Abstract

The long-term objective of this proposal is to understand stem cell commitment and differentiation to a myocardial lineage. Our group has recently discovered a previously unknown secondary heart field that produces the myocardium of the definitive outflow tract in chick embryos. We have found that failure of outflow lengthening by addition of myocardial cells from the secondary heart field during cardiac looping results in dextroposed aorta. The overall hypothesis of the application is that the process of stem cell commitment to a myocardial lineage is common to all myocardial progenitor populations. The specific hypotheses to be tested in these experiments are: (1) The secondary heart field has an origin distinct from the primary heart field. This will be determined using three state-of-the-art cell tracing techniques in chick embryos. (2) Commitment of cells in the secondary heart field to the myocardial lineage is induced by members of the same growth factor families that induce myocardial commitment in the primary heart fields. TGFbeta and FGF family members are expressed in proximity to the outflow tract during its lengthening. Specific members of this family, including FGF-8 and BMP-2, will be manipulated in a variety of ways to determine their role in inducing differentiation of secondary heart field cells into myocardium. The studies proposed will establish the developmental history of the secondary heart field. Furthermore, because the outflow myocardium is critical for correct septation of the arterial pole of the heart, these studies will enhance our knowledge of normal development of the definitive outflow myocardium, and will provide new insights into the basis of conotruncal malformations. ? ?

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Heart, Lung, and Blood Institute (NHLBI)
Type
Research Project (R01)
Project #
5R01HL070140-02
Application #
6722778
Study Section
Cardiovascular and Pulmonary Research A Study Section (CVA)
Program Officer
Schramm, Charlene A
Project Start
2003-04-01
Project End
2007-03-31
Budget Start
2004-04-01
Budget End
2005-03-31
Support Year
2
Fiscal Year
2004
Total Cost
$308,000
Indirect Cost

  Institution

Name
Duke University
Department
Pediatrics
Type
Schools of Medicine
DUNS #
044387793
City
Durham
State
NC
Country
United States
Zip Code
27705

  Publications

Sato, Asako; Scholl, Ann Marie; Kuhn, E B et al. (2011) FGF8 signaling is chemotactic for cardiac neural crest cells. Dev Biol 354:18-30
Evans, Sylvia M; Yelon, Deborah; Conlon, Frank L et al. (2010) Myocardial lineage development. Circ Res 107:1428-44
Kirby, Margaret L; Hutson, Mary R (2010) Factors controlling cardiac neural crest cell migration. Cell Adh Migr 4:609-21
Hutson, Mary Redmond; Zeng, Xiaopei Lily; Kim, Andrew J et al. (2010) Arterial pole progenitors interpret opposing FGF/BMP signals to proliferate or differentiate. Development 137:3001-11
Dyer, Laura A; Makadia, Frini A; Scott, Alexandria et al. (2010) BMP signaling modulates hedgehog-induced secondary heart field proliferation. Dev Biol 348:167-76
Dyer, Laura A; Kirby, Margaret L (2009) Sonic hedgehog maintains proliferation in secondary heart field progenitors and is required for normal arterial pole formation. Dev Biol 330:305-17
Kirby, Margaret L (2009) Why don't they beat?: Cripto, apelin/APJ, and myocardial differentiation. Circ Res 105:211-3
Hutson, Mary Redmond; Sackey, Faustina N; Lunney, Katherine et al. (2009) Blocking hedgehog signaling after ablation of the dorsal neural tube allows regeneration of the cardiac neural crest and rescue of outflow tract septation. Dev Biol 335:367-73
Dyer, Laura A; Kirby, Margaret L (2009) The role of secondary heart field in cardiac development. Dev Biol 336:137-44
van den Berg, Gert; Abu-Issa, Radwan; de Boer, Bouke A et al. (2009) A caudal proliferating growth center contributes to both poles of the forming heart tube. Circ Res 104:179-88

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