Reviewed clinical summary · Source-linked · Educational use only

Does Dapagliflozin Improve Coronary Blood Flow in Diabetes? DAPAHEART 4-Year Follow-up

Clinical Bottom Line

The 4-year DAPAHEART follow-up finds dapagliflozin raises coronary flow reserve by 34% and reduces epicardial fat, apparently independent of weight loss. PICO summary and commentary.

Summary: In the 4-year DAPAHEART follow-up in type 2 diabetes with stable coronary disease, dapagliflozin increased coronary flow reserve by 34.4% and reduced epicardial adipose tissue by about 29%, with the fat reduction appearing independent of weight loss.

PICO Summary

ElementDetail
PopulationPatients with type 2 diabetes and stable coronary artery disease; DAPAHEART pilot, single-centre, with PET/CT imaging.
InterventionDapagliflozin 10 mg; coronary flow reserve and epicardial fat measured at baseline, 4 weeks, and 4 years (placebo group later crossed to dapagliflozin).
ComparisonInitial placebo, then within-patient change over 4 years.
OutcomeCoronary flow reserve rose 34.4% at 4 years (2.15±0.19 to 2.85±0.26; p=0.001) with a 29.18% reduction in epicardial adipose thickness (p=0.03). BMI fell in all patients, but BMI and epicardial-fat changes were not correlated, suggesting a weight-independent effect. The crossover group showed similar changes after starting treatment.
RCT Cardiovasc Diabetol · 2025

DAPAHEART 4-Year Follow-up

Pilot RCT · type 2 diabetes + CAD · 4 years

Trial design
T2D + stable coronary disease Enrolled & assessed RANDOMISED 1:1 Dapagliflozin Dapagliflozin 10 mg n = 16 Placebo Placebo (then crossover) n = 15 Coronary flow reserve change at 4 years
Change from baseline — both arms
Coronary flow reserve Baseline 4 years +34.4% Dapagliflozin Placebo
CFR baseline
2.15
±0.19
CFR at 4 yr
2.85
±0.26
CFR increase
+34.4%
p=0.001
Epicardial fat
-29.2%
p=0.03
⬡ Bottom Line

Over 4 years, dapagliflozin raised coronary flow reserve by 34.4% and cut epicardial fat by about 29%, with the fat reduction uncorrelated with weight loss.

Expert Commentary

This is a mechanistically satisfying study that helps answer why SGLT2 inhibitors protect the heart, not merely that they do. Coronary flow reserve is a meaningful surrogate for microvascular health, and a 34% improvement sustained over four years is substantial, plausibly shifting patients from an abnormal to a more normal range, while the parallel fall in epicardial adipose tissue offers a coherent mechanism, less local inflammation around the coronary arteries. The observation that epicardial-fat reduction did not track with BMI change is the most interesting detail, hinting at a direct effect on this metabolically active depot rather than a simple consequence of weight loss. The honest constraints are important: this is a small pilot with imaging endpoints rather than clinical events, the placebo-then-crossover design weakens the comparator, and coronary flow reserve, however predictive, is not a heart attack avoided. Can I use this with my patients? Supportively. It strengthens the rationale I already follow for favouring SGLT2 inhibitors in diabetic patients with cardiovascular risk and for continuing them long-term, while I remain clear that the hard outcome trials, not this surrogate study, justify the indication.

References

Cinti F, Morciano C, Guarneri A, et al. Coronary flow reserve increase after 4-year dapagliflozin treatment in patients with type 2 diabetes: the DAPAHEART follow-up study. Cardiovasc Diabetol. 2025;24(1):351. doi:10.1186/s12933-025-02912-4

Educational use: Hormone Insight is intended for healthcare professionals and learners. Interpret each summary alongside the primary source, local guidance, and patient-specific clinical judgement.

Subscribe now

Welcome to Hormone Insight. Our mission is to support clinical decision-making with accessible, evidence-based insights from recent studies and trials.

© 2024-2026 Hormone Insight. All rights reserved.