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SoxB1 转录因子通过抑制 Wnt 信号下游的多个事件来限制组织者基因的表达。

SoxB1 transcription factors restrict organizer gene expression by repressing multiple events downstream of Wnt signalling.

机构信息

Institute of Genetics, Queen's Medical Centre, University of Nottingham, Nottingham, NG7 2UH, UK.

出版信息

Development. 2010 Aug;137(16):2671-81. doi: 10.1242/dev.054130. Epub 2010 Jul 7.

Abstract

Formation of the organizer is one of the most central patterning events in vertebrate development. Organizer-derived signals are responsible for establishing the CNS and patterning the dorsal ventral axis. The mechanisms promoting organizer formation are known to involve cooperation between Nodal and Wnt signalling. However, the organizer forms in a very restricted region, suggesting the presence of mechanisms that repress its formation. Here, we show in zebrafish that the transcription factor Sox3 represses multiple steps in the signalling events that lead to organizer formation. Although beta-catenin, Bozozok and Squint are known to play major roles in establishing the dorsal organizer in vertebrate embryos, overexpression of any of these is insufficient to induce robust expression of markers of the organizer in ectopic positions in the animal pole, where Sox3 is strongly expressed. We show that a dominant-negative nuclear localisation mutant of Sox3 can cause ectopic expression of organizer genes via a mechanism that activates all of these earlier factors, resulting in later axis duplication including major bifurcations of the CNS. We also find that the related SoxB1 factor, Sox19b, can act redundantly with Sox3 in these effects. It therefore seems that the broad expression of these SoxB1 genes throughout the early epiblast and their subsequent restriction to the ectoderm is a primary regulator of when and where the organizer forms.

摘要

组织者的形成是脊椎动物发育中最核心的模式形成事件之一。组织者衍生的信号负责建立中枢神经系统并对背腹轴进行模式化。已知促进组织者形成的机制涉及 Nodal 和 Wnt 信号之间的合作。然而,组织者仅在非常有限的区域形成,这表明存在抑制其形成的机制。在这里,我们在斑马鱼中表明,转录因子 Sox3 抑制导致组织者形成的信号事件中的多个步骤。尽管β-连环蛋白、Bozozok 和 Squint 已知在脊椎动物胚胎中建立背侧组织者中发挥主要作用,但过表达这些蛋白中的任何一种都不足以在动物极的异位位置诱导组织者标记物的强烈表达,而 Sox3 在动物极中强烈表达。我们表明,Sox3 的显性负核定位突变体可以通过激活所有这些早期因子的机制引起异位表达组织者基因,导致后期轴重复,包括中枢神经系统的主要分叉。我们还发现相关的 SoxB1 因子 Sox19b 可以在这些效应中与 Sox3 冗余发挥作用。因此,这些 SoxB1 基因在早期外胚层中的广泛表达及其随后在外胚层中的限制似乎是调节组织者何时以及何地形成的主要调节剂。

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