Altered Cardiac Energetics and Mitochondrial Dysfunction in Hypertrophic Cardiomyopathy

Sara Ranjbarvaziri; Kristina B Kooiker; Mathew Ellenberger; Giovanni Fajardo; Mingming Zhao; Alison Schroer Vander Roest; Rahel A Woldeyes; Tiffany T Koyano; Robyn Fong; Ning Ma; Lei Tian; Gavin M Traber; Frandics Chan; John Perrino; Sushma Reddy; Wah Chiu; Joseph C Wu; Joseph Y Woo; Kathleen M Ruppel; James A Spudich; Michael P Snyder; Kévin Contrepois; Daniel Bernstein

doi:10.1161/CIRCULATIONAHA.121.053575

Altered Cardiac Energetics and Mitochondrial Dysfunction in Hypertrophic Cardiomyopathy

Circulation. 2021 Nov 23;144(21):1714-1731. doi: 10.1161/CIRCULATIONAHA.121.053575. Epub 2021 Oct 21.

Authors

Sara Ranjbarvaziri^{1

2}, Kristina B Kooiker³, Mathew Ellenberger⁴, Giovanni Fajardo^{1

2}, Mingming Zhao^{1

2}, Alison Schroer Vander Roest^{1

2}, Rahel A Woldeyes⁵, Tiffany T Koyano⁶, Robyn Fong⁶, Ning Ma^{2

7}, Lei Tian^{2

7}, Gavin M Traber⁴, Frandics Chan⁸, John Perrino⁹, Sushma Reddy^{1

2}, Wah Chiu^{5

10}, Joseph C Wu^{2

7}, Joseph Y Woo⁶, Kathleen M Ruppel^{1

11}, James A Spudich, Michael P Snyder⁴, Kévin Contrepois⁴, Daniel Bernstein^{1

2}

Affiliations

¹ Department of Pediatrics (S.Ranjbarvaziri, G.F., M.Z., A.S.V.R., S.Reddy, K.M.R., D.B.), Stanford University School of Medicine, CA.
² Cardiovascular Research Institute (S.Ranjbarvaziri, G.F., M.Z., A.S.V.R., N.M., L.T., S.Reddy, J.C.W., D.B.), Stanford University School of Medicine, CA.
³ Department of Medicine, Division of Cardiology, University of Washington, Seattle (K.B.K.).
⁴ Department of Genetics (M.E., G.M.T., M.P.S., K.C.), Stanford University School of Medicine, CA.
⁵ Department of Bioengineering (R.A.W., W.C.), Stanford University, CA.
⁶ Department of Cardiothoracic Surgery (T.T.K., R.F., J.Y.W.), Stanford University, CA.
⁷ Department of Medicine, Division of Cardiology (N.M., L.T., J.C.W.), Stanford University, CA.
⁸ Department of Radiology (F.C.), Stanford University, CA.
⁹ Cell Sciences Imaging Facility (J.P.), Stanford University, CA.
¹⁰ Division of Cryo-Electron Microscopy and Bioimaging, SLAC National Accelerator Laboratory (W.C.), Stanford University, CA.
¹¹ Department of Biochemistry (K.M.R.), Stanford University School of Medicine, CA.

Abstract

Background: Hypertrophic cardiomyopathy (HCM) is a complex disease partly explained by the effects of individual gene variants on sarcomeric protein biomechanics. At the cellular level, HCM mutations most commonly enhance force production, leading to higher energy demands. Despite significant advances in elucidating sarcomeric structure-function relationships, there is still much to be learned about the mechanisms that link altered cardiac energetics to HCM phenotypes. In this work, we test the hypothesis that changes in cardiac energetics represent a common pathophysiologic pathway in HCM.

Methods: We performed a comprehensive multiomics profile of the molecular (transcripts, metabolites, and complex lipids), ultrastructural, and functional components of HCM energetics using myocardial samples from 27 HCM patients and 13 normal controls (donor hearts).

Results: Integrated omics analysis revealed alterations in a wide array of biochemical pathways with major dysregulation in fatty acid metabolism, reduction of acylcarnitines, and accumulation of free fatty acids. HCM hearts showed evidence of global energetic decompensation manifested by a decrease in high energy phosphate metabolites (ATP, ADP, and phosphocreatine) and a reduction in mitochondrial genes involved in creatine kinase and ATP synthesis. Accompanying these metabolic derangements, electron microscopy showed an increased fraction of severely damaged mitochondria with reduced cristae density, coinciding with reduced citrate synthase activity and mitochondrial oxidative respiration. These mitochondrial abnormalities were associated with elevated reactive oxygen species and reduced antioxidant defenses. However, despite significant mitochondrial injury, HCM hearts failed to upregulate mitophagic clearance.

Conclusions: Overall, our findings suggest that perturbed metabolic signaling and mitochondrial dysfunction are common pathogenic mechanisms in patients with HCM. These results highlight potential new drug targets for attenuation of the clinical disease through improving metabolic function and reducing mitochondrial injury.

Keywords: cardiomyopathy, hypertrophic; metabolism; mitochondria; mitophagy; reactive oxygen species.

Publication types

Research Support, N.I.H., Extramural
Research Support, Non-U.S. Gov't

MeSH terms

Adult
Aged
Cardiomyopathy, Hypertrophic / diagnosis
Cardiomyopathy, Hypertrophic / etiology*
Cardiomyopathy, Hypertrophic / metabolism*
Cardiomyopathy, Hypertrophic / therapy
Cell Respiration / genetics
Computational Biology / methods
Disease Management
Disease Susceptibility*
Energy Metabolism*
Female
Gene Expression Profiling
Heart Function Tests
Humans
Lipidomics
Male
Metabolome
Metabolomics / methods
Middle Aged
Mitochondria / genetics*
Mitochondria / metabolism*
Mitochondria / ultrastructure
Mutation
Oxidative Stress
Reactive Oxygen Species
Transcriptome

Substances

Reactive Oxygen Species

Abstract

Publication types

MeSH terms

Substances

Grants and funding