Cardiovascular Development and the Colonizing Cardiac Neural Crest Lineage
TL;DR: Recent data suggest mouse and chick are more similar to each other than to the zebrafish neural crest cell lineage, and potential function/s of cardiac neural crest-derived cells during cardiovascular developmental remodeling are discussed.
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Abstract: Although it is well established that transgenic manipulation of mammalian neural crest-related gene expression and microsurgical removal of premigratory chicken and Xenopus embryonic cardiac neural crest progenitors results in a wide spectrum of both structural and functional congenital heart defects, the actual functional mechanism of the cardiac neural crest cells within the heart is poorly understood. Neural crest cell migration and appropriate colonization of the pharyngeal arches and outflow tract septum is thought to be highly dependent on genes that regulate cell-autonomous polarized movement (i.e., gap junctions, cadherins, and noncanonical Wnt1 pathway regulators). Once the migratory cardiac neural crest subpopulation finally reaches the heart, they have traditionally been thought to participate in septation of the common outflow tract into separate aortic and pulmonary arteries. However, several studies have suggested these colonizing neural crest cells may also play additional unexpected roles during cardiovascular development and may even contribute to a crest-derived stem cell population. Studies in both mice and chick suggest they can also enter the heart from the venous inflow as well as the usual arterial outflow region, and may contribute to the adult semilunar and atrioventricular valves as well as part of the cardiac conduction system. Furthermore, although they are not usually thought to give rise to the cardiomyocyte lineage, neural crest cells in the zebrafish (Danio rerio) can contribute to the myocardium and may have different functions in a species-dependent context. Intriguingly, both ablation of chick and Xenopus premigratory neural crest cells, and a transgenic deletion of mouse neural crest cell migration or disruption of the normal mammalian neural crest gene expression profiles, disrupts ventral myocardial function and/or cardiomyocyte proliferation. Combined, this suggests that either the cardiac neural crest secrete factor/s that regulate myocardial proliferation, can signal to the epicardium to subsequently secrete a growth factor/s, or may even contribute directly to the heart. Although there are species differences between mouse, chick, and Xenopus during cardiac neural crest cell morphogenesis, recent data suggest mouse and chick are more similar to each other than to the zebrafish neural crest cell lineage. Several groups have used the genetically defined Pax3 (splotch) mutant mice model to address the role of the cardiac neural crest lineage. Here we review the current literature, the neural crest-related role of the Pax3 transcription factor, and discuss potential function/s of cardiac neural crest-derived cells during cardiovascular developmental remodeling.
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Citations
Reprogramming Axial Level Identity to Rescue Neural-Crest-Related Congenital Heart Defects.
TL;DR: Results reveal a transcriptional program sufficient to confer cardiac potential onto trunk neural crest cells, thus implicating new genes in cardiovascular birth defects, and identifies cardiac-crest-specific transcription factors.
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Cardiac outflow tract development relies on the complex function of Sox4 and Sox11 in multiple cell types.
TL;DR: It is demonstrated that Sox4 and Sox11 have multiple functions in several cell types during outflow tract formation and may thus help to understand the basis of congenital heart defects in humans.
49
Lineage-specific responses to reduced embryonic Pax3 expression levels.
TL;DR: There are different minimum threshold requirements for Pax3 within different Pax3-expressing lineages, which demonstrate a lineage-specific response to approximately 80% loss of Pax3 protein expression, with myogenesis of limb and tongue being most sensitive to reduced Pax3 levels.
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Trigenic neural crest-restricted Smad7 over-expression results in congenital craniofacial and cardiovascular defects
TL;DR: TGFbeta superfamily signaling plays an essential role during craniofacial and cardiac NCC colonization and cell survival in vivo, and induction of Smad7 in post-migratory NCC resulted in interventricular septal chamber septation defects.
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Development of cardiac form and function in ectothermic sauropsids.
TL;DR: This essay attempts a synthesis of sauropsid cardiovascular development based on the limited literature and identifies fertile regions for future studies of this diverse vertebrate lineage.
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