One of the fundamental
challenges in vascular morphogenesis is
to understand how the microstructural morphology of a 3D matrix can
provide the spatial cues to organize the endothelial cells (ECs) into
specific vascular structures. Colloidal gels can provide well-controlled
distinct morphological matrices because these gels are formed by the
aggregation of particles. By altering the aggregation mode, the spatial
organization of the particles can be controlled to yield different
microstructural morphology. To demonstrate this, colloidal aggregates
and gels were developed by electrostatic interaction-mediated aggregation
of cationic polyurethane (PU) colloidal particles by using low molecular
weight electrolyte and polyelectrolyte to develop microstructurally
different colloidal gels without altering their bulk elasticity. Compact
dense colloidal aggregates with constricted voids were developed via
electrolyte-mediated aggregation, whereas stranded branched networks
with interconnected voids were formed via polyelectrolyte-mediated
bridging interactions. Results show that the microstructure of aggregated
colloids and gels can regulate EC organizations. Within endothelial
matrices, ECs track the microstructure of particulate phase to interconnect
with stranded colloidal network but cluster around compact colloidal
aggregate. Similarly, in colloidal gels, ECs formed capillary-like
structures by interconnecting along the stranded networks with enhanced
cell–matrix interactions and increased cell extension but aggregated
within the constricted voids of compact dense gel with enhanced cell–cell
interaction. Both morphometric analysis and expression of EC markers
corroborated the cell organizations in these gels. Using these colloidal
gels, we demonstrated the role of 3D microstructural morphology as
an important regulator for spatial guidance of ECs and simultaneously
established the significance of colloidal gels as 3D matrix to regulate
cellular morphogenesis.
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