During the early stages of gastrulation in Drosophila embryo, the epithelial cells composing the single tissue layer of the egg undergo large strains and displacements. These movements have been usually modelled by decomposing the total deformation gradient in an (imposed or strain/stress dependent) active part and a passive response. Although the influence of the chemical and genetic activity in the mechanical response of the cell has been experimentally observed, the effects of the mechanical deformation on the latter have been far less studied, and much less modelled. Here, we propose a model that couples morphogen transport and the cell mechanics during embryogenesis. A diffusion-reaction equation is introduced as an additional mechanical regulator of morphogenesis. Consequently, the active deformations are not directly imposed in the analytical formulation, but they rather depend on the morphogen concentration, which is introduced as a new variable. In this study, we show that strain patterns similar to those observed during biological experiments can be reproduced by properly combining the two phenomena. In addition, we use a novel technique to parameterise the embryo geometry by solving two Laplace problems with specific boundary conditions. We apply the method to two morphogenetic movements: ventral furrow invagination and germ band extension. The matching between our results and the observed experimental deformations confirms that diffusion-reaction of morphogens can actually be controlling large morphogenetic movements.
Published on 01/01/2011
DOI: 10.1080/10255842.2011.616944
Licence: CC BY-NC-SA license
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