Abstract

Division of the cardiac tube into four chambers and two outflow vessels is critical in normal heart development. The septum that converts the original single outflow vessel into an aorta and pulmonary trunk depends on the integrity of the cardiac neural crest cell population that migrates from the caudal hindbrain via the pharyngeal arches into the outflow tract. This cell population subdivides into ectomesenchymal and neural lineages. The ectomesenchymal lineage participates in structural development of the outflow septum while the neural lineage forms the cardiac parasympathetic innervation. The lineage decision is critical because commitment of too many cells to either lineage will affect the other population and result in either congenital cardiac defects or disturbed innervation of the heart. The cellular mechanism for the separation of the neural crest cells into these two lineages is not known. The hypothesis for this proposal is that Mash-1 and the Notch family of genes are involved in the lineage decisions. Many of these genes have recently been targeted for null mutation in mice. The homozygote Mash-1 mutant mouse has no parasympathetic cardiac innervation, indicating an inability of the cardiac neural crest to commit to the neural lineage. In this case, it is not known what happens to the ectomesenchymal lineage. Mice with null mutations in Notch family genes do not survive into the period when cardiac neural crest can be analyzed. We propose to rescue the mutant mouse cardiac neural crest cells by constructing mouse-chick chimeras. The cardiac region of the neural tube will be transplanted into chick embryos lacking the cardiac neural crest. The prospective potency of Mash-1-/- and Notch-/- cells will be determined by analyzing cell fate, proliferation and cell death at three times after implantation of the cells. The role of gene dosage will be determined by mixing cells from wide-type, heterozygote, and homozygote mutant mice prior to implantation into the chick host. Finally, it has been proposed that the development of the coronary vascular tree and Purkinje cells depends on formation of the cardiac ganglia. The development of the conduction system will be assessed in Mash-/- chimeras.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
Eunice Kennedy Shriver National Institute of Child Health & Human Development (NICHD)
Type
Research Project (R01)
Project #
2R01HD017063-13
Application #
2025063
Study Section
Human Embryology and Development Subcommittee 1 (HED)
Project Start
1982-04-01
Project End
2002-03-31
Budget Start
1997-04-01
Budget End
1998-03-31
Support Year
13
Fiscal Year
1997
Total Cost
Indirect Cost

  Institution

Name
Medical College of Georgia (MCG)
Department
Internal Medicine/Medicine
Type
Schools of Medicine
DUNS #
City
Augusta
State
GA
Country
United States
Zip Code
30912

  Publications

Hutson, Mary Redmond; Kirby, Margaret L (2003) Neural crest and cardiovascular development: a 20-year perspective. Birth Defects Res C Embryo Today 69:2-13
Yelbuz, T Mesud; Waldo, Karen L; Zhang, Xiaowei et al. (2003) Myocardial volume and organization are changed by failure of addition of secondary heart field myocardium to the cardiac outflow tract. Dev Dyn 228:152-60
Li, Yin-Xiong; Zdanowicz, Marzena; Young, Lori et al. (2003) Cardiac neural crest in zebrafish embryos contributes to myocardial cell lineage and early heart function. Dev Dyn 226:540-50
Kirby, Margaret L; Lawson, Aaron; Stadt, Harriett A et al. (2003) Hensen's node gives rise to the ventral midline of the foregut: implications for organizing head and heart development. Dev Biol 253:175-88
Yelbuz, T Mesud; Zhang, Xiaowei; Choma, Michael A et al. (2003) Images in cardiovascular medicine. Approaching cardiac development in three dimensions by magnetic resonance microscopy. Circulation 108:e154-5
Li, Yin-Xiong; Kirby, Margaret L (2003) Coordinated and conserved expression of alphoid repeat and alphoid repeat-tagged coding sequences. Dev Dyn 228:72-81
Farrell, M J; Burch, J L; Wallis, K et al. (2001) FGF-8 in the ventral pharynx alters development of myocardial calcium transients after neural crest ablation. J Clin Invest 107:1509-17
Waldo, K L; Kumiski, D H; Wallis, K T et al. (2001) Conotruncal myocardium arises from a secondary heart field. Development 128:3179-88
Li, Y X; Farrell, M J; Liu, R et al. (2000) Double-stranded RNA injection produces null phenotypes in zebrafish. Dev Biol 217:394-405
Waldo, K L; Lo, C W; Kirby, M L (1999) Connexin 43 expression reflects neural crest patterns during cardiovascular development. Dev Biol 208:307-23

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