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Computational model of mesenchymal migration in 3D under chemotaxis

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DataCite Commons2020-09-04 更新2024-07-27 收录
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https://tandf.figshare.com/articles/dataset/Computational_model_of_mesenchymal_migration_in_3D_under_chemotaxis/3458936
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Cell chemotaxis is an important characteristic of cellular migration, which takes part in crucial aspects of life and development. In this work, we propose a novel <i>in silico</i> model of mesenchymal 3D migration with competing protrusions under a chemotactic gradient. Based on recent experimental observations, we identify three main stages that can regulate mesenchymal chemotaxis: chemosensing, dendritic protrusion dynamics and cell–matrix interactions. Therefore, each of these features is considered as a different module of the main regulatory computational algorithm. The numerical model was particularized for the case of fibroblast chemotaxis under a PDGF-bb gradient. Fibroblasts migration was simulated embedded in two different 3D matrices – collagen and fibrin – and under several PDGF-bb concentrations. Validation of the model results was provided through qualitative and quantitative comparison with <i>in vitro</i> studies. Our numerical predictions of cell trajectories and speeds were within the measured <i>in vitro</i> ranges in both collagen and fibrin matrices. Although in fibrin, the migration speed of fibroblasts is very low, because fibrin is a stiffer and more entangling matrix. Testing PDGF-bb concentrations, we noticed that an increment of this factor produces a speed increment. At 1 ng mL<sup>−1</sup> a speed peak is reached after which the migration speed diminishes again. Moreover, we observed that fibrin exerts a dampening behavior on migration, significantly affecting the migration efficiency.
提供机构:
Taylor & Francis
创建时间:
2016-06-23
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