Cardiovascular outcomes in patients treated with sodium-glucose transport protein 2 inhibitors, a network meta-analysis of randomized trials

Dániel Tornyos; Maximilian Meuer; Réka Lukács; Oumaima El Alaoui El Abdallaoui; Péter Kupó; Réka Faludi; András Komócsi

doi:10.3389/fcvm.2022.1041200

Cardiovascular outcomes in patients treated with sodium-glucose transport protein 2 inhibitors, a network meta-analysis of randomized trials

Front Cardiovasc Med. 2022 Dec 5:9:1041200. doi: 10.3389/fcvm.2022.1041200. eCollection 2022.

Authors

Dániel Tornyos¹, Maximilian Meuer¹, Réka Lukács¹, Oumaima El Alaoui El Abdallaoui¹, Péter Kupó¹, Réka Faludi¹, András Komócsi¹

Affiliation

¹ Heart Institute, Medical School, University of Pécs, Pécs, Hungary.

Abstract

Background: Gliflozins altering the sodium-glucose transport protein 2 (SGLT2) in the nephron, represent alone or in combination a promising treatment option for patients with type II diabetes mellitus. In addition to glucose control, these drugs provide benefits including reduced risk of long-term cardiovascular (CV) and renal complications. Several trials evaluated gliflozins in patients with various degrees of cardiac dysfunction with heterogeneous results.

Objectives: We aimed to perform a comprehensive analysis of the effect of gliflozins on CV outcomes.

Methods: Systematic searches of electronic databases were conducted until September 2022. Multiple treatment network meta-analysis was performed in R. Random-effects model was used to combine risk estimates across trials calculating risk ratio (RR) with 95% confidence intervals as summary statistics. The primary endpoint of interest was the rate of heart failure-related hospitalization (HHF) and the composite of HHF with CV mortality (HHF + CVD). Secondary outcomes included major adverse cardiac events (MACE), CV- and overall mortality, myocardial infarction (MI), and stroke.

Results: Twenty-nine studies randomizing 88,418 patients were identified. Gliflozins reduced the risk of HHF (RR: 0.72 [0.69; 0.76]) and HHF + CVD (RR: 0.78 [0.75; 0.82]). The risk of MACE and its component also improved significantly except for stroke. The network analyses did not explore major differences among the individual substances. The only exception was sotagliflozin which appeared to be more effective regarding HHF + CVD, stroke, and MI compared to ertugliflozin, in HHF + CVD and stroke compared to dapagliflozin, and in stroke endpoint compared to empagliflozin.

Conclusion: Our meta-analysis supports a group effect of gliflozins beneficial in a wide spectrum of patients with a risk of heart failure (HF) development. In addition to the improvement of HF-related outcomes, the risk of major adverse events is also reduced with SGLT2 inhibition.

Systematic review registration: [www.ClinicalTrials.gov], identifier [CRD42022358078].

Keywords: cardiovascular event; heart failure; major adverse cardiac events (MACE); mortality; network meta-analysis; sodium glucose co-transport-2 (SGLT2) inhibitors.

Publication types

Systematic Review