Literature DB >> 17238175

Morphological and molecular left-right asymmetries in the development of the proepicardium: a comparative analysis on mouse and chick embryos.

Inga Schulte1, Jan Schlueter, Radwan Abu-Issa, Thomas Brand, Jörg Männer.   

Abstract

The proepicardium (PE) is an embryonic progenitor cell population that delivers the epicardium, the majority of the cardiac interstitium, and the coronary vasculature. In the present study, we compared PE development in mouse and chick embryos. In the mouse, a left and a right PE anlage appear simultaneously, which subsequently merge at the embryonic midline to form a single PE. In chick embryos, the right PE anlage appears earlier than the left and only the right anlage acquires the full PE-phenotype. The left anlage remains in a rudimentary state. The expression patterns of PE marker genes (Tbx18, Wt1) correspond to the morphological data, being bilateral in the mouse and unilateral in the chick. Bmp4, which is unilaterally expressed in the right PE of chick embryos, is symmetrically expressed in the sinus venosus wall cranial to the PE in mouse embryos. Asymmetric development of the chicken PE might reflect side-specific differences in topographical relationships to tissues with PE-inducing or repressing activity or might result from the PE-repressing activity of the right PE, which grows earlier. To test these hypotheses, we analyzed PE development in chick embryos, firstly, subsequent to experimentally induced inversion of PE topographical relationships to neighbouring tissues; secondly, in organ cultures; and, thirdly, subsequent to induction of cardia bifida. In all three experiments, only the right PE develops the full PE phenotype. Our results suggest that PE development might be controlled by the L-R pathway in the chick but not in the mouse embryo.

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Year:  2007        PMID: 17238175     DOI: 10.1002/dvdy.21065

Source DB:  PubMed          Journal:  Dev Dyn        ISSN: 1058-8388            Impact factor:   3.780


  31 in total

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Journal:  J Cardiovasc Transl Res       Date:  2012-06-01       Impact factor: 4.132

2.  Identification of a novel developmental mechanism in the generation of mesothelia.

Authors:  Nichelle I Winters; Rebecca T Thomason; David M Bader
Journal:  Development       Date:  2012-07-04       Impact factor: 6.868

3.  The Lhx9-integrin pathway is essential for positioning of the proepicardial organ.

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Journal:  Development       Date:  2016-01-25       Impact factor: 6.868

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5.  Effects of endothelial growth media on proepicardial cell gene expression and morphogenesis in 3D collagen matrices.

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Journal:  In Vitro Cell Dev Biol Anim       Date:  2009-12       Impact factor: 2.416

Review 6.  Coronary vessel development and insight towards neovascular therapy.

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7.  Tcf21 regulates the specification and maturation of proepicardial cells.

Authors:  Panna Tandon; Yana V Miteva; Lauren M Kuchenbrod; Ileana M Cristea; Frank L Conlon
Journal:  Development       Date:  2013-05-01       Impact factor: 6.868

Review 8.  Cardiac cell lineages that form the heart.

Authors:  Sigolène M Meilhac; Fabienne Lescroart; Cédric Blanpain; Margaret E Buckingham
Journal:  Cold Spring Harb Perspect Med       Date:  2014-09-02       Impact factor: 6.915

9.  A caudal proliferating growth center contributes to both poles of the forming heart tube.

Authors:  Gert van den Berg; Radwan Abu-Issa; Bouke A de Boer; Mary R Hutson; Piet A J de Boer; Alexandre T Soufan; Jan M Ruijter; Margaret L Kirby; Maurice J B van den Hoff; Antoon F M Moorman
Journal:  Circ Res       Date:  2008-12-04       Impact factor: 17.367

10.  Epicardium and myocardium separate from a common precursor pool by crosstalk between bone morphogenetic protein- and fibroblast growth factor-signaling pathways.

Authors:  Bram van Wijk; Gert van den Berg; Radwan Abu-Issa; Phil Barnett; Saskia van der Velden; Martina Schmidt; Jan M Ruijter; Margaret L Kirby; Antoon F M Moorman; Maurice J B van den Hoff
Journal:  Circ Res       Date:  2009-07-23       Impact factor: 17.367

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