Diabetes and Excess Aldosterone Promote Heart Failure With Preserved Ejection Fraction.
Bence HegyiJuliana Mira HernandezChristopher Y KoJunyoung HongErin Y ShenEmily R SpencerDaria SmoliarchukManuel F NavedoDonald M BersJulie BossuytPublished in: Journal of the American Heart Association (2022)
Background The pathobiology of heart failure with preserved ejection fraction (HFpEF) is still poorly understood, and effective therapies remain limited. Diabetes and mineralocorticoid excess are common and important pathophysiological factors that may synergistically promote HFpEF. The authors aimed to develop a novel animal model of HFpEF that recapitulates key aspects of the complex human phenotype with multiorgan impairments. Methods and Results The authors created a novel HFpEF model combining leptin receptor-deficient db/db mice with a 4-week period of aldosterone infusion. The HFpEF phenotype was assessed using morphometry, echocardiography, Ca 2+ handling, and electrophysiology. The sodium-glucose cotransporter-2 inhibitor empagliflozin was then tested for reversing the arrhythmogenic cardiomyocyte phenotype. Continuous aldosterone infusion for 4 weeks in db/db mice induced marked diastolic dysfunction with preserved ejection fraction, cardiac hypertrophy, high levels of B-type natriuretic peptide, and significant extracardiac comorbidities (including severe obesity, diabetes with marked hyperglycemia, pulmonary edema, and vascular dysfunction). Aldosterone or db/db alone induced only a mild diastolic dysfunction without congestion. At the cellular level, cardiomyocyte hypertrophy, prolonged Ca 2+ transient decay, and arrhythmogenic action potential remodeling (prolongation, increased short-term variability, delayed afterdepolarizations), and enhanced late Na + current were observed in aldosterone-treated db/db mice. All of these arrhythmogenic changes were reversed by empagliflozin pretreatment of HFpEF cardiomyocytes. Conclusions The authors conclude that the db/db +aldosterone model may represent a distinct clinical subgroup of HFpEF that has marked hyperglycemia, obesity, and increased arrhythmia risk. This novel HFpEF model can be useful in future therapeutic testing and should provide unique opportunities to better understand disease pathobiology.
Keyphrases
- angiotensin ii
- type diabetes
- ejection fraction
- high fat diet induced
- high glucose
- cardiovascular disease
- oxidative stress
- endothelial cells
- diabetic rats
- insulin resistance
- left ventricular
- blood pressure
- metabolic syndrome
- pulmonary hypertension
- computed tomography
- randomized controlled trial
- body mass index
- climate change
- adipose tissue
- physical activity
- aortic stenosis
- blood brain barrier
- clinical trial
- protein kinase
- current status
- gestational age
- induced pluripotent stem cells
- double blind
- study protocol