BMP signaling positively regulates Nodal expression during left right specification in the chick embryo

M. Elisa Piedra; Mana A. Ros

doi:10.1242/dev.129.14.3431

BMP signaling positively regulates Nodal expression during left right specification in the chick embryo

Development ◽

10.1242/dev.129.14.3431 ◽

2002 ◽

Vol 129 (14) ◽

pp. 3431-3440 ◽

Cited By ~ 2

Author(s):

M. Elisa Piedra ◽

Mana A. Ros

Keyword(s):

Bmp Signaling ◽

Lateral Plate Mesoderm ◽

Lateral Plate ◽

Positive Role ◽

Molecular Control ◽

Left And Right ◽

Left Right Asymmetry ◽

The Right ◽

Rapid Activation ◽

Positive Effect

Exogenous application of BMP to the lateral plate mesoderm (LPM) of chick embryos at the early somite stage had a positive effect on Nodal expression. BMP applications into the right LPM were followed by a rapid activation of Nodal, while applications into the left LPM resulted in expansion of the normal domain of Nodal expression. Conversely, blocking of BMP signaling by Noggin in the left LPM interfered with the activation of Nodal expression. These results support a positive role for endogenous BMP on Nodal expression in the LPM. We also report that BMP positively regulates the expression of Caronte, Snail and Cfc in both the left and right LPM. BMP-treated embryos had molecular impairment of the midline with downregulation of Lefty1, Brachyury and Shh but we also show that the midline defect was not sufficient to induce ectopic Nodal expression. We discuss our findings in the context of the known molecular control of the specification of left-right asymmetry.

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The homeobox gene Pitx2: mediator of asymmetric left-right signaling in vertebrate heart and gut looping

Development ◽

10.1242/dev.126.6.1225 ◽

1999 ◽

Vol 126 (6) ◽

pp. 1225-1234 ◽

Cited By ~ 12

Author(s):

M. Campione ◽

H. Steinbeisser ◽

A. Schweickert ◽

K. Deissler ◽

F. van Bebber ◽

...

Keyword(s):

Ectopic Expression ◽

Homeobox Gene ◽

Zebrafish Embryos ◽

Lateral Plate Mesoderm ◽

Lateral Plate ◽

Left Right Asymmetry ◽

The Right ◽

Pitx2 Expression

Left-right asymmetry in vertebrates is controlled by activities emanating from the left lateral plate. How these signals get transmitted to the forming organs is not known. A candidate mediator in mouse, frog and zebrafish embryos is the homeobox gene Pitx2. It is asymmetrically expressed in the left lateral plate mesoderm, tubular heart and early gut tube. Localized Pitx2 expression continues when these organs undergo asymmetric looping morphogenesis. Ectopic expression of Xnr1 in the right lateral plate induces Pitx2 transcription in Xenopus. Misexpression of Pitx2 affects situs and morphology of organs. These experiments suggest a role for Pitx2 in promoting looping of the linear heart and gut.

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Persistent Ventricle Partitioning in the Adult Zebrafish Heart

Journal of Cardiovascular Development and Disease ◽

10.3390/jcdd8040041 ◽

2021 ◽

Vol 8 (4) ◽

pp. 41

Author(s):

Catherine Pfefferli ◽

Hannah R. Moran ◽

Anastasia Felker ◽

Christian Mosimann ◽

Anna Jaźwińska

Keyword(s):

Lateral Plate Mesoderm ◽

Adult Zebrafish ◽

Lateral Plate ◽

Second Heart Field ◽

Heart Field ◽

Left And Right ◽

First Heart Field ◽

The Right ◽

Physical Boundary ◽

Zebrafish Heart

The vertebrate heart integrates cells from the early-differentiating first heart field (FHF) and the later-differentiating second heart field (SHF), both emerging from the lateral plate mesoderm. In mammals, this process forms the basis for the development of the left and right ventricle chambers and subsequent chamber septation. The single ventricle-forming zebrafish heart also integrates FHF and SHF lineages during embryogenesis, yet the contributions of these two myocardial lineages to the adult zebrafish heart remain incompletely understood. Here, we characterize the myocardial labeling of FHF descendants in both the developing and adult zebrafish ventricle. Expanding previous findings, late gastrulation-stage labeling using drl-driven CreERT2 recombinase with a myocardium-specific, myl7-controlled, loxP reporter results in the predominant labeling of FHF-derived outer curvature and the right side of the embryonic ventricle. Raised to adulthood, such lineage-labeled hearts retain broad areas of FHF cardiomyocytes in a region of the ventricle that is positioned at the opposite side to the atrium and encompasses the apex. Our data add to the increasing evidence for a persisting cell-based compartmentalization of the adult zebrafish ventricle even in the absence of any physical boundary.

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BMP2 is a positive regulator of Nodal signaling during left-right axis formation in the chicken embryo

Development ◽

10.1242/dev.129.14.3421 ◽

2002 ◽

Vol 129 (14) ◽

pp. 3421-3429

Author(s):

Thomas Schlange ◽

Hans-Henning Arnold ◽

Thomas Brand

Keyword(s):

Bone Morphogenetic Proteins ◽

Target Genes ◽

Bmp Signaling ◽

Paraxial Mesoderm ◽

Axis Formation ◽

Nodal Signaling ◽

Lateral Plate Mesoderm ◽

Lateral Plate ◽

Positive Regulator ◽

The Right

A model of left-right axis formation in the chick involves inhibition of bone morphogenetic proteins by the antagonist Car as a mechanism of upregulating Nodal in the left lateral plate mesoderm. By contrast, expression of CFC, a competence factor, which is absolutely required for Nodal signaling in the lateral plate mesoderm is dependent on a functional BMP signaling pathway. We have therefore investigated the relationship between BMP and Nodal in further detail. We implanted BMP2 and Noggin-expressing cells into the left lateral plate and paraxial mesoderm and observed a strong upregulation of Nodal and its target genes Pitx2 and Nkx3.2. In addition Cfc, the Nodal type II receptor ActrIIa and Snr were found to depend on BMP signaling for their expression. Comparison of the expression domains of Nodal, Bmp2, Car and Cfc revealed co-expression of Nodal, Cfc and Bmp2, while Car and Nodal only partially overlapped. Ectopic application of BMP2, Nodal, and Car as well as combinations of this signaling molecules to the right lateral plate mesoderm revealed that BMP2 and Car need to synergize in order to specify left identity. We propose a novel model of left-right axis formation, which involves BMP as a positive regulator of Nodal signaling in the chick embryo.

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Persistent ventricle partitioning in the adult zebrafish heart

10.1101/2021.03.16.435658 ◽

2021 ◽

Author(s):

Catherine Pfefferli ◽

Hannah R. Moran ◽

Anastasia Felker ◽

Christian Mosimann ◽

Anna Jazwinska

Keyword(s):

Lateral Plate Mesoderm ◽

Adult Zebrafish ◽

Lateral Plate ◽

Second Heart Field ◽

Heart Field ◽

Left And Right ◽

First Heart Field ◽

The Right ◽

Physical Boundary ◽

Zebrafish Heart

The vertebrate heart integrates cells from the early-differentiating first heart field (FHF) and the later-differentiating second heart field (SHF) emerging from the lateral plate mesoderm. In mammals, this process forms the basis for the development of the left and right ventricle chambers and subsequent chamber septation. The single ventricle-forming zebrafish heart also integrates FHF and SHF lineages during embryogenesis, yet the contributions of these two myocardial lineages to the adult zebrafish heart remain incompletely understood. Here, we characterize the myocardial labeling of FHF descendants in both the developing and adult zebrafish ventricle. Expanding previous findings, late gastrulation-stage labeling using drl-driven CreERT2 recombinase with a myocardium-specific, myl7-controlled loxP reporter results in predominant labeling of FHF-derived outer curvature and the right side of the embryonic ventricle. Raised to adulthood, such lineage-labeled hearts retain broad areas of FHF cardiomyocytes in a region of the ventricle that is positioned at the opposite side to the atrium and encompasses the apex. Our data add to the increasing evidence for a persisting cell-based compartmentalization of the adult zebrafish ventricle even in the absence of any physical boundary.

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Faculty Opinions recommendation of An Hh-dependent pathway in lateral plate mesoderm enables the generation of left/right asymmetry.

Faculty Opinions – Post-Publication Peer Review of the Biomedical Literature ◽

10.3410/f.1199963.665063 ◽

2009 ◽

Author(s):

Jonathan Eggenschwiler

Keyword(s):

Lateral Plate Mesoderm ◽

Lateral Plate ◽

Left Right Asymmetry ◽

Dependent Pathway

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Antagonistic interactions in the zebrafish midline prior to the emergence of asymmetric gene expression are important for left–right patterning

Philosophical Transactions of the Royal Society B Biological Sciences ◽

10.1098/rstb.2015.0402 ◽

2016 ◽

Vol 371 (1710) ◽

pp. 20150402 ◽

Cited By ~ 6

Author(s):

Rebecca D. Burdine ◽

Daniel T. Grimes

Keyword(s):

Gene Expression ◽

Lateral Plate Mesoderm ◽

Internal Organs ◽

Lateral Plate ◽

Left Right Asymmetry ◽

Antagonistic Interactions

Left–right (L-R) asymmetry of the internal organs of vertebrates is presaged by domains of asymmetric gene expression in the lateral plate mesoderm (LPM) during somitogenesis. Ciliated L-R coordinators (LRCs) are critical for biasing the initiation of asymmetrically expressed genes, such as nodal and pitx2 , to the left LPM. Other midline structures, including the notochord and floorplate, are then required to maintain these asymmetries. Here we report an unexpected role for the zebrafish EGF-CFC gene one-eyed pinhead ( oep ) in the midline to promote pitx2 expression in the LPM. Late zygotic oep (LZ oep ) mutants have strongly reduced or absent pitx2 expression in the LPM, but this expression can be rescued to strong levels by restoring oep in midline structures only. Furthermore, removing midline structures from LZ oep embryos can rescue pitx2 expression in the LPM, suggesting the midline is a source of an LPM pitx2 repressor that is itself inhibited by oep . Reducing lefty1 activity in LZ oep embryos mimics removal of the midline, implicating lefty1 in the midline-derived repression. Together, this suggests a model where Oep in the midline functions to overcome a midline-derived repressor, involving lefty1 , to allow for the expression of left side-specific genes in the LPM. This article is part of the themed issue ‘Provocative questions in left–right asymmetry’.

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Primary cilium polarity: morphogenetic consequences.

10.31219/osf.io/zkgsx ◽

2018 ◽

Author(s):

Marco Regolini

Keyword(s):

Primary Cilia ◽

Break Symmetry ◽

Otic Vesicle ◽

Nodal Signaling ◽

Lateral Plate Mesoderm ◽

Cell Orientation ◽

Lateral Plate ◽

Situs Solitus ◽

Left And Right ◽

Breaking Symmetry

In zebrafish inner ear, hair cell orientation in anterior and posterior maculae of the embryonic otic vesicle is different (about 30-40 degrees): this is rather unusual in planar polarity mechanism of action, instead suggests that kinocilia may be rotationally polarized. In mice node, the innermost monociliated cells generate a left-ward fluid flow sensed by the immotile primary cilia of Left peri-nodal cells: the Nodal signaling pathway is then expressed asymmetrically, in the Left lateral plate mesoderm, breaking symmetry in visceral organs (situs solitus); however, Right peri-nodal cells also, if artificially excited by a right-ward flow, break symmetry and activate the Nodal cascade, though inverting visceral organ asymmetry (situs inversus); surprisingly, peri-nodal cells prove to be adept at distinguishing flow directionality. Recently, in the Kupffer vesicle (the zebrafish laterality organ), chiral primary cilia orientation has been described: primary cilia, in the left and right side, are symmetrically oriented, showing a mirror average divergence of about 15-20 degrees from the midline. This finding, taken together with the mirror behavior of mouse perinodal cells and zebrafish hair cells, champions the idea of primary cilia enantiomerism.

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Gut endoderm is involved in the transfer of left-right asymmetry from the node to the lateral plate mesoderm in the mouse embryo

Development ◽

10.1242/dev.079921 ◽

2012 ◽

Vol 139 (13) ◽

pp. 2426-2435 ◽

Cited By ~ 19

Author(s):

R. S. Saund ◽

M. Kanai-Azuma ◽

Y. Kanai ◽

I. Kim ◽

M. T. Lucero ◽

...

Keyword(s):

Mouse Embryo ◽

Lateral Plate Mesoderm ◽

Lateral Plate ◽

Left Right Asymmetry ◽

Gut Endoderm

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Hippo signaling determines the number of venous pole cells that originate from the anterior lateral plate mesoderm in zebrafish

eLife ◽

10.7554/elife.29106 ◽

2018 ◽

Vol 7 ◽

Cited By ~ 5

Author(s):

Hajime Fukui ◽

Takahiro Miyazaki ◽

Renee Wei-Yan Chow ◽

Hiroyuki Ishikawa ◽

Hiroyuki Nakajima ◽

...

Keyword(s):

Cell Number ◽

Bmp Signaling ◽

Hippo Signaling ◽

Lateral Plate Mesoderm ◽

Cardiomyocyte Proliferation ◽

Heart Tube ◽

Lateral Plate ◽

Large Tumor ◽

Developmental Potential ◽

Anterior Lateral Plate Mesoderm

The differentiation of the lateral plate mesoderm cells into heart field cells constitutes a critical step in the development of cardiac tissue and the genesis of functional cardiomyocytes. Hippo signaling controls cardiomyocyte proliferation, but the role of Hippo signaling during early cardiogenesis remains unclear. Here, we show that Hippo signaling regulates atrial cell number by specifying the developmental potential of cells within the anterior lateral plate mesoderm (ALPM), which are incorporated into the venous pole of the heart tube and ultimately into the atrium of the heart. We demonstrate that Hippo signaling acts through large tumor suppressor kinase 1/2 to modulate BMP signaling and the expression of hand2, a key transcription factor that is involved in the differentiation of atrial cardiomyocytes. Collectively, these results demonstrate that Hippo signaling defines venous pole cardiomyocyte number by modulating both the number and the identity of the ALPM cells that will populate the atrium of the heart.

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Hindlimb patterning and mandible development require the Ptx1 gene

Development ◽

10.1242/dev.126.9.1805 ◽

1999 ◽

Vol 126 (9) ◽

pp. 1805-1810 ◽

Cited By ~ 6

Author(s):

C. Lanctot ◽

A. Moreau ◽

M. Chamberland ◽

M.L. Tremblay ◽

J. Drouin

Keyword(s):

Gene Knockout ◽

Proximal Part ◽

Branchial Arch ◽

Dorsal Side ◽

Lateral Plate Mesoderm ◽

Lateral Plate ◽

Similar Time ◽

The Right ◽

Tetrapod Evolution

The restricted expression of the Ptx1 (Pitx1) gene in the posterior half of the lateral plate mesoderm has suggested that it may play a role in specification of posterior structures, in particular, specification of hindlimb identity. Ptx1 is also expressed in the most anterior ectoderm, the stomodeum, and in the first branchial arch. Ptx1 expression overlaps with that of Ptx2 in stomodeum and in posterior left lateral plate mesoderm. We now show that targeted inactivation of the mouse Ptx1 gene severely impairs hindlimb development: the ilium and knee cartilage are absent and the long bones are underdeveloped. Greater reduction of the right femur size in Ptx1 null mice suggests partial compensation by Ptx2 on the left side. The similarly sized tibia and fibula of mutant hindlimbs may be taken to resemble forelimb bones: however, the mutant limb buds appear to have retained their molecular identity as assessed by forelimb expression of Tbx5 and by hindlimb expression of Tbx4, even though Tbx4 expression is decreased in Ptx1 null mice. The hindlimb defects appear to be, at least partly, due to abnormal chondrogenesis. Since the most affected structures derive from the dorsal side of hindlimb buds, the data suggest that Ptx1 is responsible for patterning of these dorsal structures and that as such it may control development of hindlimb-specific features. Ptx1 inactivation also leads to loss of bones derived from the proximal part of the mandibular mesenchyme. The dual role of Ptx1 revealed by the gene knockout may reflect features of the mammalian jaw and hindlimbs that were acquired at a similar time during tetrapod evolution.

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