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Organism-Scale Modeling of Early Drosophila Patterning via Bone Morphogenetic Proteins

Advances in image acquisition and informatics technology have led to organism-scale spatiotemporal atlases of gene expression and protein distributions. To maximize the utility of this information for the study of developmental processes, a new generation of mathematical models is needed for discove...

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Bibliographic Details
Published in:Developmental cell 2010-02, Vol.18 (2), p.260-274
Main Authors: Umulis, David M., Shimmi, Osamu, O'Connor, Michael B., Othmer, Hans G.
Format: Article
Language:English
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Summary:Advances in image acquisition and informatics technology have led to organism-scale spatiotemporal atlases of gene expression and protein distributions. To maximize the utility of this information for the study of developmental processes, a new generation of mathematical models is needed for discovery and hypothesis testing. Here, we develop a data-driven, geometrically accurate model of early Drosophila embryonic bone morphogenetic protein (BMP)-mediated patterning. We tested nine different mechanisms for signal transduction with feedback, eight combinations of geometry and gene expression prepatterns, and two scale-invariance mechanisms for their ability to reproduce proper BMP signaling output in wild-type and mutant embryos. We found that a model based on positive feedback of a secreted BMP-binding protein, coupled with the experimentally measured embryo geometry, provides the best agreement with population mean image data. Our results demonstrate that using bioimages to build and optimize a three-dimensional model provides significant insights into mechanisms that guide tissue patterning. [Display omitted] ► Capturing 3D spatiotemporal content of expression data increases model utility ► Embryo geometry shapes signaling; prepatterns compensate in misshapen embryos ► Cell-surface binding proteins compensate for weak ligand/inhibitor/receptor binding ► BMP-mediated patterning is “nearly” scale-invariant
ISSN:1534-5807
1878-1551
DOI:10.1016/j.devcel.2010.01.006