首页> 外文期刊>Biology Open >Foxa2 mediates critical functions of prechordal plate in patterning and morphogenesis and is cell autonomously required for early ventral endoderm morphogenesis
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Foxa2 mediates critical functions of prechordal plate in patterning and morphogenesis and is cell autonomously required for early ventral endoderm morphogenesis

机译:Foxa2介导前庭板在模式和形态发生中的关键功能,是早期腹侧内胚层形态发生的自主细胞

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Axial mesendoderm is comprised of prechordal plate and notochord. Lack of a suitable Cre driver has hampered the ability to genetically dissect the requirement for each of these components, or genes expressed within them, to anterior patterning. Here, we have utilized Isl1-Cre to investigate roles of the winged helix transcription factor Foxa2 specifically in prechordal plate and ventral endoderm. Foxa2loxP/loxP ; Isl1-Cre mutants died at 13.5 dpc, exhibiting aberrations in anterior neural tube and forebrain patterning, and in ventral foregut morphogenesis and cardiac fusion. Molecular analysis of Foxa2loxP/loxP ; Isl1-Cre mutants indicated that Foxa2 is required in Isl1 lineages for expression of notochord and dorsal foregut endoderm markers, Shh. Brachyury , and Hlxb9 . Our results support a requirement for Foxa2 in prechordal plate for notochord morphogenesis, axial patterning, and patterning of dorsal foregut endoderm. Loss of Foxa2 in ventral endoderm resulted in reduced expression of Sox17, Gata4, and ZO proteins, accounting at least in part for observed lack of foregut fusion, cardia bifida, and increased apoptosis of ventral endoderm.
机译:轴向中胚层由前庭板和脊索组成。缺乏合适的Cre驱动因子已经阻碍了将这些成分或其中表达的基因从遗传学角度分解为前模式的能力。在这里,我们已经利用Isl1-Cre来研究翅螺旋转录因子Foxa2在先兆板和腹内胚层中的作用。 Foxa2loxP / loxP; Isl1-Cre突变体在13.5 dpc死亡,在前神经管和前脑模式以及腹侧前肠形态发生和心脏融合中表现出畸变。 Foxa2loxP / loxP的分子分析Isl1-Cre突变体表明在Isl1谱系中Foxa2是表达脊索和背前肠内胚层标记Shh所必需的。 Brachyury和Hlxb9。我们的结果支持脊索前板中Foxa2对脊索形态发生,轴向构图和背前肠内胚层构图的要求。腹内胚层中Foxa2的缺失导致Sox17,Gata4和ZO蛋白的表达降低,至少部分原因是观察到的前肠融合、,门裂和腹内胚层凋亡的增加。

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