Functionalization of Microstructured Open-Porous Bioceramic Scaffolds with Human Fetal Bone Cells

生物陶瓷 脚手架 化学 生物相容性 生物医学工程 活力测定 骨细胞 纳米技术 材料科学 细胞 细胞生物学 生物化学 医学 生物 有机化学
作者
Franziska Krauss Juillerat,Françoise Borcard,Davide Staedler,Corinne Scaletta,Lee Ann Applegate,Horacio Comas,Ludwig J. Gauckler,Sandrine Gerber-Lemaire,Lucienne Juillerat-Jeanneret,Urs T. Gonzenbach
出处
期刊:Bioconjugate Chemistry [American Chemical Society]
卷期号:23 (11): 2278-2290 被引量:11
标识
DOI:10.1021/bc300407x
摘要

Bone substitute materials allowing trans-scaffold migration and in-scaffold survival of human bone-derived cells are mandatory for development of cell-engineered permanent implants to repair bone defects. In this study, we evaluated the influence on human bone-derived cells of the material composition and microstructure of foam scaffolds of calcium aluminate. The scaffolds were prepared using a direct foaming method allowing wide-range tailoring of the microstructure for pore size and pore openings. Human fetal osteoblasts (osteo-progenitors) attached to the scaffolds, migrated across the entire bioceramic depending on the scaffold pore size, colonized, and survived in the porous material for at least 6 weeks. The long-term biocompatibility of the scaffold material for human bone-derived cells was evidenced by in-scaffold determination of cell metabolic activity using a modified MTT assay, a repeated WST-1 assay, and scanning electron microscopy. Finally, we demonstrated that the osteo-progenitors can be covalently bound to the scaffolds using biocompatible click chemistry, thus enhancing the rapid adhesion of the cells to the scaffolds. Therefore, the different microstructures of the foams influenced the migratory potential of the cells, but not cell viability. Scaffolds allow covalent biocompatible chemical binding of the cells to the materials, either localized or widespread integration of the scaffolds for cell-engineered implants.
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