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斑马鱼中形态发生素梯度形成的可视化与定量分析

Visualisation and quantification of morphogen gradient formation in the zebrafish.

作者信息

Harvey Steven A, Smith James C

机构信息

Wellcome Trust/CR-UK Gurdon Institute and Department of Zoology, The University of Cambridge, Cambridge, United Kingdom.

出版信息

PLoS Biol. 2009 May;7(5):e1000101. doi: 10.1371/journal.pbio.1000101. Epub 2009 May 5.

Abstract

During embryonic development, signalling molecules known as morphogens act in a concentration-dependent manner to provide positional information to responding tissues. In the early zebrafish embryo, graded signalling by members of the nodal family induces the formation of mesoderm and endoderm, thereby patterning the embryo into three germ layers. Nodal signalling has also been implicated in the establishment of the dorso-ventral axis of the embryo. Although one can infer the existence of nodal gradients by comparing gene expression patterns in wild-type embryos and embryos in which nodal signalling is diminished or augmented, real understanding can only come from directly observing the gradients. One approach is to determine local ligand concentrations in the embryo, but this is technically challenging, and the presence of inhibitors might cause the effective concentration of a ligand to differ from its actual concentration. We have therefore taken two approaches to visualise a direct response to nodal signalling. In the first, we have used transgenic embryos to study the nuclear accumulation of a Smad2-Venus fusion protein, and in the second we have used bimolecular fluorescence complementation to visualise the formation of a complex between Smad2 and Smad4. This has allowed us to visualise, in living embryos, the formation of a graded distribution of nodal signalling activity. We have quantified the formation of the gradient in time and space, and our results not only confirm that nodal signalling patterns the embryo into three germ layers, but also shed light on its role in patterning the dorso-ventral axis and highlight unexpected complexities of mesodermal patterning.

摘要

在胚胎发育过程中,被称为形态发生素的信号分子以浓度依赖的方式起作用,为响应组织提供位置信息。在斑马鱼早期胚胎中,结节家族成员的梯度信号诱导中胚层和内胚层的形成,从而将胚胎划分为三个胚层。结节信号也与胚胎背腹轴的建立有关。虽然通过比较野生型胚胎和结节信号减弱或增强的胚胎中的基因表达模式可以推断结节梯度的存在,但真正的理解只能来自直接观察这些梯度。一种方法是确定胚胎中的局部配体浓度,但这在技术上具有挑战性,并且抑制剂的存在可能导致配体的有效浓度与其实际浓度不同。因此,我们采用了两种方法来可视化对结节信号的直接反应。第一种方法是使用转基因胚胎研究Smad2-维纳斯融合蛋白的核积累,第二种方法是使用双分子荧光互补来可视化Smad2和Smad4之间复合物的形成。这使我们能够在活胚胎中可视化结节信号活性的梯度分布的形成。我们已经在时间和空间上对梯度的形成进行了量化,我们的结果不仅证实了结节信号将胚胎划分为三个胚层,还揭示了其在背腹轴模式形成中的作用,并突出了中胚层模式形成中意想不到的复杂性。

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