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截短的成纤维细胞生长因子受体可阻断非洲爪蟾内源性诱导因子的神经诱导作用。

A truncated FGF receptor blocks neural induction by endogenous Xenopus inducers.

作者信息

Launay C, Fromentoux V, Shi D L, Boucaut J C

机构信息

Groupe de Biologie Expérimentale, Différenciation Moléculaire et Cellulaire du Développement, CNRS URA-1135, Université P. et M. Curie, Paris, France.

出版信息

Development. 1996 Mar;122(3):869-80. doi: 10.1242/dev.122.3.869.

Abstract

We have examined the role of fibroblast growth factor (FGF) signalling in neural induction. The approach takes advantage of the fact that both noggin and the dominant negative mutant activin receptor (delta1XAR1) directly induce neural tissues in the absence of dorsal mesoderm. A truncated FGF receptor (XFD) is co-expressed with noggin or delta1XAR1 in both whole embryos and isolated animal caps. We demonstrate that inhibition of FGF signalling prevents neural induction by both factors. Furthermore, neural induction by organizers (the dorsal lip of blastopore and Hensen's node) is also blocked by inhibiting FGF signalling in ectoderm. It has been proposed that the specification of anterior neuroectoderm, including the cement gland, occurs in a sequential manner as gastrulation proceeds. We show that the specification of the most anterior neuroectoderm by noggin may occur before gastrulation and does not require FGF signalling, since both the cement gland marker XCG-1 and the anterior neural marker Otx-2 are normally expressed in ectodermal explants co-injected with noggin and XFD RNAs, but the cement gland cells are poorly differentiated. In contrast, the expression of both genes induced by CSKA.noggin, which is expressed after the mid-blastula transition, is strongly inhibited by the presence of XFD. Therefore the noggin-mediated neural induction that takes place at gastrula stages is abolished in the absence of FGF signalling. Since inhibition of FGF signalling blocks the neuralizing effect of different neural inducers that function through independent mechanisms, we propose that FGF receptor-related-signalling is required for the response to inducing signals of ectodermal cells from gastrula.

摘要

我们研究了成纤维细胞生长因子(FGF)信号通路在神经诱导中的作用。该方法利用了这样一个事实,即头蛋白和显性负性突变激活素受体(delta1XAR1)在没有背侧中胚层的情况下均可直接诱导神经组织。在整个胚胎和分离的动物帽中,截短的FGF受体(XFD)与头蛋白或delta1XAR1共表达。我们证明,抑制FGF信号通路可阻止这两种因子诱导神经。此外,通过抑制外胚层中的FGF信号通路,组织者(胚孔背唇和亨氏结)诱导神经的作用也会被阻断。有人提出,随着原肠胚形成的进行,包括黏液腺在内的前神经外胚层的特化是按顺序发生的。我们表明,头蛋白对最前端神经外胚层的特化可能发生在原肠胚形成之前,且不需要FGF信号通路,因为黏液腺标记物XCG-1和前神经标记物Otx-2通常在与头蛋白和XFD RNA共注射的外胚层外植体中表达,但黏液腺细胞分化较差。相比之下,在囊胚中期转变后表达的CSKA.头蛋白诱导的这两种基因的表达,会因XFD的存在而受到强烈抑制。因此,在没有FGF信号通路的情况下,原肠胚阶段发生的头蛋白介导的神经诱导被消除。由于抑制FGF信号通路会阻断通过独立机制发挥作用的不同神经诱导剂的神经化作用,我们提出FGF受体相关信号通路是外胚层细胞对原肠胚诱导信号作出反应所必需的。

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