP-1RA in T2D.

Data sources: A systematic review of PubMed was conducted (to 7 February 2025).

Study selection: Randomized placebo-controlled CV and kidney outcomes trials of GLP-1RA with ≥500 individuals with T2D were included.

Data extraction: A random-effects model was used to estimate hazard ratios (HRs) for MACE, its components, all-cause mortality, hospitalization for heart failure (HHF), a composite kidney outcome (kidney failure [kidney replacement therapy or persistent estimated glomerular filtration rate [eGFR] <15 mL/min/1.73 m2], sustained ≥50% eGFR decline or nearest equivalent, or kidney-related death), worsening kidney function, and safety outcomes.

Data synthesis: Across 10 trials (n = 71,351), long-acting GLP-1RA reduced incidence rate of MACE by 14% (HR 0.86 [95% CI 0.81, 0.90]; I2 = 27.6%), HHF by 14% (0.86 [0.79, 0.93]; I2 = 2.1%), and the composite kidney outcome by 17% (0.83 [0.75, 0.92]; I2 = 20.4%) and all-cause mortality by 12% (0.88 [0.82, 0.93]; I2 = 17.5%). A consistent 14% reduction was seen for all MACE components. There was no significant heterogeneity by GLP-1RA administration route (subcutaneous vs. oral). There were no increased risks of severe hypoglycemia, retinopathy, or pancreatic events.

Limitations: Trial-level meta-analyses preclude detailed subgroup analyses and may introduce ecological bias.

Conclusions: As a group, long-acting GLP-1RA, including both injectable and oral formulations, reduce incidence of MACE, HHF, and kidney events and all-cause mortality in T2D.

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来源期刊

Diabetes care

CiteScore

29.50

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0.00%

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