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Literature DB >> 19835857

The role of secondary heart field in cardiac development.

Abstract

Although de la Cruz and colleagues showed as early as 1977 that the outflow tract was added after the heart tube formed, the source of these secondarily added cells was not identified for nearly 25 years. In 2001, three pivotal publications described a secondary or anterior heart field that contributed to the developing outflow tract. This review details the history of the heart field, the discovery and continuing elucidation of the secondarily adding myocardial cells, and how the different populations identified in 2001 are related to the more recent lineage tracing studies that defined the first and second myocardial heart fields/lineages. Much recent work has focused on secondary heart field progenitors that give rise to the myocardium and smooth muscle at the definitive arterial pole. These progenitors are the last to be added to the arterial pole and are particularly susceptible to abnormal development, leading to conotruncal malformations in children. The major signaling pathways (Wnt, BMP, FGF8, Notch, and Shh) that control various aspects of secondary heart field progenitor behavior are discussed.

Entities: CellLine Chemical Disease Gene Species

Mesh：

Year: 2009 PMID： 19835857 PMCID： PMC2794420 DOI： 10.1016/j.ydbio.2009.10.009

Source DB: PubMed Journal: Dev Biol ISSN： 0012-1606 Impact factor: 3.582

84 in total

Review 1. Heart development: molecular insights into cardiac specification and early morphogenesis.

Authors: Thomas Brand
Journal: Dev Biol Date: 2003-06-01 Impact factor: 3.582

2. A retrospective clonal analysis of the myocardium reveals two phases of clonal growth in the developing mouse heart.

Authors: Sigolène M Meilhac; Robert G Kelly; Didier Rocancourt; Sophie Eloy-Trinquet; Jean-François Nicolas; Margaret E Buckingham
Journal: Development Date: 2003-08 Impact factor: 6.868

3. Differential requirements for Smad4 in TGFbeta-dependent patterning of the early mouse embryo.

Authors: Gerald C Chu; N Ray Dunn; Dorian C Anderson; Leif Oxburgh; Elizabeth J Robertson
Journal: Development Date: 2004-06-23 Impact factor: 6.868

Review 4. Heart fields: one, two or more?

Authors: Radwan Abu-Issa; Karen Waldo; Margaret L Kirby
Journal: Dev Biol Date: 2004-08-15 Impact factor: 3.582

5. Experimental study of the development of the truncus and the conus in the chick embryo.

Authors: M V de la Cruz; C Sánchez Gómez; M M Arteaga; C Argüello
Journal: J Anat Date: 1977-07 Impact factor: 2.610

6. The precardiac areas and formation of the tubular heart in the chick embryo.

Authors: H Stalsberg; R L DeHaan
Journal: Dev Biol Date: 1969-02 Impact factor: 3.582

7. Wnt-11 activation of a non-canonical Wnt signalling pathway is required for cardiogenesis.

Authors: Petra Pandur; Matthias Läsche; Leonard M Eisenberg; Michael Kühl
Journal: Nature Date: 2002-08-08 Impact factor: 49.962

8. Isl1 identifies a cardiac progenitor population that proliferates prior to differentiation and contributes a majority of cells to the heart.

Authors: Chen-Leng Cai; Xingqun Liang; Yunqing Shi; Po-Hsien Chu; Samuel L Pfaff; Ju Chen; Sylvia Evans
Journal: Dev Cell Date: 2003-12 Impact factor: 12.270

9. Dynamic patterns of expression of BMP isoforms 2, 4, 5, 6, and 7 during chicken heart development.

Authors: Semir Somi; Anita A M Buffing; Antoon F M Moorman; Maurice J B Van Den Hoff
Journal: Anat Rec A Discov Mol Cell Evol Biol Date: 2004-07

10. Fgf8 is required for pharyngeal arch and cardiovascular development in the mouse.

Authors: Radwan Abu-Issa; Graham Smyth; Ida Smoak; Ken-ichi Yamamura; Erik N Meyers
Journal: Development Date: 2002-10 Impact factor: 6.868

98 in total

1. Arterial pole progenitors interpret opposing FGF/BMP signals to proliferate or differentiate.

Authors: Mary Redmond Hutson; Xiaopei Lily Zeng; Andrew J Kim; Emily Antoon; Stephen Harward; Margaret L Kirby
Journal: Development Date: 2010-08-11 Impact factor: 6.868

2. AcvR1-mediated BMP signaling in second heart field is required for arterial pole development: implications for myocardial differentiation and regional identity.

Authors: Penny S Thomas; Sudha Rajderkar; Jamie Lane; Yuji Mishina; Vesa Kaartinen
Journal: Dev Biol Date: 2014-03-27 Impact factor: 3.582

10. Disheveled mediated planar cell polarity signaling is required in the second heart field lineage for outflow tract morphogenesis.

Authors: Tanvi Sinha; Bing Wang; Sylvia Evans; Anthony Wynshaw-Boris; Jianbo Wang
Journal: Dev Biol Date: 2012-07-27 Impact factor: 3.582

The role of secondary heart field in cardiac development.

Review 1. Heart development: molecular insights into cardiac specification and early morphogenesis.

2. A retrospective clonal analysis of the myocardium reveals two phases of clonal growth in the developing mouse heart.

3. Differential requirements for Smad4 in TGFbeta-dependent patterning of the early mouse embryo.

Review 4. Heart fields: one, two or more?

5. Experimental study of the development of the truncus and the conus in the chick embryo.

6. The precardiac areas and formation of the tubular heart in the chick embryo.

7. Wnt-11 activation of a non-canonical Wnt signalling pathway is required for cardiogenesis.

8. Isl1 identifies a cardiac progenitor population that proliferates prior to differentiation and contributes a majority of cells to the heart.

9. Dynamic patterns of expression of BMP isoforms 2, 4, 5, 6, and 7 during chicken heart development.

10. Fgf8 is required for pharyngeal arch and cardiovascular development in the mouse.

1. Arterial pole progenitors interpret opposing FGF/BMP signals to proliferate or differentiate.

2. AcvR1-mediated BMP signaling in second heart field is required for arterial pole development: implications for myocardial differentiation and regional identity.

3. Wnt signaling balances specification of the cardiac and pharyngeal muscle fields.

Review 4. The neural crest in cardiac congenital anomalies.

5. Complex trait analysis of ventricular septal defects caused by Nkx2-5 mutation.

6. Cardiac origin of smooth muscle cells in the inflow tract.

Review 7. The cardiac hypoxic niche: emerging role of hypoxic microenvironment in cardiac progenitors.

8. Cadm4 restricts the production of cardiac outflow tract progenitor cells.

9. Disruption of spatiotemporal hypoxic signaling causes congenital heart disease in mice.

10. Disheveled mediated planar cell polarity signaling is required in the second heart field lineage for outflow tract morphogenesis.