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评价 BMP 介导的斑马鱼囊胚胚胎 3D 数学模型中的模式形成。

Evaluation of BMP-mediated patterning in a 3D mathematical model of the zebrafish blastula embryo.

机构信息

Weldon School of Biomedical Engineering, Purdue University, West Lafayette, USA.

Department of Agricultural and Biological Engineering, Purdue University, West Lafayette, USA.

出版信息

J Math Biol. 2020 Jan;80(1-2):505-520. doi: 10.1007/s00285-019-01449-x. Epub 2019 Nov 26.

Abstract

Bone Morphogenetic Proteins (BMPs) play an important role in dorsal-ventral (DV) patterning of the early zebrafish embryo. BMP signaling is regulated by a network of extracellular and intracellular factors that impact the range and signaling of BMP ligands. Recent advances in understanding the mechanism of pattern formation support a source-sink mechanism, however it is not clear how the source-sink mechanism shapes patterns in 3D, nor how sensitive the pattern is to biophysical rates and boundary conditions along both the anteroposterior (AP) and DV axes of the embryo. We propose a new three-dimensional growing Partial Differential Equation (PDE)-based model to simulate the BMP patterning process during the blastula stage. This model provides a starting point to elucidate how different mechanisms and components work together in 3D to create and maintain the BMP gradient in the embryo. We also show how the 3D model fits the BMP signaling gradient data at multiple time points along both axes. Furthermore, sensitivity analysis of the model suggests that the spatiotemporal patterns of Chordin and BMP ligand gene expression are dominant drivers of shape in 3D and more work is needed to quantify the spatiotemporal profiles of gene and protein expression to further refine the models.

摘要

骨形态发生蛋白(BMPs)在斑马鱼早期胚胎的背腹(DV)模式形成中起着重要作用。BMP 信号受细胞外和细胞内因素网络的调节,这些因素影响 BMP 配体的范围和信号。对模式形成机制的最新研究进展支持源汇机制,但尚不清楚源汇机制如何在 3D 中形成图案,以及图案对胚胎前后(AP)和 DV 轴上的生物物理速率和边界条件的敏感性如何。我们提出了一种新的基于三维生长偏微分方程(PDE)的模型来模拟囊胚期 BMP 模式形成过程。该模型为阐明不同机制和组件如何在 3D 中协同工作以在胚胎中创建和维持 BMP 梯度提供了一个起点。我们还展示了 3D 模型如何拟合沿两个轴的多个时间点的 BMP 信号梯度数据。此外,模型的敏感性分析表明,Chordin 和 BMP 配体基因表达的时空模式是 3D 形状的主要驱动因素,需要进一步研究基因和蛋白质表达的时空分布,以进一步完善模型。

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