| Literature DB >> 33613110 |
Weiyan Yuan1, Zhaokai Yao1, Veeramohan Veerapandian1,2, Xinyan Yang1, Xiaoman Wang1,3, Dingyao Chen1, Linzi Ma1, Chaohui Li1,2, Yi Zheng1, Fang Luo1, Xiao-Yang Zhao1,4,5,6,7.
Abstract
Germline specification is a fundamental step for human reproduction and this biological phenomenon possesses technical challenges to study in vivo as it occurs immediately after blastocyst implantation. The establishment of in vitro human primordial germ cell-like cells (hPGCLCs) induction system allows sophisticated characterization of human primordial germ cells (hPGCs) development. However, the underlying molecular mechanisms of hPGCLC specification are not fully elucidated. Here, we observed particularly high expression of the histone demethylase KDM2B in male fetal germ cells (FGCs) but not in male somatic cells. Besides, KDM2B shared similar expression pattern with hPGC marker genes in hPGCLCs, suggesting an important role of KDM2B in germ cell development. Although deletion of KDM2B had no significant effects on human embryonic stem cell (hESC)'s pluripotency, loss of KDM2B dramatically impaired hPGCLCs differentiation whereas ectopically expressed KDM2B could efficiently rescue such defect, indicating this defect was due to KDM2B's loss in hPGCLC specification. Mechanistically, as revealed by the transcriptional profiling, KDM2B suppressed the expression of somatic genes thus inhibited somatic differentiation during hPGCLC specification. These data collectively indicate that KDM2B is an indispensable epigenetic regulator for hPGCLC specification, shedding lights on how epigenetic regulations orchestrate transcriptional events in hPGC development for future investigation. © The author(s).Entities:
Keywords: KDM2B; epigenetic regulator; fertility; human primordial germ cell-like cells
Mesh:
Substances:
Year: 2021 PMID: 33613110 PMCID: PMC7893587 DOI: 10.7150/ijbs.55873
Source DB: PubMed Journal: Int J Biol Sci ISSN: 1449-2288 Impact factor: 6.580