Pitx2 regulates gonad morphogenesis

Rodríguez-León, Joaquín; Esteban, Concepción Rodrı́guez; Martí, Mercè; Santiago-Josefat, Belen; Dubova, Ilir; Rubiralta, Xavier; Belmonte, Juan Carlos Izpisúa

doi:10.1073/pnas.0804904105

Cited by 62 publications

(63 citation statements)

References 48 publications

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“…Nodal establishes a large expression domain in the left lateral plate mesoderm (LPM) and induces the expression of Pitx2, a homeobox gene of the bicoid class (7). Pitx2 determines morphological L-R asymmetries in most organ systems (9-12) via modulation of cell-cell adhesion, cell morphology, extracellular matrix composition, spindle orientation, and cell proliferation (13)(14)(15).…”

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confidence: 99%

A right-sided pathway involving FGF8 / Snai1 controls asymmetric development of the proepicardium in the chick embryo

Schlueter

Brand

2009

Proc. Natl. Acad. Sci. U.S.A.

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The proepicardium (PE) is a transient structure that forms at the venous pole of the embryonic vertebrate heart. This cardiac progenitor cell population gives rise to the epicardium, coronary vasculature, and fibroblasts. In the chicken embryo, the PE displays left-right (L-R) asymmetry and develops only on the right side, while on the left only a vestigial PE is formed, which subsequently gets lost by apoptosis. In this study, we analyzed how the L-R asymmetry pathway affects PE formation. Experimental manipulation of left-side determinants such as Shh, Nodal, and Cfc as well as forced expression of Pitx2 had no effect on the sidedness of PE development. In contrast, inhibition of early-acting regulators of L-R axis formation such as H ؉ /K ؉ -ATPase or primitive streak apoptosis affected the sidedness of PE development. Experimental interference with the right-side determinants Fgf8 or Snai1 prevented PE formation, whereas ectopic left-sided expression of Fgf8 or Snai1 resulted in bilateral PE development. These data provide novel insight into the molecular control of asymmetric morphogenesis suggesting that also the right side harbors an instructive signaling pathway that is involved in the control of PE development. This pathway might be of general relevance for setting up L-R asymmetries at the venous pole of the heart. left-right asymmetry ͉ Tbx18 ͉ Pitx2 ͉ venous pole morphogenesis T he left-right (L-R) axis controls asymmetric organogenesis in vertebrates (1-3). In lower chordates, Xenopus, and chick, breaking of the initial bilateral body symmetry involves the asymmetric distribution of ion channels and transporters, resulting in the development of membrane potential differences between the left and right body side, which may drive an asymmetric transport of small molecules through gap junctions (4, 5). In mammals, Xenopus, and zebrafish, ciliated cells in the organizer generate a fluid flow to the left that transports L-R determinants (6). In mammals, this nodal flow is believed to be the sole mechanism by which L-R asymmetry is initiated (7). In the chicken embryo, asymmetric gene expression in Hensen's node of gastrula stage embryos is an important intermediate step of establishing L-R asymmetry (2). Shh, for example, is asymmetrically expressed on the left side of Hensen's node and induces Nodal expression in a small left-sided domain adjacent to Hensen's node (8). Nodal establishes a large expression domain in the left lateral plate mesoderm (LPM) and induces the expression of Pitx2, a homeobox gene of the bicoid class (7). Pitx2 determines morphological L-R asymmetries in most organ systems (9-12) via modulation of cell-cell adhesion, cell morphology, extracellular matrix composition, spindle orientation, and cell proliferation (13-15).A right-sided regulatory cascade of gene expression is also initiated in Hensen's node including Bmp4 that induces asymmetric expression of Fgf18 and Fgf8 on the right side (16-18). It is believed that the right side does not initiate its own sidespecific morphogene...

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confidence: 99%

A right-sided pathway involving FGF8 / Snai1 controls asymmetric development of the proepicardium in the chick embryo

Schlueter

Brand

2009

Proc. Natl. Acad. Sci. U.S.A.

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“…Therefore, the higher prevalence of GCOC in the right ovary may be further elucidated by understanding the asymmetrical development of the gonads in the chicken. Regarding EOC, there is no evidence supporting a role for gonadal asymmetry in the prevalence of the disease in the right or left ovary (84); interestingly, however, paired-like homeodomain transcription factor 2 (PITX2), which is overexpressed in EOC, is also a key player in the asymmetric development of chicken female gonads (85,86). The expression of PITX2 in the left gonad promotes proliferation of the left cortex, leading to the asymmetric development of the gonads (85,87).…”

Section: Incessant Ovulation Hypothesismentioning

confidence: 99%

Advantages of the avian model for human ovarian cancer

Bernardo

Þorsteinsdóttir

Mummery

2015

Molecular and Clinical Oncology

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Abstract. Ovarian cancer (OC) is the most lethal gynecological cancer. Early detection of OC is crucial for providing efficient treatment, whereas high mortality rates correlate with late detection of OC, when the tumor has already metastasized to other organs. The most prevalent type of OC is epithelial OC (EOC). Models that have been used to study EOC include the fruit fly, mouse and laying hen, in addition to human EOC cells in 3D culture in vitro. These models have helped in the elucidation of the genetic component of this disease and the development of drug therapies. However, the histological origin of EOC and early markers of the disease remain largely unknown. In this study, we aimed to review the relative value of each of the different models in EOC and their contributions to understanding this disease. It was concluded that the spontaneous occurrence of EOC in the adult hen, the prolific ovulation, the similarity of metastatic progression with that in humans and the advantages of using the chicken embryo for modelling the development of the reproductive system, renders the hen particularly suitable for studying the early development of EOC. Further investigation of this avian model may contribute to a better understanding of EOC, improve clinical insight and ultimately contribute to decreasing its mortality rates among humans.

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“…There is no further development of the right gonad and this leads to the formation of vestigial structures (Carlon and Stahl, 1985) or complete regression (Romanoff, 1960) at the adult stage. The molecular mechanism underlying asymmetrical development and the degeneration of the right ovary in female birds relies on PITX2 (Guioli and Lovell-Badge, 2007;Ishimaru et al, 2008;Rodriguez-Leon et al, 2008). Guioli and LovellBadge (2007) demonstrated that misexpression of Pitx2 in the right gonad using transfection with the RCAS retroviral vector is sufficient not only to induce symmetric development of the gonads but also to rescue the degeneration of the right ovary.…”

Section: Gonadogenesis and Left-right Asymmetry Of Embryonic Gonadsmentioning

confidence: 99%

“…Pitx2-knockout mice have abnormalities of internal organ asymmetry (Lin et al, 1999;Lu et al, 1999). Recently, Pitx2 was reported to play a role in embryonic gonad asymmetry in both sexes (Guioli and LovellBadge, 2007;Ishimaru et al, 2008;Rodriguez-Leon et al, 2008).…”

Section: Introductionmentioning

confidence: 99%

Left-Right Asymmetry in Chicken Embryonic Gonads

Intarapat

Stern

2014

J. Poult. Sci.

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Avian embryos have reproductive organs with unique characteristics. In female, the gonads develop asymmetrically: the left gonad generates a functional ovary, whereas the right gonad and associated embryonic oviduct (Müllerian duct) regress. In males, however, both left and right gonads develop into testes. Recent evidence, however, revealed that left-right asymmetry can be detected in both sexes. Even male embryos have a greater number of germ cells in the left gonad. Moreover, pluripotency-associated markers, as well as SSEA1, the surface antigen that is strongly expressed in chick embryonic stem cells, also show asymmetric expression in both sexes both in germ cells and in stromal cells of the gonad. This review provides an update of the state of the field.

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Pitx2 regulates gonad morphogenesis

Cited by 62 publications

References 48 publications

A right-sided pathway involving FGF8 / Snai1 controls asymmetric development of the proepicardium in the chick embryo

A right-sided pathway involving FGF8 / Snai1 controls asymmetric development of the proepicardium in the chick embryo

Advantages of the avian model for human ovarian cancer

Left-Right Asymmetry in Chicken Embryonic Gonads

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