Nucleolar stress regulation of endometrial receptivity in mouse models and human cell lines

Embryo implantation is essential to the successful establishment of pregnancy. A previous study has demonstrated that actinomycin D (ActD) could initiate the activation of mouse delayed implantation. However, the mechanism underlying this activation remains to be elucidated. A low dose of ActD is an...

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Veröffentlicht in:Cell death & disease 2019-11, Vol.10 (11), p.831-16, Article 831
Hauptverfasser: Hu, Wei, Liang, Yu-Xiang, Luo, Jia-Mei, Gu, Xiao-Wei, Chen, Zi-Cong, Fu, Tao, Zhu, Yu-Yuan, Lin, Shuai, Diao, Hong-Lu, Jia, Bo, Yang, Zeng-Ming
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Sprache:eng
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Zusammenfassung:Embryo implantation is essential to the successful establishment of pregnancy. A previous study has demonstrated that actinomycin D (ActD) could initiate the activation of mouse delayed implantation. However, the mechanism underlying this activation remains to be elucidated. A low dose of ActD is an inducer of nucleolar stress. This study was to examine whether nucleolar stress is involved in embryo implantation. We showed that nucleolar stress occurred when delayed implantation was activated by ActD in mice. ActD treatment also stimulated the Lif-STAT3 pathway. During early pregnancy, nucleolar stress was detected in the luminal epithelial cells during the receptive phase. Blastocyst-derived lactate could induce nucleolar stress in cultured luminal epithelial cells. The inhibition of nucleophosmin1 (NPM1), which was a marker of nucleolar stress, compromised uterine receptivity and decreased the implantation rates in pregnant mice. To translate these mouse data into humans, we examined nucleolar stress in human endometrium. Our data demonstrated that ActD-induced nucleolar stress had positive effects on the embryo attachment by upregulating IL32 expression in non-receptive epithelial cells rather than receptive epithelial cells. Our data should be the first to demonstrate that nucleolar stress is present during early pregnancy and is able to induce embryo implantation in both mice and humans.
ISSN:2041-4889
2041-4889
DOI:10.1038/s41419-019-2071-6