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通过 N-钙黏蛋白触发的活性肌动蛋白驱动的迁移形成内胚层原基。

Endodermal germ-layer formation through active actin-driven migration triggered by N-cadherin.

机构信息

CNRS UMR8197, F-75005 Paris, France.

INSERM U1024, F-75005 Paris, France.

出版信息

Proc Natl Acad Sci U S A. 2017 Sep 19;114(38):10143-10148. doi: 10.1073/pnas.1708116114. Epub 2017 Sep 5.

Abstract

Germ-layer formation during gastrulation is both a fundamental step of development and a paradigm for tissue formation and remodeling. However, the cellular and molecular basis of germ-layer segregation is poorly understood, mostly because of the lack of direct in vivo observations. We used mosaic zebrafish embryos to investigate the formation of the endoderm. High-resolution live imaging and functional analyses revealed that endodermal cells reach their characteristic innermost position through an active, oriented, and actin-based migration dependent on Rac1, which contrasts with the previously proposed differential adhesion cell sorting. Rather than being attracted to their destination, the yolk syncytial layer, cells appear to migrate away from their neighbors. This migration depends on N-cadherin that, when imposed in ectodermal cells, is sufficient to trigger their internalization without affecting their fate. Overall, these results lead to a model of germ-layer formation in which, upon N-cadherin expression, endodermal cells actively migrate away from their epiblastic neighbors to reach their internal position, revealing cell-contact avoidance as an unexplored mechanism driving germ-layer formation.

摘要

原肠胚形成过程中胚层的形成既是发育的基本步骤,也是组织形成和重塑的典范。然而,胚层分离的细胞和分子基础还知之甚少,主要是因为缺乏直接的体内观察。我们使用嵌合体斑马鱼胚胎来研究内胚层的形成。高分辨率的活体成像和功能分析表明,内胚层细胞通过依赖 Rac1 的活跃、定向和肌动蛋白为基础的迁移到达其特征的最内层位置,这与之前提出的差异粘附细胞分选形成鲜明对比。细胞似乎不是被吸引到它们的目的地——卵黄合胞层,而是从它们的邻居处迁移出去。这种迁移依赖于 N-钙黏蛋白,当它在外胚层细胞中表达时,足以引发它们的内化,而不影响它们的命运。总的来说,这些结果提出了一个胚层形成的模型,即在 N-钙黏蛋白表达后,内胚层细胞主动地从它们的外胚层邻居处迁移出去,到达它们的内部位置,揭示了细胞接触回避是驱动胚层形成的一个未被探索的机制。

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