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Bmp梯度对Msx基因的调控对于神经嵴特化至关重要。

Regulation of Msx genes by a Bmp gradient is essential for neural crest specification.

作者信息

Tribulo Celeste, Aybar Manuel J, Nguyen Vu H, Mullins Mary C, Mayor Roberto

机构信息

Millennium Nucleus in Developmental Biology, Facultad de Ciencias, Universidad de Chile, Casilla 653, Santiago, Chile.

出版信息

Development. 2003 Dec;130(26):6441-52. doi: 10.1242/dev.00878. Epub 2003 Nov 19.

Abstract

There is evidence in Xenopus and zebrafish embryos that the neural crest/neural folds are specified at the border of the neural plate by a precise threshold concentration of a Bmp gradient. In order to understand the molecular mechanism by which a gradient of Bmp is able to specify the neural crest, we analyzed how the expression of Bmp targets, the Msx genes, is regulated and the role that Msx genes has in neural crest specification. As Msx genes are directly downstream of Bmp, we analyzed Msx gene expression after experimental modification in the level of Bmp activity by grafting a bead soaked with noggin into Xenopus embryos, by expressing in the ectoderm a dominant-negative Bmp4 or Bmp receptor in Xenopus and zebrafish embryos, and also through Bmp pathway component mutants in the zebrafish. All the results show that a reduction in the level of Bmp activity leads to an increase in the expression of Msx genes in the neural plate border. Interestingly, by reaching different levels of Bmp activity in animal cap ectoderm, we show that a specific concentration of Bmp induces msx1 expression to a level similar to that required to induce neural crest. Our results indicate that an intermediate level of Bmp activity specifies the expression of Msx genes in the neural fold region. In addition, we have analyzed the role that msx1 plays on neural crest specification. As msx1 has a role in dorsoventral pattering, we have carried out conditional gain- and loss-of-function experiments using different msx1 constructs fused to a glucocorticoid receptor element to avoid an early effect of this factor. We show that msx1 expression is able to induce all other early neural crest markers tested (snail, slug, foxd3) at the time of neural crest specification. Furthermore, the expression of a dominant negative of Msx genes leads to the inhibition of all the neural crest markers analyzed. It has been previously shown that snail is one of the earliest genes acting in the neural crest genetic cascade. In order to study the hierarchical relationship between msx1 and snail/slug we performed several rescue experiments using dominant negatives for these genes. The rescuing activity by snail and slug on neural crest development of the msx1 dominant negative, together with the inability of msx1 to rescue the dominant negatives of slug and snail strongly argue that msx1 is upstream of snail and slug in the genetic cascade that specifies the neural crest in the ectoderm. We propose a model where a gradient of Bmp activity specifies the expression of Msx genes in the neural folds, and that this expression is essential for the early specification of the neural crest.

摘要

在非洲爪蟾和斑马鱼胚胎中,有证据表明神经嵴/神经褶是由Bmp梯度的精确阈值浓度在神经板边界处特化形成的。为了理解Bmp梯度能够特化神经嵴的分子机制,我们分析了Bmp靶基因Msx基因的表达是如何被调控的,以及Msx基因在神经嵴特化中所起的作用。由于Msx基因直接位于Bmp的下游,我们通过将浸泡有头蛋白的珠子移植到非洲爪蟾胚胎中、在非洲爪蟾和斑马鱼胚胎的外胚层中表达显性负性Bmp4或Bmp受体,以及通过斑马鱼中的Bmp信号通路组分突变体,在实验性改变Bmp活性水平后分析Msx基因的表达。所有结果表明,Bmp活性水平的降低会导致神经板边界处Msx基因的表达增加。有趣的是,通过在动物帽外胚层中达到不同水平的Bmp活性,我们发现特定浓度的Bmp诱导msx1表达至与诱导神经嵴所需水平相似的程度。我们的结果表明,Bmp活性的中间水平特化了神经褶区域中Msx基因的表达。此外,我们分析了msx1在神经嵴特化中所起的作用。由于msx1在背腹模式形成中起作用,我们使用与糖皮质激素受体元件融合的不同msx1构建体进行了条件性功能获得和功能缺失实验,以避免该因子的早期影响。我们发现,在神经嵴特化时,msx1的表达能够诱导所有其他测试的早期神经嵴标记物(蜗牛蛋白、蛞蝓蛋白、叉头框D3)的表达。此外,Msx基因显性负性的表达导致所有分析的神经嵴标记物的抑制。先前已经表明,蜗牛蛋白是在神经嵴遗传级联反应中最早起作用的基因之一。为了研究msx1与蜗牛蛋白/蛞蝓蛋白之间的层级关系,我们使用这些基因的显性负性进行了多项拯救实验。蜗牛蛋白和蛞蝓蛋白对msx1显性负性的神经嵴发育的拯救活性,以及msx1无法拯救蛞蝓蛋白和蜗牛蛋白的显性负性,有力地表明在特化外胚层中神经嵴的遗传级联反应中,msx1位于蜗牛蛋白和蛞蝓蛋白的上游。我们提出了一个模型,其中Bmp活性梯度特化了神经褶中Msx基因的表达,并且这种表达对于神经嵴的早期特化至关重要。

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