Abstract

The mechanism whereby cardiomyocytes precisely regulate the assembly of their actin-containing thin filaments at the level of single molecules is still largely unknown. We have discovered that Leiomodin 2 (Lmod2), a striated muscle specific actin-binding protein, functions as the first described actin filament pointed- end elongation factor in mammals. Little is known, however, regarding the function of Lmod2 in the heart. Preliminary analysis of our unique Lmod2 knockout (KO) mice reveal that they die ~3 weeks following birth, with hearts displaying severe contractile dysfunction and ventricular chamber enlargement, consistent with dilated cardiomyopathy (DCM). Strikingly, Lmod2 KO hearts have shorter thin filaments. When we analyzed human heart samples with DCM and hearts from multiple mouse models of DCM we discovered that they too have shorter thin filaments. Remarkably, when DCM was rescued in the hearts of a well-studied mouse model of DCM (muscle LIM protein (MLP) knockout mice), proper thin filament lengths were restored. We hypothesize that thin filament length changes are a general mechanism of the complex remodeling that occurs in DCM. The long-term goal of the proposed work is to discover common pathophysiologies of dilated hearts that can be used as therapeutic targets for the treatment of DCM. The immediate goals of this proposal are to determine mechanisms by which actin-thin filament architecture is regulated in cardiac muscle, the role Lmod2 plays in this regulation, and how defects in this regulation contribute to DCM. Using novel transgenic mice (with either abnormally long or short thin filaments), human muscle samples and primary cardiomyocytes, we will take a multidisciplinary approach to accomplish three Specific Aims focused on determining: 1) the effect loss of Lmod2 has on cardiac development and function; 2) the mechanism by which Lmod2 functions to elongate thin filaments; and 3) the role thin filament length dysregulation plays in cardiomyopathies, and whether heart function and remodeling can be rescued if thin filament regulation is restored in a dilated heart in vivo. We predict that completion of this project will result in the discovery of one critical general mechanism and a novel structural biomarker (i.e., thin filament length dysregulation) of the complex remodeling seen in DCM. These discoveries will potentially facilitate early detection of DCM and lead to new therapeutic options.

Public Health Relevance

The mechanisms regulating actin filament dynamics are critical for heart muscle development, contraction and in disease, yet they are remarkably understudied. Here we propose to take a multidisciplinary approach to decipher the role of the actin filament elongation protein, Lmod2, in cardiac development and in dilated cardiomyopathy. Our identification of the connection between thin filament length and cardiac function, as well as the role thin filament length dysregulation plays in cardiomyopathies will likely uncover insights into novel therapeutic targets for cardiomyopathy.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Heart, Lung, and Blood Institute (NHLBI)
Type
Research Project (R01)
Project #
5R01HL123078-03
Application #
9245733
Study Section
Cardiac Contractility, Hypertrophy, and Failure Study Section (CCHF)
Program Officer
Adhikari, Bishow B
Project Start
2015-04-01
Project End
2019-03-31
Budget Start
2017-04-01
Budget End
2018-03-31
Support Year
3
Fiscal Year
2017
Total Cost
$442,774
Indirect Cost
$151,272

  Institution

Name
University of Arizona
Department
Anatomy/Cell Biology
Type
Schools of Medicine
DUNS #
806345617
City
Tucson
State
AZ
Country
United States
Zip Code
85721

  Publications

Trembley, Michael A; Quijada, Pearl; Agullo-Pascual, Esperanza et al. (2018) Mechanosensitive Gene Regulation by Myocardin-Related Transcription Factors Is Required for Cardiomyocyte Integrity in Load-Induced Ventricular Hypertrophy. Circulation 138:1864-1878
Chu, Miensheng; Novak, Stefanie Mares; Cover, Cathleen et al. (2018) Increased Cardiac Arrhythmogenesis Associated With Gap Junction Remodeling With Upregulation of RNA-Binding Protein FXR1. Circulation 137:605-618
Sun, Xin; Hota, Swetansu K; Zhou, Yu-Qing et al. (2018) Cardiac-enriched BAF chromatin-remodeling complex subunit Baf60c regulates gene expression programs essential for heart development and function. Biol Open 7:
Pappas, Christopher T; Farman, Gerrie P; Mayfield, Rachel M et al. (2018) Cardiac-specific knockout of Lmod2 results in a severe reduction in myofilament force production and rapid cardiac failure. J Mol Cell Cardiol 122:88-97
Henderson, Christine A; Gomez, Christopher G; Novak, Stefanie M et al. (2017) Overview of the Muscle Cytoskeleton. Compr Physiol 7:891-944
Wu, Tongbin; Mu, Yongxin; Bogomolovas, Julius et al. (2017) HSPB7 is indispensable for heart development by modulating actin filament assembly. Proc Natl Acad Sci U S A 114:11956-11961
Kolb, Justin; Li, Frank; Methawasin, Mei et al. (2016) Thin filament length in the cardiac sarcomere varies with sarcomere length but is independent of titin and nebulin. J Mol Cell Cardiol 97:286-94
Behunin, Samantha M; Lopez-Pier, Marissa A; Mayfield, Rachel M et al. (2016) Liver Kinase B1 complex acts as a novel modifier of myofilament function and localizes to the Z-disk in cardiac myocytes. Arch Biochem Biophys 601:32-41
Ly, Thu; Moroz, Natalia; Pappas, Christopher T et al. (2016) The N-terminal tropomyosin- and actin-binding sites are important for leiomodin 2's function. Mol Biol Cell 27:2565-75
Winter, Josine M de; Joureau, Barbara; Lee, Eun-Jeong et al. (2016) Mutation-specific effects on thin filament length in thin filament myopathy. Ann Neurol 79:959-69

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