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Geometry driven fluid dynamics and cytocompatibility of 3D printed TPMS bone scaffolds

Authors
Lawal, Oluwarotimi
 Arafat, Abul
 Gupta, Abhishek
 Arjunan, Arun
 Baroutaji, Ahmad
 Adebayo, David
 Robinson, John
 Appiah, Martin
 Wanniarachchi, Chameekara
 Singh, Manpreet
 Ashwood, Neil
 Butcher, Kate
 Vance, Aaron
Editors
Other contributors
Affiliation
Additive Manufacturing of Functional Materials Research Group, School of Pharmacy and Life Sciences, Research Institute in Healthcare Science, Faculty of Science and Engineering, University of Wolverhampton
Epub Date
Issue Date
2026-02-20
Submitted date
Subjects
triply periodic minimal surface
 additive manufacturing
 computational fluid dynamics
 bone tissue engineering
 biocompatibility
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Abstract
Triply Periodic Minimal Surfaces (TPMS) can mimic the complex architecture of trabecular bone while facilitating controlled fluid transport and cellular colonisation. This study integrates computational fluid dynamics (CFD), laser powder bed fusion (L-PBF), and in vitro cell assays to evaluate the structure-function relationship of four Ti6Al4V TPMS scaffolds informed by Schwartz Primitive (SSC), Lidinoid (LSC), Gyroid (GSC), and Diamond (DSC) featuring 60% porosity. CFD simulations at inlet velocities ranging from 0.001 to 0.01 m/s revealed architecture-specific permeability ranging from 1.89 × 10−9 m2 (DSC) to 4.29 × 10−9 m2 (SSC) at low flow rates, with a consistent inverse relationship between flow velocity and permeability (R2 > 0.99). Mid-plane velocity fields highlighted scaffold-specific vortex formations and nutrient mixing dynamics, with SSC exhibiting pronounced swirling zones, promoting fluid homogenisation. In vitro cytocompatibility assessed via MTT assay on U-2OS osteosarcoma cells showed >85% viability across all geometries after 24 h and >88% after 7 days, with the LSC scaffold exhibiting the most consistent viability (101.8 ± 7.7%) and SSC showing significant improvement over time (87.2 ± 3.3% to 121.4 ± 6.2%, p < 0.015). Immunofluorescence imaging confirmed cell attachment across all architectures, with GSC and DSC supporting uniform cytoskeletal spreading and enhanced cell-pore integration. Degradation studies in PBS at 37 °C showed that DSC scaffolds underwent the highest mass loss (4.42% at day 7), correlating with their larger surface area, while pH monitoring suggested early ion release followed by buffering over time. These results demonstrate that scaffold topology significantly impacts permeability, degradation, and biological performance with SSC and GSC emerging as promising 3D printed microenvironments.
Citation
Lawal, O., Arafat, A., Gupta, A., Arjunan, A., Baroutaji, A., Adebayo, D., Robinson, J., Appiah, M., Wanniarachchi, C., Singh, M., Ashwood, N., Butcher, K., Vance, A. (2026) Geometry driven fluid dynamics and cytocompatibility of 3D printed TPMS bone scaffolds. Medicine in Novel Technology and Devices, 30, 100436.
Publisher
Elsevier
Journal
Medicine in Novel Technology and Devices
Research Unit
URI
https://wlv.openrepository.com/handle/2436/626242
DOI
10.1016/j.medntd.2026.100436
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PubMed Central ID
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https://doi.org/10.1016/j.medntd.2026.100436
Type
Journal article
Language
en
Description
© 2026 The Authors. Published by Elsevier. This is an open access article available under a Creative Commons licence. The published version can be accessed at the following link on the publisher’s website: https://doi.org/10.1016/j.medntd.2026.100436
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ISSN
2590-0935
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