Cdx2 is required for correct cell fate specification and differentiation of trophectoderm in the mouse blastocyst

Strumpf, D.; Mao, Chai An; Yamanaka, Yojiro; Ralston, Amy; Chawengsaksophak, Kallayanee; Beck, Felix; Rossant, Janet

doi:10.1242/dev.01801

Cited by 991 publications

(1,058 citation statements)

References 36 publications

(62 reference statements)

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“…Another regulatory network involving Oct3/4 and a Cdx gene has been described in mouse embryos during trophectodermal differentiation (Niwa et al, 2005;Strumpf et al, 2005;Tolkunova et al, 2006). In this case, Cdx2 represses the expression of Oct3/4 in trophoblast cells, similar to our case in which Cdx1 represses the expression of the Pou5f1 genes with the transition into gastrulation.…”

Section: Cross-regulation Betweensupporting

confidence: 82%

Negative autoregulation of Oct3/4 through Cdx1 promotes the onset of gastrulation

et al. 2011

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Gastrulation marks the onset of germ layer formation from undifferentiated precursor cells maintained by a network including the Pou5f1 gene, Oct3/4. Negative regulation of the undifferentiated state is a prerequisite for germ layer formation and subsequent development. A novel cross-regulatory network was characterized including the Pou5f1 and Cdx1 genes as part of the signals controlling the onset of gastrulation. Of particular interest was the observation that, preceding gastrulation, the Xenopus Oct3/4 factors, Oct60, Oct25, and Oct91, positively regulate Cdx1 expression through FGF signaling, and during gastrulation the Oct3/4 factors become repressors of Cdx1. Cdx1 negatively regulates the Pou5f1 genes during gastrulation, thus contributing to the repression of the network maintaining the undifferentiated state and promoting the onset of gastrulation. These regulatory interactions suggest that Oct3/4 initiates its own negative autoregulation through Cdx1 up-regulation to begin the repression of pluripotency in preparation for the onset of gastrulation and germ layer differentiation. Developmental Dynamics 240:796-807,

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Section: Cross-regulation Betweensupporting

confidence: 82%

Negative autoregulation of Oct3/4 through Cdx1 promotes the onset of gastrulation

et al. 2011

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“…Molecularly, TE and ICM lineages can be distinguished by the expression patterns of several lineage-specific transcription factors. Cdx2, which is related to Drosophila Caudal, is expressed in the TE of the blastocyst where it is required for promoting TE fate (Beck et al, 1995;Strumpf et al, 2005). Two ICMspecific transcription factors are Oct4, a POU domain protein, and Nanog, a homeodomain protein (Palmieri et al, 1994;Chambers et al, 2003;Mitsui et al, 2003).…”

Section: Development Of the Te Classical Models Of Te Formationmentioning

confidence: 99%

“…Furthermore, Oct4 protein is not detectable in nuclei A gene important for early TE development also has been identified. Cdx2 encodes a Caudal-like transcription factor and is expressed in the TE of the blastocyst (Beck et al, 1995;Strumpf et al, 2005). Cdx2 protein is first detectable in the nuclei of select cells at the eight-cell stage (Niwa et al, 2005) and becomes restricted to outer cells of the late morula (Niwa et al, 2005;Strumpf et al, 2005).…”

Section: Maintenance Of the Icm/te Lineage Restrictionmentioning

confidence: 99%

“…Cdx2 encodes a Caudal-like transcription factor and is expressed in the TE of the blastocyst (Beck et al, 1995;Strumpf et al, 2005). Cdx2 protein is first detectable in the nuclei of select cells at the eight-cell stage (Niwa et al, 2005) and becomes restricted to outer cells of the late morula (Niwa et al, 2005;Strumpf et al, 2005). Cdx2 mutant embryos form a normal-appearing blastocyst, although ICM markers such as Oct4 and Nanog fail to be repressed in the TE , indicating a defect in restriction of the ICM/TE lineage.…”

Section: Maintenance Of the Icm/te Lineage Restrictionmentioning

confidence: 99%

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Cell and molecular regulation of the mouse blastocyst

Yamanaka

Ralston

Stephenson

et al. 2006

Developmental Dynamics

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262

218

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Animals use diverse strategies to specify tissue lineages during development. A common strategy is to partition maternally supplied and localized lineage determinants into progenitor cells. The mouse embryo appears to use a different, more regulative strategy to specify the first three lineages: the epiblast (EPI: future embryo), the trophectoderm (TE: future placenta), and the primitive endoderm (PE: future yolk sac). These lineages are specified during two successive differentiation steps leading to formation of the blastocyst. Here, we review classic and contemporary models of early lineage specification in the mouse, and describe recent efforts to understand the molecular regulation of these events. We describe evidence that trophectoderm differentiation bears resemblance to the process of epithelialization and describe the importance of apical/basal protein complexes in regulating this process. Next, we present a revised model of PE specification, and describe evidence that PE cells in the inner cell mass sort out to occupy their ultimate position on the surface of the EPI. Finally, we describe factors that reinforce these lineages and three distinct stem cell types that can be isolated from them. Together, these mechanisms guide the differentiation of the first lineages of the mouse and thereby set up tissues that will be important for the first steps of embryonic body patterning. Developmental Dynamics 235:2301-2314, 2006.

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“…Ces protéines impliquées dans la polarité cellulaire influencent donc la position de la cellule dans l'embryon, mais cependant ne lui donnent pas une identité définitive. L'identité trophoblastique est fixée entre les stades 32 et 64 cellules (début de la formation du blastocyste) et peut être visualisée grâce à l'expression sélective du facteur de transcription Cdx2 dans les cellules externes [13][14][15][16]. À l'inverse, celle des gènes de pluripotence tels que Oct-4, Sox2 et Nanog est restreinte aux cellules internes du blastocyste.…”

Section: Revuesunclassified

L’embryogenèse précoce des mammifères

Chazaud

2008

Med Sci (Paris)

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Cdx2 is required for correct cell fate specification and differentiation of trophectoderm in the mouse blastocyst

Cited by 991 publications

References 36 publications

Negative autoregulation of Oct3/4 through Cdx1 promotes the onset of gastrulation

Negative autoregulation of Oct3/4 through Cdx1 promotes the onset of gastrulation

Cell and molecular regulation of the mouse blastocyst

L’embryogenèse précoce des mammifères

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