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一个同源域反馈回路为 Shh 形态发生素梯度在腹侧神经模式形成过程中的阶跃函数解释提供了基础。

A homeodomain feedback circuit underlies step-function interpretation of a Shh morphogen gradient during ventral neural patterning.

机构信息

Department of Cell and Molecular Biology, Karolinska Institutet, Stockholm, Sweden.

出版信息

Development. 2010 Dec;137(23):4051-60. doi: 10.1242/dev.054288.

Abstract

The deployment of morphogen gradients is a core strategy to establish cell diversity in developing tissues, but little is known about how small differences in the concentration of extracellular signals are translated into robust patterning output in responding cells. We have examined the activity of homeodomain proteins, which are presumed to operate downstream of graded Shh signaling in neural patterning, and describe a feedback circuit between the Shh pathway and homeodomain transcription factors that establishes non-graded regulation of Shh signaling activity. Nkx2 proteins intrinsically strengthen Shh responses in a feed-forward amplification and are required for ventral floor plate and p3 progenitor fates. Conversely, Pax6 has an opposing function to antagonize Shh signaling, which provides intrinsic resistance to Shh responses and is important to constrain the inductive capacity of the Shh gradient over time. Our data further suggest that patterning of floor plate cells and p3 progenitors is gated by a temporal switch in neuronal potential, rather than by different Shh concentrations. These data establish that dynamic, non-graded changes in responding cells are essential for Shh morphogen interpretation, and provide a rationale to explain mechanistically the phenomenon of cellular memory of morphogen exposure.

摘要

形态发生梯度的部署是在发育组织中建立细胞多样性的核心策略,但对于细胞如何将细胞外信号浓度的微小差异转化为响应细胞中强大的模式输出,我们知之甚少。我们研究了同源域蛋白的活性,这些蛋白被认为在神经模式形成中位于梯度 Shh 信号的下游,并描述了 Shh 途径和同源域转录因子之间的反馈回路,该回路建立了 Shh 信号活性的非分级调节。Nkx2 蛋白内在地增强了 Shh 反应的前馈放大作用,对于腹侧基板和 p3 祖细胞命运是必需的。相反,Pax6 具有拮抗 Shh 信号的功能,为 Shh 反应提供内在抗性,对于随着时间推移限制 Shh 梯度的诱导能力非常重要。我们的数据进一步表明,基板细胞和 p3 祖细胞的模式形成由神经元潜力的时间转换控制,而不是由不同的 Shh 浓度控制。这些数据表明,响应细胞中动态的、非分级的变化对于 Shh 形态发生因子的解释是必不可少的,并为从机制上解释形态发生因子暴露的细胞记忆现象提供了依据。

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