Use of Sodium-Glucose Cotransporter 2 (SGLT2) Inhibitors in Heart Failure Without Diabetes
Jeilyn Jiron Vindas, Maynor Jose Lopez Mendoza, María Jennifer Valle Mena, Maria Antonieta Salazar Estrada, Asdrubal Ulloa, Nicolle Contreras Figueroa

TL;DR
SGLT2 inhibitors are now key heart failure treatments, working beyond diabetes to improve heart function and reduce hospitalizations.
Contribution
This paper highlights the non-glycemic cardioprotective mechanisms and broad clinical benefits of SGLT2 inhibitors in heart failure.
Findings
SGLT2 inhibitors improve mitochondrial efficiency and cellular energy balance in the heart.
They reduce oxidative stress, inflammation, and maladaptive remodeling in heart failure patients.
Large trials show reduced hospitalizations and improved outcomes across various heart failure types.
Abstract
Sodium-glucose cotransporter 2 (SGLT2) inhibitors have become foundational therapies in the management of heart failure, extending beyond their original indication as glucose-lowering agents. Experimental and clinical evidence indicates that their cardioprotective effects are largely independent of glycemic control and are mediated through integrated hemodynamic, metabolic, and anti-inflammatory mechanisms. At the myocardial level, SGLT2 inhibitors promote a shift in substrate utilization toward fatty acids and ketone bodies, improving mitochondrial efficiency and cellular energy balance. These effects are accompanied by reductions in oxidative stress, inflammation, and maladaptive remodeling, as well as favorable vascular and cardiorenal interactions. Large randomized controlled trials have consistently demonstrated significant reductions in heart failure hospitalization across…
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Taxonomy
TopicsDiabetes Treatment and Management · Pancreatic function and diabetes · Heart Failure Treatment and Management
