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在生长组织中形态发生源形成的动力学。

Dynamics of morphogen source formation in a growing tissue.

机构信息

Institute of Theoretical Physics and Mark Kac Center for Complex Systems Research, Jagiellonian University, Krakow, Poland.

The Njord Centre, Department of Physics, University of Oslo, Oslo, Norway.

出版信息

PLoS Comput Biol. 2024 Oct 14;20(10):e1012508. doi: 10.1371/journal.pcbi.1012508. eCollection 2024 Oct.

Abstract

A tight regulation of morphogen production is key for morphogen gradient formation and thereby for reproducible and organised organ development. Although many genetic interactions involved in the establishment of morphogen production domains are known, the biophysical mechanisms of morphogen source formation are poorly understood. Here we addressed this by focusing on the morphogen Sonic hedgehog (Shh) in the vertebrate neural tube. Shh is produced by the adjacently located notochord and by the floor plate of the neural tube. Using a data-constrained computational screen, we identified different possible mechanisms by which floor plate formation can occur, only one of which is consistent with experimental data. In this mechanism, the floor plate is established rapidly in response to Shh from the notochord and the dynamics of regulatory interactions within the neural tube. In this process, uniform activators and Shh-dependent repressors are key for establishing the floor plate size. Subsequently, the floor plate becomes insensitive to Shh and increases in size due to tissue growth, leading to scaling of the floor plate with neural tube size. In turn, this results in scaling of the Shh amplitude with tissue growth. Thus, this mechanism ensures a separation of time scales in floor plate formation, so that the floor plate domain becomes growth-dependent after an initial rapid establishment phase. Our study raises the possibility that the time scale separation between specification and growth might be a common strategy for scaling the morphogen gradient amplitude in growing organs. The model that we developed provides a new opportunity for quantitative studies of morphogen source formation in growing tissues.

摘要

形态发生素产生的严格调控是形态发生素梯度形成的关键,也是可重复和有序的器官发育的关键。尽管已知许多参与建立形态发生素产生域的遗传相互作用,但形态发生素源形成的生物物理机制仍知之甚少。在这里,我们通过关注脊椎动物神经管中的形态发生素 Sonic hedgehog(Shh)来解决这个问题。Shh 由相邻的脊索和神经管的基板产生。我们使用数据约束的计算筛选,确定了基板形成可能发生的不同机制,其中只有一种与实验数据一致。在这个机制中,基板快速响应脊索和神经管内的调控相互作用产生的 Shh 而建立。在此过程中,均匀的激活剂和 Shh 依赖性抑制剂对于建立基板大小是关键的。随后,基板对 Shh 不敏感并且由于组织生长而增大,导致基板大小与神经管大小成比例。反过来,这导致 Shh 幅度随组织生长而缩放。因此,该机制确保了基板形成中的时间尺度分离,使得基板域在初始快速建立阶段之后变得依赖于生长。我们的研究提出了这样一种可能性,即特化和生长之间的时间尺度分离可能是生长器官中形态发生素梯度幅度缩放的一种常见策略。我们开发的模型为研究生长组织中形态发生素源形成的定量研究提供了新的机会。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/64af/11501038/7aabb03a6f5a/pcbi.1012508.g001.jpg

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