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Thymopoiesis in mice depends on a Foxn 1-positive thymic epithelial cell lineage

机译:小鼠的胸腺生成取决于Foxn 1阳性胸腺上皮细胞谱系

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The thymus is essential for T-cell development. Here, we focus on the role of the transcription factor Foxn1 in the development and function of thymic epithelial cells (TECs) of the mouse. TECs are of endodermal origin; they initially express Foxn1 and give rise to orthotopic (thoracic) and additional (cervical) thymi. Using Foxn1-directed cytoablation, we show that during embryogenesis, cervical thymi develop a few days after the thoracic lobes, and that bipotent epithelial progenitors of cortical and medullary compartments express Foxn1. We also show that following acute selective near-total ablation during embryogenesis, complete regeneration of TECs does not occur, providing an animal model for human thymic aplasia syndromes. Finally, we address the functional role of Foxn 1-negative TECs that arise postnatally in the mouse. Lineage tracing shows that such Foxn 1-negative TECs are descendants of Foxn1-positive progenitors; furthermore, Foxn 1-directed subacute intoxication of TECs by polyglutamine-containing EGFP proteins indicates that a presumptive Foxn 1-independent lineage does not contribute to thymopoietic function of the adult thymus. Our findings therefore support the notion that Foxni is the essential transcription factor regulating the differentiation of TECs and that its expression marks the major functional lineage of TECs in embryonic ahd adult thymic tissue.
机译:胸腺对于T细胞发育至关重要。在这里,我们专注于小鼠胸腺上皮细胞(TECs)的发育和功能中转录因子Foxn1的作用。 TEC是内皮来源的;他们最初表达Foxn1并引起原位(胸廓)和其他(宫颈)胸腺。使用Foxn1指导的细胞消融,我们显示在胚胎发生过程中,在胸叶后几天发育出胸腺胸腺,并且皮质和髓腔的双能上皮祖细胞表达了Foxn1。我们还表明,在胚胎发生过程中进行急性选择性近全消融后,TECs不会完全再生,从而为人类胸腺发育不良综合征提供了动物模型。最后,我们解决了小鼠中出生后出现的Foxn 1阴性TEC的功能角色。谱系追踪显示,此类Foxn 1阴性TECs是Foxn1阳性祖细胞的后代。此外,含有多聚谷氨酰胺的EGFP蛋白对TECs的Foxn 1引起的亚急性中毒表明,推定的不依赖Foxn 1的谱系对成年胸腺的造血功能没有贡献。因此,我们的发现支持以下观点:Foxni是调节TECs分化的必需转录因子,其表达标志着胚胎ahd成人胸腺组织中TECs的主要功能谱系。

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