| Literature DB >> 32032525 |
Fan Yang1, Xin Huang2, Ruge Zang3, Jiayu Chen4, Miguel Fidalgo5, Carlos Sanchez-Priego2, Jihong Yang2, Alexander Caichen2, Fanglin Ma1, Todd Macfarlan6, Huayan Wang7, Shaorong Gao8, Hongwei Zhou2, Jianlong Wang9.
Abstract
Mouse embryonic stem cells (ESCs) sporadically express preimplantation two-cell-stage (2C) transcripts, including MERVL endogenous retrovirus and Zscan4 cluster genes. Such 2C-like cells (2CLCs) can contribute to both embryonic and extraembryonic tissues when reintroduced into early embryos, although the molecular mechanism underlying such an expanded 2CLC potency remains elusive. We examine global nucleosome occupancy and gene expression in 2CLCs and identified miR-344 as the noncoding molecule that positively controls 2CLC potency. We find that activation of endogenous MERVL or miR-344-2 alone is sufficient to induce 2CLCs with activation of 2C genes and an expanded potency. Mechanistically, miR-344 is activated by DUX and post-transcriptionally represses ZMYM2 and its partner LSD1, and ZMYM2 recruits LSD1/HDAC corepressor complex to MERVL LTR for transcriptional repression. Consistently, zygotic depletion of Zmym2 compromises the totipotency-to-pluripotency transition during early development. Our studies establish the previously unappreciated DUX-miR-344-Zmym2/Lsd1 axis that controls MERVL for expanded stem cell potency.Entities:
Keywords: 2C-like cells; Dux; Gata2; Lsd1; MERVL; Zmym2; endogenous retrovirus; miR-344; totipotency
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Year: 2020 PMID: 32032525 PMCID: PMC8074926 DOI: 10.1016/j.stem.2020.01.004
Source DB: PubMed Journal: Cell Stem Cell ISSN: 1875-9777 Impact factor: 24.633