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Foxn1 maintains thymic epithelial cells to support T-cell development via mcm2 in zebrafish

机译:Foxn1维持胸腺上皮细胞通过斑马鱼中的mcm2支持T细胞发育

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摘要

The thymus is mainly comprised of thymic epithelial cells (TECs), which form the unique thymic epithelial microenvironment essential for intrathymic T-cell development. Foxn1, a member of the forkhead transcription factor family, is required for establishing a functional thymic rudiment. However, the molecular mechanisms underlying the function of Foxn1 are still largely unclear. Here, we show that Foxn1 functions in thymus development through Mcm2 in the zebrafish. We demonstrate that, in foxn1 knockdown embryos, the thymic rudiment is reduced and T-cell development is impaired. Genome-wide expression profiling shows that a number of genes, including some known thymopoiesis genes, are dysregulated during the initiation of the thymus primordium and immigration of T-cell progenitors to the thymus. Functional and epistatic studies show that mcm2 and cdca7 are downstream of Foxn1, and mcm2 is a direct target gene of Foxn1 in TECs. Finally, we find that the thymus defects in foxn1 and mcm2 morphants might be attributed to reduced cell proliferation rather than apoptosis. Our results reveal that the foxn1-mcm2 axis plays a central role in the genetic regulatory network controlling thymus development in zebrafish.
机译:胸腺主要由胸腺上皮细胞(TECs)组成,形成了胸腺内T细胞发育必不可少的独特胸腺上皮微环境。 Foxn1是叉头转录因子家族的成员,对于建立功能性胸腺残基是必需的。但是,Foxn1功能的分子机制仍然不清楚。在这里,我们显示Foxn1通过斑马鱼中的Mcm2在胸腺发育中起作用。我们证明,在foxn1击倒的胚胎中,胸腺残基减少,T细胞发育受损。全基因组表达谱分析表明,在胸腺原基启动和T细胞祖细胞迁移到胸腺过程中,许多基因(包括一些已知的胸腺生成基因)失调。功能和上位性研究表明,mcm2和cdca7位于Foxn1的下游,而mcm2是TEC中Foxn1的直接靶基因。最后,我们发现foxn1和mcm2 morphant中的胸腺缺陷可能归因于细胞增殖减少而不是凋亡。我们的结果表明,foxn1-mcm2轴在控制斑马鱼胸腺发育的遗传调控网络中起着核心作用。

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