Derivation of new pluripotent stem cells from human extended pluripotent stem cells with formative features and trophectoderm potential

诱导多能干细胞 生物 胚胎干细胞 细胞生物学 胚状体 干细胞 胚芽层 内胚层 细胞分化 外胚层 遗传学 胚胎 胚胎发生 基因
作者
Pinmou Zhu,Bohang Zhang,Ruiqi Sun,Jiachen Wang,Liu Zhao-de,Xiaorui Liu,Min Yan,Yiqiang Cui,Jiahao Sha,Yan Yuan
出处
期刊:Cell Proliferation [Wiley]
卷期号:56 (11) 被引量:1
标识
DOI:10.1111/cpr.13480
摘要

Previous studies have demonstrated the existence of intermediate stem cells, which have been successfully obtained from human naive pluripotent stem cells (PSCs) and peri-implantation embryos. However, it is not known whether human extended pluripotent stem cells (hEPSCs) can be directly induced into intermediate stem cells. Moreover, the ability of extra-embryonic lineage differentiation in intermediate stem cells has not been verified. In this issue, we transformed hEPSCs into a kind of novel intermediate pluripotent stem cell resembling embryonic days 8-9 (E8-E9) epiblasts and proved its feature of formative epiblasts. We engineered hEPSCs from primed hPSCs under N2B27-LCDM (N2B27 plus Lif, CHIR, DiH and MiH) conditions. Then, we added Activin A, FGF and XAV939 to modulate signalling pathways related to early humans' embryogenesis. We performed RNA-seq and CUT&Tag analysis to compare with AF9-hPSCs from different pluripotency stages of hPSCs. Trophectoderm (TE), primordial germ cells-like cells (PGCLC) and endoderm, mesoderm, and neural ectoderm induction were conducted by specific small molecules and proteins. AF9-hPSCs transcription resembled that of E8-E9 peri-implantation epiblasts. Signalling pathway responsiveness and histone methylation further revealed their formative pluripotency. Additionally, AF9-hPSCs responded directly to primordial germ cells (PGCs) specification and three germ layer differentiation signals in vitro. Moreover, AF9-hPSCs could differentiate into the TE lineage. Therefore, AF9-hPSCs represented an E8-E9 formative pluripotency state between naïve and primed pluripotency, opening new avenues for studying human pluripotency development during embryogenesis.
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