Abstract

Cardiovascular diseases remain a leading cause of morbidity and mortality. Many of these diseases originate at least in part from genetic defects that impact the development and maturation of the cardiovascular system. Despite substantial progress in our understanding of cardiovascular development and its role in disease susceptibility, much remains to be learned. The focus of this proposal is on cardiac trabeculation, a fundamental aspect of cardiac development that modulates cardiomyocyte mass and cardiac function. Interestingly, trabeculae initially form only in the ventricle but not the atrium, and within the ventricle, they only form in the outer but not the inner curvature. These observations indicate that cardiac trabeculation is regulated by genetic as well as epigenetic factors, such as flow. We will continue to take advantage of the zebrafish system to investigate several aspects of cardiac trabeculation. Our data indicate that 1) cardiac trabeculation initiates by the directed migration/delamination of cardiomyocytes from the compact layer, 2) in zebrafish, as in mouse, Erbb2 signaling is absolutely required for cardiac trabeculation (but importantly why or how it is required remains unclear), and 3) cardiac function is required for cardiac trabeculation. These and other data lead us to propose to test the following three hypotheses: 1) cardiac trabeculation initiates via the directed migration/ delamination of cardiomyocytes. We will analyze at single cell resolution a) the distribution and behavior of small clones of labeled cardiomyocytes as trabeculae form, b) the patterns of cardiomyocyte division during the initiation and expansion of trabeculae, and c) apicobasal polarity of cardiomyocytes in the compact and trabecular layers. 2) Erbb2 signaling regulates cardiac trabeculation via its role in modulating cardiomyocyte epithelial to mesenchymal transformation (EMT) including the loss of apicobasal polarity. Experiments are designed to a) test the cell autonomy of Erbb2 function in the initiation of cardiac trabeculation, b) investigate the regulation of Neuregulin (Nrg) in the initiation of cardiac trabeculation, c) investigate the mechanism of action of Erbb2 signaling in the initiation of cardiac trabeculation, and d) investigate the potential link between Erbb2 signaling and cardiomyocyte EMT, loss of apicobasal polarity and apical constriction. 3) cardiomyocyte contractility and shear stress regulate cardiac trabeculation. Experiments are designed to a) test the role of cardiomyocyte contractility in the initiation of cardiac trabeculation, and b) test the role of flow in the initiation of cardiac trabeculation. These studies will help understand mechanisms of cardiac trabeculation. They should also shed new light on the function of Erbb signaling in cardiomyocyte biology beyond trabeculation as Erbb signaling has been implicated in differentiated cardiomyocyte proliferation and repair of heart injury. Furthermore, they should help elucidate the critical, yet poorly understood, role of cardiac function in cardiac development.

Public Health Relevance

Cardiovascular diseases remain a leading cause of morbidity and mortality. Many of these diseases originate at least in part from genetic defects that impact the development and maturation of the cardiovascular system. Despite substantial progress in our understanding of cardiovascular development and its role in disease susceptibility, much remains to be learned. The focus of this proposal is on cardiac trabeculation, a fundamental aspect of cardiac development that modulates cardiomyocyte mass and cardiac function. For example, defects in trabeculation have been associated with some cases of Non-Compaction of the Left Ventricular Myocardium, a severe pediatric malformation. The proposed studies will help us understand cellular and molecular mechanisms of cardiac trabeculation. Recently, Nrg/Erbb signaling has also been implicated in differentiated cardiomyocyte proliferation and repair of heart injury (Bersell et al., 2009), and anticancer drugs targeted to the Erbb2 receptor frequently cause ventricular dysfunction (reviewed by De Keulenaer et al., 2010). Thus, by investigating the downstream mechanisms of Erbb2 signaling in the heart, our studies should shed new light on the action of this important signaling pathway in cardiomyocyte biology beyond trabecular formation. Our studies will also generate new tools and reagents to investigate and manipulate cardiomyocyte proliferation. Furthermore, they should help elucidate the critical, yet poorly understood, role of cardiac function (via cardiomyocyte contractility and flow) in cardiac development.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Heart, Lung, and Blood Institute (NHLBI)
Type
Research Project (R01)
Project #
2R01HL054737-16
Application #
8108111
Study Section
Cardiovascular Differentiation and Development Study Section (CDD)
Program Officer
Schramm, Charlene A
Project Start
1996-04-01
Project End
2016-04-30
Budget Start
2011-05-01
Budget End
2012-04-30
Support Year
16
Fiscal Year
2011
Total Cost
$376,215
Indirect Cost

  Institution

Name
University of California San Francisco
Department
Biochemistry
Type
Schools of Medicine
DUNS #
094878337
City
San Francisco
State
CA
Country
United States
Zip Code
94143

  Publications

Zhang, Qiang; Huang, Hai; Zhang, Luqing et al. (2018) Visualizing Dynamics of Cell Signaling In Vivo with a Phase Separation-Based Kinase Reporter. Mol Cell 69:334-346.e4
Schepis, Antonino; Barker, Adrian; Srinivasan, Yoga et al. (2018) Protease signaling regulates apical cell extrusion, cell contacts, and proliferation in epithelia. J Cell Biol 217:1097-1112
Reade, Anna; Motta-Mena, Laura B; Gardner, Kevin H et al. (2017) TAEL: a zebrafish-optimized optogenetic gene expression system with fine spatial and temporal control. Development 144:345-355
Pestel, Jenny; Ramadass, Radhan; Gauvrit, Sebastien et al. (2016) Real-time 3D visualization of cellular rearrangements during cardiac valve formation. Development 143:2217-27
Ahuja, Suchit; Dogra, Deepika; Stainier, Didier Y R et al. (2016) Id4 functions downstream of Bmp signaling to restrict TCF function in endocardial cells during atrioventricular valve development. Dev Biol 412:71-82
Clay, Hilary; Wilsbacher, Lisa D; Wilson, Stephen J et al. (2016) Sphingosine 1-phosphate receptor-1 in cardiomyocytes is required for normal cardiac development. Dev Biol 418:157-165
Matsuoka, Ryota L; Marass, Michele; Avdesh, Avdesh et al. (2016) Radial glia regulate vascular patterning around the developing spinal cord. Elife 5:
To, Tsz-Leung; Schepis, Antonino; Ruiz-González, Rubén et al. (2016) Rational Design of a GFP-Based Fluorogenic Caspase Reporter for Imaging Apoptosis In Vivo. Cell Chem Biol 23:875-882
Reischauer, Sven; Stone, Oliver A; Villasenor, Alethia et al. (2016) Cloche is a bHLH-PAS transcription factor that drives haemato-vascular specification. Nature 535:294-8
Orr, Nathan; Arnaout, Rima; Gula, Lorne J et al. (2016) A mutation in the atrial-specific myosin light chain gene (MYL4) causes familial atrial fibrillation. Nat Commun 7:11303

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