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Nodal-related signaling during zebrafish embryogenesis.

机译:斑马鱼胚胎发生过程中与节点有关的信号传导。

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摘要

I describe the Nodal-related family of signaling molecules that have been implicated in mesodermal and neural patterning, and left-right asymmetry, in mouse, frog, and chicken embryos. My studies focus on the isolation and characterization of one zebrafish nodal orthologue, squint (sqt). The early expression pattern of sqt begins dorsally in both the embryonic and extraembryonic tissue. Overexpression of sqt in whole embryos expands or duplicates axial cell fates. Furthermore, Sqt overexpression, exclusively in the extraembryonic yolk syncytial layer (YSL), causes broadened or duplicated dorsal mesodermal marker gene expression in the overlying blastoderm. Additionally, the inductive properties of Sqt are compared to another fish Nodal-related ligand, Cyc. Sqt is an efficient inducer of organizer-type mesendodermal markers, while Cyc induces both mesodermal and neural fates.; Additionally, using cyc;sqt double mutants, I describe the process of neural posteriorization/transformation, which is essential for anterior-posterior (A-P) regionalization of the vertebrate central nervous system (CNS). I explore the molecular identity of the influence present in lateral mesodermal precursors that are maintained in Nodal-deficient embryos, which exerts a posteriorizing effect on anterior neural tissue. Employing a variety of genetic situations that vary the extent of mesendodermal precursor formation, I find that expression of wnt8, a previously implicated neural transformer, is necessary for posteriorization. Moreover, specific inhibition of wnt8 abrogates posteriorization in vivo. My findings provide strong evidence that Wnt8 acts in lateral mesendodermal precursors, independent of Sqt and Cyc, as an essential component of the neural transformation process.; Lastly, I define cis-acting regulatory regions within the sqt upstream region that drive GFP reporter gene expression in the endogenous sqt expression domains in transient transgenic assays. A −9 kb segment upstream of the start ATG drives GFP throughout the extraembryonic yolk syncytial layer (YSL), a region of the embryo shown to induce overlying blastomeres to adopt a mesendodermal fate, and in deep and superficial cells of the marginal zone. Using standard deletion analyses, we narrowed the region mostly responsible for YSL and deep marginal blastodermal expression to a 1 kb fragment (−1.3 to −0.3 kb) upstream of the translational start site.
机译:我描述了与节点相关的信号分子家族,这些信号分子与小鼠,青蛙和鸡胚的中胚层和神经模式以及左右不对称有关。我的研究集中于分离和表征一种斑马鱼 nodal 直系同源物, squint sqt )。 sqt 的早期表达模式在胚胎和胚外组织中都从背面开始。整个胚胎中 sqt 的过度表达会扩大或复制轴向细胞命运。此外,仅在胚外卵黄合胞体层(YSL)中的Sqt过表达会导致上胚层中背中胚层标记基因的表达变宽或重复。此外,将Sqt的诱导特性与另一条与鱼类Nodal相关的配体Cyc进行了比较。 Sqt是组织型中胚层标记的有效诱导剂,而Cyc诱导中胚层和神经命运。此外,使用 cyc ; sqt 双重突变体,我描述了神经后部化/转化的过程,这对于脊椎动物中枢神经系统的前后(AP)区域化至关重要(CNS)。我探讨了在节点缺失的胚胎中维持的外侧中胚层前体中存在的影响的分子同一性,这对前神经组织产生后效应。我发现,利用多种遗传条件改变中胚层前体形成的程度,我发现表达 wnt8 (一种先前牵涉的神经变形因子)对于后继化是必要的。此外,对 wnt8 的特异性抑制消除了体内的恶化。神经转化过程。最后,我定义了 sqt 上游区域中的 cis 作用调节区域,该区域在瞬时转基因的内源性 sqt 表达域中驱动GFP报告基因表达。分析。起始ATG上游的-9 kb片段在整个胚外卵黄合胞体层(YSL)中驱动GFP,这是胚的一个区域,可诱导上卵裂球采取中胚层命运,并位于边缘区的深层和浅层细胞中。使用标准的缺失分析,我们将主要负责YSL和深缘胚泡表达的区域缩小到了翻译起始位点上游的1 kb片段(-1.3至-0.3 kb)。

著录项

  • 作者

    Erter, Caroline Elizabeth.;

  • 作者单位

    Vanderbilt University.;

  • 授予单位 Vanderbilt University.;
  • 学科 Biology Cell.; Biology Genetics.
  • 学位 Ph.D.
  • 年度 2000
  • 页码 p.5664
  • 总页数 195
  • 原文格式 PDF
  • 正文语种 eng
  • 中图分类 细胞生物学;
  • 关键词

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