Cell biology of cardiac cushion development

Anthony D. Person; Scott E. Klewer; Raymond B. Runyan

doi:10.1016/S0074-7696(05)43005-3

Cell biology of cardiac cushion development

Anthony D. Person, Scott E. Klewer, Raymond B. Runyan

Research output: Contribution to journal › Article › peer-review

304 Scopus citations

Abstract

The valves of the heart develop in the embryo from precursor structures called endocardial cushions. After cardiac looping, endocardial cushion swellings form and become populated by valve precursor cells formed by an epithelial-mesenchymal transition (EMT). Endocardial cushions subsequently undergo directed growth and remodeling to form the valvular structures and the membranous septa of the mature heart. The developmental processes that mediate cushion formation include many prototypic cellular actions including adhesion, signaling, migration, secretion, replication, differentiation, and apoptosis. Cushion morphogenesis is unique in that these cellular possesses occur in a functioning organ where the cushions act as valves even while developing into definitive valvular structures. Cardiovascular defects are the most common congenital defects, and one of the most common causes of death during infancy. Thus, there is significant interest in understanding the mechanisms that underlie this complex developmental process. In this regard, substantial progress has been made by incorporating an understanding of cardiac morphology and cell biology with the rapidly expanding repertoire of molecular mechanisms gained through human genetics and research using animal models. This article reviews cardiac morphogenesis as it relates to heart valve formation and highlights selected growth factors, intracellular signaling mediators, and extracellular matrix components involved in the creation and remodeling of endocardial cushions into mature cardiac structures.

Original language	English (US)
Pages (from-to)	287-335
Number of pages	49
Journal	International Review of Cytology
Volume	243
DOIs	https://doi.org/10.1016/S0074-7696(05)43005-3
State	Published - 2005

Keywords

BMP
Cell invasion
Extracellular matrix
Notch
Transforming growth factor β
Wnt
erbB3
β-Catenin

ASJC Scopus subject areas

Histology
Cell Biology

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10.1016/S0074-7696(05)43005-3

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@article{bc84202a66a747aa923e079e0be5a054,

title = "Cell biology of cardiac cushion development",

abstract = "The valves of the heart develop in the embryo from precursor structures called endocardial cushions. After cardiac looping, endocardial cushion swellings form and become populated by valve precursor cells formed by an epithelial-mesenchymal transition (EMT). Endocardial cushions subsequently undergo directed growth and remodeling to form the valvular structures and the membranous septa of the mature heart. The developmental processes that mediate cushion formation include many prototypic cellular actions including adhesion, signaling, migration, secretion, replication, differentiation, and apoptosis. Cushion morphogenesis is unique in that these cellular possesses occur in a functioning organ where the cushions act as valves even while developing into definitive valvular structures. Cardiovascular defects are the most common congenital defects, and one of the most common causes of death during infancy. Thus, there is significant interest in understanding the mechanisms that underlie this complex developmental process. In this regard, substantial progress has been made by incorporating an understanding of cardiac morphology and cell biology with the rapidly expanding repertoire of molecular mechanisms gained through human genetics and research using animal models. This article reviews cardiac morphogenesis as it relates to heart valve formation and highlights selected growth factors, intracellular signaling mediators, and extracellular matrix components involved in the creation and remodeling of endocardial cushions into mature cardiac structures.",

keywords = "BMP, Cell invasion, Extracellular matrix, Notch, Transforming growth factor β, Wnt, erbB3, β-Catenin",

author = "Person, {Anthony D.} and Klewer, {Scott E.} and Runyan, {Raymond B.}",

note = "Funding Information: The majority of clinical heart defects involving abnormal AV cushion morphogenesis are diagnosed in infants with trisomy 21 (Down syndrome) ( Korenberg et al ., 1992 ). Likewise, most heart defects in trisomy 21 infants are atrioventricular septal defects (AVSDs) ( Adams et al ., 1981; Carmi et al ., 1992 ). This association has led to speculation that chromosome 21 genes are important in AV valve development. Genetic analyses have shown that variations in the collagen type VI (Col VI) locus on chromosome 21 are associated with AVSD in trisomy 21 ( Davies et al ., 1995 ). A potential role for Col VI, a microfibrillar component of the ECM ( Aumailley et al ., 1989, 1991 ), in AV valve morphogenesis is supported by its expression pattern in the developing heart. Col VI is expressed commensurate with cell migration within the developing AV cushions. Later in development, Col VI forms an organized extracellular network within the valve leaflets ( Klewer et al ., 1998 ). In human trisomy 21 and normal fetal hearts, consistent with gene dosage predictions, Col VI is increased in trisomy 21 AV valves. Importantly, however, increased Col VI immunoreactivity is similar in trisomy 21 hearts with AVSD and those without a congenital heart defect (CHD) ( Gittenberger-de Groot et al ., 2003 ). These data indicate that, although Col VI is an excellent molecular marker for cells in the developing AV valves, the clinical association between Col VI and AVSD is not direct. ",

year = "2005",

doi = "10.1016/S0074-7696(05)43005-3",

language = "English (US)",

volume = "243",

pages = "287--335",

journal = "International Review of Cytology",

issn = "0074-7696",

publisher = "Elsevier Inc.",

}

TY - JOUR

T1 - Cell biology of cardiac cushion development

AU - Person, Anthony D.

AU - Klewer, Scott E.

AU - Runyan, Raymond B.

N1 - Funding Information: The majority of clinical heart defects involving abnormal AV cushion morphogenesis are diagnosed in infants with trisomy 21 (Down syndrome) ( Korenberg et al ., 1992 ). Likewise, most heart defects in trisomy 21 infants are atrioventricular septal defects (AVSDs) ( Adams et al ., 1981; Carmi et al ., 1992 ). This association has led to speculation that chromosome 21 genes are important in AV valve development. Genetic analyses have shown that variations in the collagen type VI (Col VI) locus on chromosome 21 are associated with AVSD in trisomy 21 ( Davies et al ., 1995 ). A potential role for Col VI, a microfibrillar component of the ECM ( Aumailley et al ., 1989, 1991 ), in AV valve morphogenesis is supported by its expression pattern in the developing heart. Col VI is expressed commensurate with cell migration within the developing AV cushions. Later in development, Col VI forms an organized extracellular network within the valve leaflets ( Klewer et al ., 1998 ). In human trisomy 21 and normal fetal hearts, consistent with gene dosage predictions, Col VI is increased in trisomy 21 AV valves. Importantly, however, increased Col VI immunoreactivity is similar in trisomy 21 hearts with AVSD and those without a congenital heart defect (CHD) ( Gittenberger-de Groot et al ., 2003 ). These data indicate that, although Col VI is an excellent molecular marker for cells in the developing AV valves, the clinical association between Col VI and AVSD is not direct.

PY - 2005

Y1 - 2005

N2 - The valves of the heart develop in the embryo from precursor structures called endocardial cushions. After cardiac looping, endocardial cushion swellings form and become populated by valve precursor cells formed by an epithelial-mesenchymal transition (EMT). Endocardial cushions subsequently undergo directed growth and remodeling to form the valvular structures and the membranous septa of the mature heart. The developmental processes that mediate cushion formation include many prototypic cellular actions including adhesion, signaling, migration, secretion, replication, differentiation, and apoptosis. Cushion morphogenesis is unique in that these cellular possesses occur in a functioning organ where the cushions act as valves even while developing into definitive valvular structures. Cardiovascular defects are the most common congenital defects, and one of the most common causes of death during infancy. Thus, there is significant interest in understanding the mechanisms that underlie this complex developmental process. In this regard, substantial progress has been made by incorporating an understanding of cardiac morphology and cell biology with the rapidly expanding repertoire of molecular mechanisms gained through human genetics and research using animal models. This article reviews cardiac morphogenesis as it relates to heart valve formation and highlights selected growth factors, intracellular signaling mediators, and extracellular matrix components involved in the creation and remodeling of endocardial cushions into mature cardiac structures.

AB - The valves of the heart develop in the embryo from precursor structures called endocardial cushions. After cardiac looping, endocardial cushion swellings form and become populated by valve precursor cells formed by an epithelial-mesenchymal transition (EMT). Endocardial cushions subsequently undergo directed growth and remodeling to form the valvular structures and the membranous septa of the mature heart. The developmental processes that mediate cushion formation include many prototypic cellular actions including adhesion, signaling, migration, secretion, replication, differentiation, and apoptosis. Cushion morphogenesis is unique in that these cellular possesses occur in a functioning organ where the cushions act as valves even while developing into definitive valvular structures. Cardiovascular defects are the most common congenital defects, and one of the most common causes of death during infancy. Thus, there is significant interest in understanding the mechanisms that underlie this complex developmental process. In this regard, substantial progress has been made by incorporating an understanding of cardiac morphology and cell biology with the rapidly expanding repertoire of molecular mechanisms gained through human genetics and research using animal models. This article reviews cardiac morphogenesis as it relates to heart valve formation and highlights selected growth factors, intracellular signaling mediators, and extracellular matrix components involved in the creation and remodeling of endocardial cushions into mature cardiac structures.

KW - BMP

KW - Cell invasion

KW - Extracellular matrix

KW - Notch

KW - Transforming growth factor β

KW - Wnt

KW - erbB3

KW - β-Catenin

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AN - SCOPUS:16844380290

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JO - International Review of Cytology

JF - International Review of Cytology

ER -

Cell biology of cardiac cushion development

Abstract

Keywords

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