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Evolution of the mammalian embryonic pluripotency gene regulatory network

机译:哺乳动物胚胎多能性基因调控网络的演变

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摘要

Embryonic pluripotency in the mouse is established and maintained by a gene-regulatory network under the control of a core set of transcription factors that include octamer-binding protein 4 (Oct4; official name POU domain, class 5, transcription factor 1, Pou5f1), sex-determining region Y (SRY)-box containing gene 2 (Sox2), and homeobox protein Nanog. Although this network is largely conserved in eutherian mammals, very little information is available regarding its evolutionary conservation in other vertebrates. We have compared the embryonic pluripotency networks in mouse and chick by means of expression analysis in the pregastrulation chicken embryo, genomic comparisons, and functional assays of pluripotency-related regulatory elements in ES cells and blastocysts. We find that multiple components of the network are either novel to mammals or have acquired novel expression domains in early developmental stages of the mouse. We also find that the downstream action of the mouse core pluripotency factors is mediated largely by genomic sequence elements nonconserved with chick. In the case of Sox2 and Fgf4, we find that elements driving expression in embryonic pluripotent cells have evolved by a small number of nucleotide changes that create novel binding sites for core factors. Our results show that the network in charge of embryonic pluripotency is an evolutionary novelty of mammals that is related to the comparatively extended period during which mammalian embryonic cells need to be maintained in an undetermined state before engaging in early differentiation events.
机译:小鼠的胚胎多能性是通过基因调控网络在一组核心转录因子的控制下建立和维持的,这些转录因子包括八聚体结合蛋白4(Oct4;正式名称POU域,第5类,转录因子1,Pou5f1),包含基因2(Sox2)和同源盒蛋白Nanog的性别决定区Y(SRY)-box。尽管该网络在自然界的哺乳动物中基本上是保存的,但是关于其在其他脊椎动物中的进化保存的信息很少。我们已经通过在妊娠前鸡胚中的表达分析,基因组比较以及ES细胞和胚泡中多能性相关调控元件的功能测定,比较了小鼠和小鸡的胚胎多能性网络。我们发现网络的多个组件要么是哺乳动物的新手,要么在小鼠的早期发育阶段获得了新的表达域。我们还发现,小鼠核心多能性因子的下游作用主要由与小鸡不保守的基因组序列元件介导。在Sox2和Fgf4的情况下,我们发现驱动胚胎多潜能细胞表达的元件已经通过少量核苷酸改变而进化,这些核苷酸改变为核心因子创造了新的结合位点。我们的结果表明,负责胚胎多能性的网络是哺乳动物的进化新奇,这与哺乳动物胚胎细胞在参与早期分化事件之前需要维持在不确定状态的相对延长时期有关。

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