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Geometrical versus Random β-TCP Scaffolds: Exploring the Effects on Schwann Cell Growth and Behavior

Title: Geometrical versus Random β-TCP Scaffolds: Exploring the Effects on Schwann Cell Growth and Behavior.
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Name(s): Sweet, Lauren, author
Kang, Yunqing, author
Czisch, Christopher, author
Witek, Lukasz, author
Shi, Yang, author
Smay, Jim, author
Plant, Giles W., author
Yang, Yunzhi, author
Guda, Teja, editor
Type of Resource: text
Genre: Article
Date Issued: 2015-10-07
Summary: Numerous studies have demonstrated that Schwann cells (SCs) play a role in nerve regeneration; however, their role in innervating a bioceramic scaffold for potential application in bone regeneration is still unknown. Here we report the cell growth and functional behavior of SCs on β-tricalcium phosphate (β-TCP) scaffolds arranged in 3D printed-lattice (P-β- TCP) and randomly-porous, template-casted (N-β-TCP) structures. Our results indicate that SCs proliferated well and expressed the phenotypic markers p75LNGFR and the S100-β subunit of SCs as well as displayed growth morphology on both scaffolds, but SCs showed spindle-shaped morphology with a significant degree of SCs alignment on the P-β-TCP scaffolds, seen to a lesser degree in the N-β-TCP scaffold. The gene expressions of nerve growth factor (β-ngf), neutrophin–3 (nt–3), platelet-derived growth factor (pdgf-bb), and vascular endothelial growth factor (vegf-a) were higher at day 7 than at day 14. While no significant differences in protein secretion were measured between these last two time points, the scaffolds promoted the protein secretion at day 3 compared to that on the cell culture plates. These results together imply that the β-TCP scaffolds can support SC cell growth and that the 3D-printed scaffold appeared to significantly promote the alignment of SCs along the struts. Further studies are needed to investigate the early and late stage relationship between gene expression and protein secretion of SCs on the scaffolds with refined characteristics, thus better exploring the potential of SCs to support vascularization and innervation in synthetic bone grafts.
Identifier: 10.1371/journal.pone.0139820 (doi), http://dx.plos.org/10.1371/journal.pone.0139820 (uri), FAUIR000025 (IID)
Persistent Link to This Record: http://purl.flvc.org/fau/fd/FAUIR000025
Use and Reproduction: publisher
Owner Institution: FAU
Is Part Of: PLOS ONE.
1932-6203