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Cardiovascular safety and glycemic control of glucagon-like peptide-1 receptor agonists for type 2 diabetes mellitus: a pairwise and network meta-analysis.

Diabetes Res Clin Pract · 2012

Last updated 2026-07-14

A review of 45 studies with 15,883 participants found no significant differences in cardiovascular safety between GLP-1 drugs, placebo, or other diabetes medications. For blood sugar control, GLP-1 drugs were more effective than placebo, but no single GLP-1 drug stood out as better than others overall. Liraglutide was the only GLP-1 drug that performed better than some other diabetes medications and exenatide in lowering blood sugar.

AI summary of the abstract below.

JournalDiabetes Res Clin Pract, 2012
Citations31
Relative citation ratio0.93
NIH percentile48
Molecules

Abstract

AIMS: Integrating evidence from all randomized controlled trials (RCTs) of glucagon-like peptide-1 receptor agonists (GLP-1s) to assess the safety of cardiovascular disease (CVD) and efficacy of glycemic control. METHODS: Besides performing pairwise meta-analysis, network meta-analysis of all RCTs was used to combine direct and indirect estimates of the effect of GLP-1 with placebo, active comparator drugs (ACD), or another GLP-1 agent with treatment duration ≥8 weeks in T2DM patients, 15,883 for CVD safety from 45 RCTs and 14,136 for glycemic control from 36 RCTs. RESULTS: For CVD safety, both of the results from pairwise and network meta-analysis failed to demonstrate significant difference between any two comparators. For glycemic control, the effect of any GLP-1 was better than placebo, but no difference was found between GLP-1s. We also found that liraglutide was the only GLP-1 drug shown to be more effective on improving glycemic control than ACD and exenatide. The results based on direct or indirect estimates were similar for two outcomes. CONCLUSION: Our network meta-analysis provides a complete picture of the associations between GLP-1s, ACD and placebo on CVD safety and glycemic control. The GLP-1s are promising candidates for the treatment of T2DM, but more long-term trials are needed to confirm potential CVD safety.

Verbatim abstract via PubMed 23020934 ↗