Maternal Yes-Associated Protein Participates in Porcine Blastocyst Development via Modulation of Trophectoderm Epithelium Barrier Function

The establishment of a functional trophectoderm (TE) epithelium is an essential prerequisite for blastocyst formation and placentation. Transcription coactivator yes-associated protein (YAP), a downstream effector of the hippo signaling pathway, is required for specification of both the TE and epibl...

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Published in:Cells (Basel, Switzerland) Switzerland), 2019-12, Vol.8 (12), p.1606
Main Authors: Cao, Zubing, Xu, Tengteng, Tong, Xu, Wang, Yiqing, Zhang, Dandan, Gao, Di, Zhang, Ling, Ning, Wei, Qi, Xin, Ma, Yangyang, Yu, Tong, Knott, Jason G, Zhang, Yunhai
Format: Article
Language:English
Subjects:
Blastocysts
Complementation
Cytoplasm
Embryos
Epithelium
Gene expression
Gene regulation
Hogs
Humidity
In vitro fertilization
Kinases
Permeability
Phenotypes
Polyvinyl alcohol
Proteins
Signal transduction
Sperm
Transcription
Trophectoderm
Yes-associated protein
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Summary:The establishment of a functional trophectoderm (TE) epithelium is an essential prerequisite for blastocyst formation and placentation. Transcription coactivator yes-associated protein (YAP), a downstream effector of the hippo signaling pathway, is required for specification of both the TE and epiblast lineages in mice. However, the biological role of YAP in porcine blastocyst development is not known. Here, we report that maternally derived YAP protein is localized to both the cytoplasm and nuclei prior to the morula stage and is then predominantly localized to the TE nuclei in blastocysts. Functionally, maternal knockdown severely impeded blastocyst formation and perturbed the allocation of the first two lineages. The treatment of embryos with verteporfin, a pharmacological inhibitor of YAP, faithfully recapitulated the phenotype observed in deleted embryos. Mechanistically, we found that maternal YAP regulates multiple genes which are important for lineage commitment, tight junction assembly, and fluid accumulation. Consistent with the effects on tight junction gene expression, a permeability assay revealed that paracellular sealing was defective in the trophectoderm epithelium. Lastly, knockdown in a single blastomere at the 2-cell stage revealed that the cellular progeny of the YAP blastomere were sufficient to sustain blastocyst formation via direct complementation of the defective trophectoderm epithelium. In summary, these findings demonstrate that maternal YAP facilitates porcine blastocyst development through transcriptional regulation of key genes that are essential for lineage commitment, tight junction assembly, and fluid accumulation.
ISSN:2073-4409
2073-4409
DOI:10.3390/cells8121606