Myosin Sequestration Regulates Sarcomere Function, Cardiomyocyte Energetics, and Metabolism, Informing the Pathogenesis of Hypertrophic Cardiomyopathy-Reference-Cited by-同舟云学术

Myosin Sequestration Regulates Sarcomere Function, Cardiomyocyte Energetics, and Metabolism, Informing the Pathogenesis of Hypertrophic Cardiomyopathy

Published:2020-03-10 Issue:10 Volume:141 Page:828-842
ISSN:0009-7322
Container-title:Circulation
language:en
Short-container-title:Circulation

Author:

Toepfer Christopher N.¹²³,Garfinkel Amanda C.¹,Venturini Gabriela¹⁴,Wakimoto Hiroko¹,Repetti Giuliana¹,Alamo Lorenzo⁵,Sharma Arun¹,Agarwal Radhika¹,Ewoldt Jourdan F.⁶,Cloonan Paige⁶,Letendre Justin⁶,Lun Mingyue⁷,Olivotto Iacopo⁸,Colan Steve⁹,Ashley Euan¹⁰,Jacoby Daniel¹¹,Michels Michelle¹²,Redwood Charles S.²,Watkins Hugh C.²³,Day Sharlene M.¹³,Staples James F.¹⁴,Padrón Raúl⁵¹⁵,Chopra Anant⁶,Ho Carolyn Y.¹⁶,Chen Christopher S.⁶,Pereira Alexandre C.¹⁴,Seidman Jonathan G.¹,Seidman Christine E.¹¹⁶¹⁷

Affiliation:

1. Department of Genetics, Harvard Medical School, Boston, MA (C.N.T., A.C.G., G.V., H.W., G.R., A.S., R.A., A.C.P., J.G.S., C.E.S.).

2. Cardiovascular Medicine, Radcliffe Department of Medicine (C.N.T., C.S.R., H.C.W.), University of Oxford, UK.

3. Wellcome Centre for Human Genetics (C.N.T., H.C.W.), University of Oxford, UK.

4. Laboratory of Genetics and Molecular Cardiology, Heart Institute (InCor)-University of São Paulo Medical School, Brazil (G.V., A.C.P.).

5. Centro de Biología Estructural, Instituto Venezolano de Investigaciones Cientifìcas (IVIC), Caracas (L.A., R.P.).

6. Department of Biomedical Engineering, Boston University, MA (J.F.E., P.C., J.L., A.C., C.S.C.).

7. Department of Medicine, Division of Genetics (M.L.), Brigham and Women’s Hospital, Boston, MA.

8. Cardiomyopathy Unit and Genetic Unit, Careggi University Hospital, Florence, Italy (I.O.).

9. Department of Cardiology, Boston Children’s Hospital, MA (S.C.).

10. Center for Inherited Cardiovascular Disease, Stanford University, CA (E.A.).

11. Department of Internal Medicine, Section of Cardiovascular Diseases, Yale School of Medicine, New Haven, CT (D.J.).

12. Department of Cardiology, Thorax Center, Erasmus MC, Rotterdam, The Netherlands (M.M.).

13. Department of Internal Medicine, University of Michigan, Ann Arbor (S.M.D.).

14. Department of Biology, University of Western Ontario, London, Canada (J.F.S.).

15. Division of Cell Biology and Imaging, Department of Radiology, University of Massachusetts Medical School, Worcester (R.P.).

16. Cardiovascular Division (C.Y.H., C.E.S.), Brigham and Women’s Hospital, Boston, MA.

17. Howard Hughes Medical Institute, Chevy Chase, MD (C.E.S.).

Abstract

Background: Hypertrophic cardiomyopathy (HCM) is caused by pathogenic variants in sarcomere protein genes that evoke hypercontractility, poor relaxation, and increased energy consumption by the heart and increased patient risks for arrhythmias and heart failure. Recent studies show that pathogenic missense variants in myosin, the molecular motor of the sarcomere, are clustered in residues that participate in dynamic conformational states of sarcomere proteins. We hypothesized that these conformations are essential to adapt contractile output for energy conservation and that pathophysiology of HCM results from destabilization of these conformations. Methods: We assayed myosin ATP binding to define the proportion of myosins in the super relaxed state (SRX) conformation or the disordered relaxed state (DRX) conformation in healthy rodent and human hearts, at baseline and in response to reduced hemodynamic demands of hibernation or pathogenic HCM variants. To determine the relationships between myosin conformations, sarcomere function, and cell biology, we assessed contractility, relaxation, and cardiomyocyte morphology and metabolism, with and without an allosteric modulator of myosin ATPase activity. We then tested whether the positions of myosin variants of unknown clinical significance that were identified in patients with HCM, predicted functional consequences and associations with heart failure and arrhythmias. Results: Myosins undergo physiological shifts between the SRX conformation that maximizes energy conservation and the DRX conformation that enables cross-bridge formation with greater ATP consumption. Systemic hemodynamic requirements, pharmacological modulators of myosin, and pathogenic myosin missense mutations influenced the proportions of these conformations. Hibernation increased the proportion of myosins in the SRX conformation, whereas pathogenic variants destabilized these and increased the proportion of myosins in the DRX conformation, which enhanced cardiomyocyte contractility, but impaired relaxation and evoked hypertrophic remodeling with increased energetic stress. Using structural locations to stratify variants of unknown clinical significance, we showed that the variants that destabilized myosin conformations were associated with higher rates of heart failure and arrhythmias in patients with HCM. Conclusions: Myosin conformations establish work-energy equipoise that is essential for life-long cellular homeostasis and heart function. Destabilization of myosin energy-conserving states promotes contractile abnormalities, morphological and metabolic remodeling, and adverse clinical outcomes in patients with HCM. Therapeutic restabilization corrects cellular contractile and metabolic phenotypes and may limit these adverse clinical outcomes in patients with HCM.

Publisher

Ovid Technologies (Wolters Kluwer Health)

Subject

Physiology (medical),Cardiology and Cardiovascular Medicine

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