A critical
step in tissue engineering is the design and synthesis of 3D biocompatible
matrices (scaffolds) to support and guide the proliferation of cells
and tissue growth. The most existing techniques rely on the processing
of scaffolds under controlled conditions and then implanting them in vivo, with questions related to biocompatibility and
implantation that are still challenging. As an alternative, it was
proposed to assemble the scaffolds in loco through
the self-organization of colloidal particles mediated by cells. To
overcome the difficulty to test experimentally all the relevant parameters,
we propose the use of large-scale numerical simulation as a tool to
reach useful predictive information and to interpret experimental
results. Thus, in this study, we combine experiments, particle-based
simulations, and mean-field calculations to show that, in general,
the size of the self-assembled scaffold scales with the cell-to-particle
ratio. However, we have found an optimal value of this ratio, for
which the size of the scaffold is maximal when the cell–cell
adhesion is suppressed. These results suggest that the size and structure
of the self-assembled scaffolds may be designed by tuning the adhesion
between cells in the colloidal suspension.
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