Abstract

The ultimate aim of this research is to determine the potential role of dystroglycan dysfunction in congenital heart disease. The overall objective of this project is to investigate the function of dystroglycan in cardiac embryogenesis. Extracellular matrix components and receptors are critical for the morphogenesis of the heart and are excellent candidates for involvement in congenital heart disease including atrioventricular canal defects and perimembranous interventricular septal defects. Dystroglycan is a broadly expressed cell surface extracellular matrix receptor that is linked to the cytoskeleton. Recent studies have indicated that dystroglycan plays a critical role in myogenesis and organogenesis. To investigate the role of dystroglycan in developmental processes, the investigators disrupted the dystroglycan gene in the mouse. The null mutation results in early embryonic lethality, prior to the onset of gastrulation. This phenotype stems from the failed development of Reichert's membrane, an extraembryonic basement membrane structure in which dystroglycan is also expressed. From these studies, dystroglycan seems to be required for either the anchorage of cells to the extracellular matrix or the assembly of networks of extracellular matrix proteins. Dystroglycan's involvement with extracellular matrix and its expression in various cell types suggest that it could be involved in many aspects of heart morphogenesis. To begin to address the role of dystroglycan in cardiac embryogenesis, the investigators will first define the developmental expression of dystroglycan in the heart (Specific Aim 1). To directly examine dystroglycan's function in heart embryogenesis, the investigators have proposed experiments to circumvent the early lethality of the dystroglycan null mutation so that the investigators may analyze dystroglycan's role later during heart development (Specific Aims 2 to 4). The first specific aim will utilize normal mouse embryos to establish a map of the spatial and temporal pattern of expression of dystroglycan during heart development.
The second aim will analyze the cellular role of dystroglycan in the development of cardiomyocytes in embryoid bodies.
The third aim will use tetraploid complementation in order to rescue the Reichert's membrane defect and thus allow them to examine dystroglycan-null embryos that develop to later stages after the onset of heart development.
The fourth aim will be the myocardium-specific disruption of the dystroglycan gene. The goal of the last two specific aims is to examine heart development in embryos that lack dystroglycan in all cells (Specific Aim 3) or just cardiomyocytes (Specific Aim 4). The complementary approaches outlined in these specific aims will yield a new understanding of the role of dystroglycan in heart development and will constitute a foundation for future investigations directed toward the identification of congenital heart disease patients with abnormalities in dystroglycan function.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Heart, Lung, and Blood Institute (NHLBI)
Type
Specialized Center (P50)
Project #
5P50HL062178-02
Application #
6302555
Study Section
Project Start
2000-02-15
Project End
2000-12-31
Budget Start
Budget End
Support Year
2
Fiscal Year
2000
Total Cost
$132,307
Indirect Cost

  Institution

Name
University of Iowa
Department
Type
DUNS #
041294109
City
Iowa City
State
IA
Country
United States
Zip Code
52242

  Publications

Patel, Sonali S; Mahoney, Larry T; Burns, Trudy L (2012) Is a shorter atrioventricular septal length an intermediate phenotype in the spectrum of nonsyndromic atrioventricular septal defects? J Am Soc Echocardiogr 25:782-9
Bartlett, Heather L; Sutherland, Lillian; Kolker, Sandra J et al. (2007) Transient early embryonic expression of Nkx2-5 mutations linked to congenital heart defects in human causes heart defects in Xenopus laevis. Dev Dyn 236:2475-84
Mitchell, Tracy; Jones, Elizabeth A; Weeks, Daniel L et al. (2007) Chordin affects pronephros development in Xenopus embryos by anteriorizing presomitic mesoderm. Dev Dyn 236:251-61
Collop, Andrew H; Broomfield, Joel A S; Chandraratna, Roshantha A S et al. (2006) Retinoic acid signaling is essential for formation of the heart tube in Xenopus. Dev Biol 291:96-109
Knauert, Melissa P; Lloyd, Janice A; Rogers, Faye A et al. (2005) Distance and affinity dependence of triplex-induced recombination. Biochemistry 44:3856-64
Kalish, Jennifer M; Seidman, Michael M; Weeks, Daniel L et al. (2005) Triplex-induced recombination and repair in the pyrimidine motif. Nucleic Acids Res 33:3492-502
Zheng, Wei; Christensen, Lance P; Tomanek, Robert J (2004) Stretch induces upregulation of key tyrosine kinase receptors in microvascular endothelial cells. Am J Physiol Heart Circ Physiol 287:H2739-45
Jallow, Zainab; Jacobi, Ulrike G; Weeks, Daniel L et al. (2004) Specialized and redundant roles of TBP and a vertebrate-specific TBP paralog in embryonic gene regulation in Xenopus. Proc Natl Acad Sci U S A 101:13525-30
Tomanek, Robert J; Zheng, Wei; Yue, Xinping (2004) Growth factor activation in myocardial vascularization: therapeutic implications. Mol Cell Biochem 264:3-11
Sheffield, Val C (2004) Use of isolated populations in the study of a human obesity syndrome, the Bardet-Biedl syndrome. Pediatr Res 55:908-11

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