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首页> 外文期刊>Blood: The Journal of the American Society of Hematology >A critical role for endoglin in the emergence of blood during embryonic development
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A critical role for endoglin in the emergence of blood during embryonic development

机译:内皮糖蛋白在胚胎发育过程中血液出现中的关键作用

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摘要

Much remains unknown about the signals that induce early mesoderm to initiate hematopoietic differentiation. Here, we show that endoglin (Eng), a receptor for the TGFβ superfamily, identifies all cells with hematopoietic fate in the early embryo. These arise in an Eng +Flk1 + mesodermal precursor population at embryonic day 7.5 (E7.5), a cell fraction also endowed with endothelial potential. In Eng-knockout embryos, hematopoietic colony activity and numbers of CD71 + Ter119 + erythroid progenitors were severely reduced. This coincided with severely reduced expression of embryonic globin and key bone morphogenic protein (BMP) target genes, including the hematopoietic regulators Scl, Gata1, Gata2, and Msx-1. To interrogate molecular pathways active in the earliest hematopoietic progenitors, we applied transcriptional profiling to sorted cells from E7.5 embryos. Eng +Flk-1 + progenitors coexpressed TGFβ and BMP receptors and target genes. Furthermore, Eng +Flk-1 + cells presented high levels of phospho-SMAD1/5, indicating active TGFβ and/or BMP signaling. Remarkably, under hematopoietic serum-free culture conditions, hematopoietic outgrowth of Eng-expressing cells was dependent on the TGFβ superfamily ligands BMP4, BMP2, or TGF-β1. These data demonstrate that the E +F + fraction at E7.5 represents mesodermal cells competent to respond to TGFβ1, BMP4, or BMP2, shaping their hematopoietic development, and that Eng acts as a critical regulator in this process by modulating TGF/BMP signaling.
机译:关于诱导早期中胚层启动造血分化的信号,目前还不清楚。在这里,我们显示内皮糖蛋白(Eng)是TGFβ超家族的受体,可以识别早期胚胎中所有具有造血命运的细胞。这些发生在胚胎第7.5天(E7.5)的Eng + Flk1 +中胚层前体种群中,这也是一种具有内皮潜能的细胞组分。在Eng基因敲除胚胎中,造血集落活动和CD71 + Ter119 +红系祖细胞的数量大大降低。这与胚胎球蛋白和关键骨形态发生蛋白(BMP)目标基因(包括造血调节因子Scl,Gata1,Gata2和Msx-1)的表达严重降低相吻合。为了询问最早的造血祖细胞中活跃的分子途径,我们将转录图谱应用于来自E7.5胚胎的分类细胞。 Eng + Flk-1 +祖细胞共表达TGFβ和BMP受体以及靶基因。此外,Eng + Flk-1 +细胞表现出高水平的磷酸-SMAD1 / 5,表明有活性的TGFβ和/或BMP信号传导。值得注意的是,在造血无血清培养条件下,表达Eng的细胞的造血生长依赖于TGFβ超家族配体BMP4,BMP2或TGF-β1。这些数据表明E7.5处的E + F +分数代表中胚层细胞能够对TGFβ1,BMP4或BMP2作出反应,从而影响其造血发育,并且Eng在此过程中通过调节TGF / BMP信号传导起着关键的调节作用。 。

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