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卷曲蛋白7在神经嵴诱导过程中介导经典Wnt信号通路。

Frizzled7 mediates canonical Wnt signaling in neural crest induction.

作者信息

Abu-Elmagd Muhammad, Garcia-Morales Carla, Wheeler Grant N

机构信息

School of Biological Sciences, University of East Anglia, Norwich NR4 7TJ, UK.

出版信息

Dev Biol. 2006 Oct 1;298(1):285-98. doi: 10.1016/j.ydbio.2006.06.037. Epub 2006 Jun 27.

Abstract

The neural crest is a multipotent cell population that migrates from the dorsal edge of the neural tube to various parts of the embryo where it differentiates into a remarkable variety of different cell types. Initial induction of neural crest is mediated by a combination of BMP, Wnt, FGF, Retinoic acid and Notch/Delta signaling. The two-signal model for neural crest induction suggests that BMP signaling induces the competence to become neural crest. The second signal involves Wnt acting through the canonical pathway and leads to expression of neural crest markers such as slug. Wnt signals from the neural plate, non-neural ectoderm and paraxial mesoderm have all been suggested to play a role in neural crest induction. We show that Xenopus frizzled7 (Xfz7) is expressed in the dorsal ectoderm including early neural crest progenitors and is a key mediator of the Wnt inductive signal. We demonstrate that Xfz7 expression is induced in response to a BMP antagonist, noggin, and that Xfz7 can induce neural crest specific genes in noggin-treated ectodermal explants (animal caps). Morpholino-mediated or dominant negative inhibition of Xfz7 inhibits Wnt induced Xslug expression in the animal cap assay and in the whole embryo leading to a loss of neural crest derived pigment cells. Full-length Xfz7 rescues the morpholino-induced phenotype, as does activated beta-catenin, suggesting that Xfz7 is signaling through the canonical pathway. We therefore demonstrate that Xfz7 is regulated by BMP antagonism and is required for neural crest induction by Wnt in the developing vertebrate embryo.

摘要

神经嵴是一种多能细胞群体,它从神经管的背侧边缘迁移至胚胎的各个部位,并在那里分化为多种不同类型的细胞。神经嵴的初始诱导是由骨形态发生蛋白(BMP)、Wnt、成纤维细胞生长因子(FGF)、视黄酸和Notch/Delta信号通路共同介导的。神经嵴诱导的双信号模型表明,BMP信号通路诱导细胞具备成为神经嵴的能力。第二个信号涉及通过经典途径发挥作用的Wnt,并导致神经嵴标志物如slug的表达。来自神经板、非神经外胚层和轴旁中胚层的Wnt信号均被认为在神经嵴诱导过程中发挥作用。我们发现非洲爪蟾卷曲蛋白7(Xfz7)在包括早期神经嵴祖细胞在内的背侧外胚层中表达,并且是Wnt诱导信号的关键介导因子。我们证明,Xfz7的表达是对BMP拮抗剂头蛋白(noggin)的响应而被诱导的,并且Xfz7能够在经noggin处理的外胚层组织块(动物帽)中诱导神经嵴特异性基因的表达。在动物帽实验和整个胚胎中,吗啉代介导的或显性负性抑制Xfz7会抑制Wnt诱导的Xslug表达,导致神经嵴衍生的色素细胞缺失。全长Xfz7能够挽救吗啉代诱导的表型,激活的β-连环蛋白也能如此,这表明Xfz7是通过经典途径进行信号传导的。因此,我们证明Xfz7受BMP拮抗作用的调节,并且是发育中的脊椎动物胚胎中Wnt诱导神经嵴形成所必需的。

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