Muscle LIM Protein Force-Sensing Mediates Sarcomeric Biomechanical Signaling in Human Familial Hypertrophic Cardiomyopathy-Reference-Cited by-同舟云学术

Muscle LIM Protein Force-Sensing Mediates Sarcomeric Biomechanical Signaling in Human Familial Hypertrophic Cardiomyopathy

Published:2022-04-19 Issue:16 Volume:145 Page:1238-1253
ISSN:0009-7322
Container-title:Circulation
language:en
Short-container-title:Circulation

Author:

Riaz Muhammad¹²³⁴^ORCID,Park Jinkyu¹²³⁴,Sewanan Lorenzo R.⁵,Ren Yongming¹²³⁴,Schwan Jonas⁵,Das Subhash K.¹²³⁴,Pomianowski Pawel T.⁶,Huang Yan¹²³⁴,Ellis Matthew W.¹³⁴⁷,Luo Jiesi¹²³⁴^ORCID,Liu Juli⁸,Song Loujin⁹¹⁰,Chen I-Ping¹¹,Qiu Caihong⁴,Yazawa Masayuki⁹¹⁰,Tellides George¹²,Hwa John¹³^ORCID,Young Lawrence H.¹³⁷^ORCID,Yang Lei⁸,Marboe Charles C.¹¹,Jacoby Daniel L.¹^ORCID,Campbell Stuart G.⁵⁷^ORCID,Qyang Yibing¹²³⁴^ORCID

Affiliation:

1. Yale Cardiovascular Research Center, Section of Cardiovascular Medicine, Department of Internal Medicine (M.R., J.P., Y.R., S.K.D., Y.H., M.W.E., J. Luo, J.H., L.H.Y., D.L.J., Y.Q.), Yale University School of Medicine, New Haven, CT.

2. Department of Pathology (M.R., J.P., Y.R., S.K.D., Y.H., J. Luo, Y.Q.), Yale University School of Medicine, New Haven, CT.

3. Vascular Biology and Therapeutics Program (M.R., J.P., Y.R., S.K.D., Y.H., M.W.E., J. Luo, J.H., L.H.Y., Y.Q.), Yale University School of Medicine, New Haven, CT.

4. Yale Stem Cell Center, New Haven, CT (M.R., J.P., Y.R., S.K.D., Y.H., M.W.E., J. Luo, C.Q., Y.Q.).

5. Department of Biomedical Engineering (L.R.S., J.S., S.G.C.), Yale University, New Haven, CT.

6. Department of Genetics (P.T.P.), Yale University, New Haven, CT.

7. Department of Cellular and Molecular Physiology (M.W.E., L.H.Y., S.G.C.), Yale University, New Haven, CT.

8. Department of Pediatrics, Anatomy and Cell Biology, Indiana University, Indianapolis (J. Liu, L.Y.).

9. Department of Rehabilitation and Regenerative Medicine, Columbia Stem Cell Initiative (L.S., M.Y.), Columbia University, New York, NY.

10. Department of Molecular Pharmacology and Therapeutics (L.S., M.Y.), Columbia University, New York, NY.

11. Department of Pathology and Cell Biology (C.C.M.), Columbia University, New York, NY.

12. Department of Surgery (G.T.), Yale University, New Haven, CT.

Abstract

Background: Familial hypertrophic cardiomyopathy (HCM) is the most common inherited cardiac disease and is typically caused by mutations in genes encoding sarcomeric proteins that regulate cardiac contractility. HCM manifestations include left ventricular hypertrophy and heart failure, arrythmias, and sudden cardiac death. How dysregulated sarcomeric force production is sensed and leads to pathological remodeling remains poorly understood in HCM, thereby inhibiting the efficient development of new therapeutics. Methods: Our discovery was based on insights from a severe phenotype of an individual with HCM and a second genetic alteration in a sarcomeric mechanosensing protein. We derived cardiomyocytes from patient-specific induced pluripotent stem cells and developed robust engineered heart tissues by seeding induced pluripotent stem cell–derived cardiomyocytes into a laser-cut scaffold possessing native cardiac fiber alignment to study human cardiac mechanobiology at both the cellular and tissue levels. Coupled with computational modeling for muscle contraction and rescue of disease phenotype by gene editing and pharmacological interventions, we have identified a new mechanotransduction pathway in HCM, shown to be essential in modulating the phenotypic expression of HCM in 5 families bearing distinct sarcomeric mutations. Results: Enhanced actomyosin crossbridge formation caused by sarcomeric mutations in cardiac myosin heavy chain ( MYH7 ) led to increased force generation, which, when coupled with slower twitch relaxation, destabilized the MLP (muscle LIM protein) stretch-sensing complex at the Z-disc. Subsequent reduction in the sarcomeric muscle LIM protein level caused disinhibition of calcineurin–nuclear factor of activated T-cells signaling, which promoted cardiac hypertrophy. We demonstrate that the common muscle LIM protein–W4R variant is an important modifier, exacerbating the phenotypic expression of HCM, but alone may not be a disease-causing mutation. By mitigating enhanced actomyosin crossbridge formation through either genetic or pharmacological means, we alleviated stress at the Z-disc, preventing the development of hypertrophy associated with sarcomeric mutations. Conclusions: Our studies have uncovered a novel biomechanical mechanism through which dysregulated sarcomeric force production is sensed and leads to pathological signaling, remodeling, and hypertrophic responses. Together, these establish the foundation for developing innovative mechanism-based treatments for HCM that stabilize the Z-disc MLP-mechanosensory complex.

Publisher

Ovid Technologies (Wolters Kluwer Health)

Subject

Physiology (medical),Cardiology and Cardiovascular Medicine

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