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首页> 外文期刊>Developmental biology >Derivation of pluripotent stem cells from nascent undifferentiated teratoma
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Derivation of pluripotent stem cells from nascent undifferentiated teratoma

机译:从新生未分化的畸胎瘤中衍生多能干细胞

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Teratomas are tumors consisting of components of the three germ layers that differentiate from pluripotent stem cells derived from germ cells. In the normal mouse testis, teratomas rarely form, but a deficiency in Dead-end1 (Dnd1) in mice with a 129/Sv genetic background greatly enhances teratoma formation. Thus, DND1 is crucial for suppression of teratoma development from germ cells. In the Dnd1 mutant testis, nascent teratoma cells emerge at E15.5. To understand the nature of early teratoma cells, we established cell lines in the presence of serum and leukemia inhibitory factor (LIF) from teratoma-forming cells in neonatal Dnd1 mutant testis. These cells, which we designated cultured Dnd1 mutant germ cells (CDGCs), were morphologically similar to embryonic stem cells (ESCs) and could be maintained in the naive pluripotent condition. In addition, the cells expressed pluripotency genes including Oct4, Nanog, and Sox2; differentiated into cells of the three germ layers in culture; and contributed to chimeric mice. The expression levels of pluripotency genes and global transcriptomes in CDGCs as well as these cells' adaption to culture conditions for primed pluripotency suggested that their pluripotent status is intermediate between naive and primed pluripotency. In addition, the teratoma-forming cells in the neonatal testis from which CDGCs were derived also showed gene expression profiles intermediate between naive and primed pluripotency. The results suggested that germ cells in embryonic testes of Dnd1 mutants acquire the intermediate pluripotent status during the course of conversion into teratoma cells.
机译:Teratomas是由三种胚层组分组成的肿瘤,其区分与衍生自生殖细胞的多能干细胞。在正常的小鼠睾丸中,Teratomas很少形成,但死亡终端1(DND1)的缺乏大大提高了畸胎瘤形成。因此,DND1对于抑制生殖细胞的畸胎瘤发育至关重要。在DND1突变体睾丸中,新鲜的畸胎瘤细胞在E15.5中出现。为了了解早期畸胎瘤细胞的性质,我们在新生儿DND1突变体睾丸中从畸胎瘤形成细胞存在血清和白血病抑制因子(LIF)存在的细胞系。我们指定培养的DND1突变生殖细胞(CDGC)的这些细胞在形态上与胚胎干细胞(ESC)相似,并且可以保持在幼稚多能条件下。此外,细胞表达多能性基因,包括OCT4,NANOG和SOX2;分化为培养的三种胚层的细胞;并导致嵌合小鼠。多能基因和全局转录om的CDGCs以及这些细胞对培养条件的表达水平表达对丙种多能性的培养条件表明,它们的多能状态是幼稚和灌注多能性之间的中间体。此外,新生儿睾丸中的畸形形成细胞来自其中CDGC的衍生,也显示出基因表达谱中中间体在幼稚和灌注多能性之间中间体。结果表明,DND1突变体的胚胎睾丸中的生殖细胞在转化过程中的中间多能状态达到畸胎瘤细胞。

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