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. 2025 Jun 6;136(12):1564-1578.
doi: 10.1161/CIRCRESAHA.125.326154. Epub 2025 May 9.

Mitochondrial NNT Promotes Diastolic Dysfunction in Cardiometabolic HFpEF

Mark E Pepin  1   2   3   4   5   6 Philipp J M Konrad  1   2   7   3 Sumra Nazir  1   2   3 Farhad Bazgir  1   2   3 Christoph Maack  8   9 Alexander Nickel  8 Joshua M Gorman  4 Mathias Hohl  10 Friederike Schreiter  1   2   3 Matthias Dewenter  1   2   3   11 Adriano de Britto Chaves Filho  12 Almut Schulze  12 Anja Karlstaedt  13 Norbert Frey  14   7   3 Christine E Seidman  4 Jonathan G Seidman  4 Johannes Backs  1   14   2   3   11
Affiliations

Mitochondrial NNT Promotes Diastolic Dysfunction in Cardiometabolic HFpEF

Mark E Pepin et al. Circ Res. .

Abstract

Background: Clinical management of heart failure with preserved ejection fraction (HFpEF) is hindered by a lack of disease-modifying therapies capable of altering its distinct pathophysiology. Despite the widespread implementation of a 2-hit model of cardiometabolic HFpEF to inform precision therapy, which utilizes HFD+L-NAME (ad libitum high-fat diet and 0.5% N[ω]-nitro-L-arginine methyl ester), we observe that C57BL6/J mice exhibit less cardiac diastolic dysfunction in response to HFD+L-NAME.

Methods: Genetic strain-specific single-nucleus transcriptomic analysis identified disease-relevant genes that enrich oxidative metabolic pathways within cardiomyocytes. Because C57BL/6J mice are known to harbor a loss-of-function mutation affecting the inner mitochondrial membrane protein Nnt (nicotinamide nucleotide transhydrogenase), we established an isogenic model of Nnt loss-of-function to determine whether intact NNT is necessary for the pathological cardiac manifestations of HFD+L-NAME. Twelve-week-old mice cross-bred to isolate wild-type (Nnt+/+) or loss-of-function (Nnt-/-) Nnt in the C57BL/6N background were challenged with HFD+L-NAME for 9 weeks (N=6-10).

Results: Nnt+/+ mice exhibited impaired ventricular diastolic relaxation and pathological remodeling, as assessed via noninvasive echocardiographic quantification of early diastolic pulse-wave velocity (E) to mitral annular velocity (e') ratio (E/e') (42.8 versus 21.5, P=1.2×10-10), E/A (early-to-late mitral inflow velocity ratio) (2.3 versus 1.4, P=4.1×10-2), diastolic stiffness (0.09 versus 0.04 mm Hg/μL, P=5.1×10-3), and myocardial fibrosis (P=2.3×10-2). Liquid chromatography and mass spectroscopy exposed a 40.0% reduction in NAD+ (P=8.4×10-3) and a 38.8% reduction in the ratio of reduced-to-oxidized glutathione (GSH: GSSG, P=2.6×10-2) among Nnt+/+ mice after HFD+L-NAME feeding. Using single-nucleus ligand-receptor analysis, we implicate Fgf1 (fibroblast growth factor 1) as a putative NNT-dependent mediator of cardiomyocyte-to-fibroblast signaling in myocardial fibrosis.

Conclusions: Together, these findings underscore the pivotal role of mitochondrial dysfunction in HFpEF pathogenesis, implicating both NNT and Fgf1 as novel therapeutic targets.

Keywords: NG-nitroarginine methyl ester; fibrosis; genetic therapy; heart failure; oxidative stress.

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Conflict of interest statement

C. Maack has received speaking/advisory honoraria from AstraZeneca, Boehringer Ingelheim, Lilly, Novo Nordisk, and Bristol Myers Squibb. J. Backs, M. Dewenter, and N. Frey are founders of Revier Therapeutics (develops drugs for cardiometabolic care). The other authors report no conflicts.

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