| Literature DB >> 29257950 |
Theresa Gross-Thebing1, Sargon Yigit1, Jana Pfeiffer1, Michal Reichman-Fried1, Jan Bandemer1, Christian Ruckert2, Christin Rathmer1, Mehdi Goudarzi1, Martin Stehling3, Katsiaryna Tarbashevich1, Jochen Seggewiss2, Erez Raz4.
Abstract
Maintaining cell fate relies on robust mechanisms that prevent the differentiation of specified cells into other cell types. This is especially critical during embryogenesis, when extensive cell proliferation, patterning, and migration events take place. Here we show that vertebrate primordial germ cells (PGCs) are protected from reprogramming into other cell types by the RNA-binding protein Dead end (Dnd). PGCs knocked down for Dnd lose their characteristic morphology and adopt various somatic cell fates. Concomitantly, they gain a gene expression profile reflecting differentiation into cells of different germ layers, in a process that we could direct by expression of specific cell-fate determinants. Importantly, we visualized these events within live zebrafish embryos, which provide temporal information regarding cell reprogramming. Our results shed light on the mechanisms controlling germ cell fate maintenance and are relevant for the formation of teratoma, a tumor class composed of cells from more than one germ layer.Entities:
Keywords: Dead end; PGC; differentiation; germ cell; nanos; pluripotency; reprogramming; teratoma; zebrafish
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Year: 2017 PMID: 29257950 DOI: 10.1016/j.devcel.2017.11.019
Source DB: PubMed Journal: Dev Cell ISSN: 1534-5807 Impact factor: 12.270