Abstract
In mouse blastocysts segregation of the inner cell mass (ICM) and the trophectoderm (TE) is regulated by the mutually antagonistic effects of the transcription factors Oct4 and Cdx2 expressed in the ICM and TE, respectively. In contrast, in other species such as bovine and human, Oct4 is not restricted to the ICM and continues to be expressed in the Cdx2-positive TE. A recent comparative study of the bovine and mouse Oct4 promoters revealed that additional mechanisms might act in conjunction with Cdx2 to downregulate Oct4 expression in the mouse TE lineage. For instance, the mouse Oct4 distal enhancer contains an AP-2γ (Tcfap2c) binding motif that is absent in the bovine and human Oct4 distal enhancer. Nonetheless, the functional relevance of Tcfap2c in Oct4 repression during mouse preimplantation development was not tested. To elucidate the role of Tcfap2c in Oct4 expression an RNA interference approach was utilized. Depletion of Tcfap2c triggered a decrease in Oct4 expression at the 8-cell and morula stage. Remarkably, at the blastocyst stage depletion of Tcfap2c and/or its family member Tcfap2a had no effect on Oct4 repression. To test whether Tcfap2c interacts with Oct4 to positively regulate Oct4 expression, chromatin immunoprecipitation and in situ co-immunoprecipitation analyses were performed. These experiments revealed Tcfap2c and Oct4 binding were enriched at the Oct4 distal enhancer in embryonic stem (ES) cells, but were rapidly lost during differentiation into trophoblast-like cells when Oct4 became repressed. Moreover, Tcfap2c and Oct4 interactions were detected at the morula stage, but were lost during blastocyst formation. In summary, these data demonstrate that Tcfap2c is not required for Oct4 silencing in mouse blastocysts, but may be necessary for the maintenance of Oct4 expression during the 8 cell-to-morula transition. These findings support the notion Cdx2 is the predominant negative regulator of Oct4 expression during blastocyst formation in mice.
Highlights
During mouse preimplantation development dynamic expression patterns of the transcription factors (TFs) Oct4, Nanog, Sox2, Tead4, Gata3, and Cdx2 affect cell fate, and specify the first two lineages, the inner cell mass (ICM) and trophectoderm (TE) at the blastocyst stage [1,2,3]
Our analysis reveals that an Oct4Tcfap2c interaction exists during mouse preimplantation development and that Tcfap2c may act as a co-activator of Oct4 transcription by interacting with Oct4 protein at the conserved region 4 (CR4) region
Recent work in a bovine model demonstrated that Cdx2 was not sufficient to downregulate Oct4 expression in the TE lineage of blastocysts [12]
Summary
During mouse preimplantation development dynamic expression patterns of the transcription factors (TFs) Oct, Nanog, Sox, Tead, Gata, and Cdx affect cell fate, and specify the first two lineages, the inner cell mass (ICM) and trophectoderm (TE) at the blastocyst stage [1,2,3]. Of these TFs, Oct (encoded by Pou5f1) is expressed uniformly in early cleavage stage embryos from oocyte to morula, and becomes confined to the ICM after blastocyst formation [4,5]. The expression of a bovine Oct4-GFP transgene was not restricted to the ICM in mouse blastocysts suggesting that Tcfap2c binding to the Oct promoter is required for repression of Oct in the TE of blastocysts
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