Rationale: Heart failure with preserved ejection fraction (HFpEF) is a mortal clinical syndrome without effective therapies. We recently demonstrated in mice that a combination of metabolic and hypertensive stress recapitulates key features of human HFpEF. Objective: Using this novel preclinical HFpEF model, we set out to define and manipulate metabolic dysregulations occurring in HFpEF myocardium. Methods and Results: We observed impairment in mitochondrial fatty acid oxidation associated with hyperacetylation of key enzymes in the pathway. Downregulation of sirtuin 3 and deficiency of NAD+secondary to an impaired NAD+salvage pathway contribute to this mitochondrial protein hyperacetylation. Impaired expression of genes involved in NAD+biosynthesis was confirmed in cardiac tissue from patients with HFpEF. Supplementing HFpEF mice with nicotinamide riboside or a direct activator of NAD+biosynthesis led to improvement in mitochondrial function and amelioration of the HFpEF phenotype. Conclusions: Collectively, these studies demonstrate that HFpEF is associated with myocardial mitochondrial dysfunction and unveil NAD+repletion as a promising therapeutic approach in the syndrome.
NAD+Repletion Reverses Heart Failure with Preserved Ejection Fraction / Tong, D.; Schiattarella, G. G.; Jiang, N.; Altamirano, F.; Szweda, P. A.; Elnwasany, A.; Lee, D. I.; Yoo, H.; Kass, D. A.; Szweda, L. I.; Lavandero, S.; Verdin, E.; Gillette, T. G.; Hill, J. A.. - In: CIRCULATION RESEARCH. - ISSN 0009-7330. - 128:11(2021), pp. 1629-1641. [10.1161/CIRCRESAHA.120.317046]
NAD+Repletion Reverses Heart Failure with Preserved Ejection Fraction
Schiattarella G. G.;Kass D. A.;
2021
Abstract
Rationale: Heart failure with preserved ejection fraction (HFpEF) is a mortal clinical syndrome without effective therapies. We recently demonstrated in mice that a combination of metabolic and hypertensive stress recapitulates key features of human HFpEF. Objective: Using this novel preclinical HFpEF model, we set out to define and manipulate metabolic dysregulations occurring in HFpEF myocardium. Methods and Results: We observed impairment in mitochondrial fatty acid oxidation associated with hyperacetylation of key enzymes in the pathway. Downregulation of sirtuin 3 and deficiency of NAD+secondary to an impaired NAD+salvage pathway contribute to this mitochondrial protein hyperacetylation. Impaired expression of genes involved in NAD+biosynthesis was confirmed in cardiac tissue from patients with HFpEF. Supplementing HFpEF mice with nicotinamide riboside or a direct activator of NAD+biosynthesis led to improvement in mitochondrial function and amelioration of the HFpEF phenotype. Conclusions: Collectively, these studies demonstrate that HFpEF is associated with myocardial mitochondrial dysfunction and unveil NAD+repletion as a promising therapeutic approach in the syndrome.I documenti in IRIS sono protetti da copyright e tutti i diritti sono riservati, salvo diversa indicazione.
