| Autor: |
Aalto-Setälä, Laura, Siekkinen, Minna, Lindfors, Nina, Hupa, Leena |
| Zdroj: |
Biomedical Materials & Devices; 20230101, Issue: Preprints p1-11, 11p |
| Abstrakt: |
Although the initial in vitro dissolution of bioactive glasses (BAG) is well characterized, the long-term behaviour of crystallized BAG scaffolds in a continuous fluid flow is incompletely understood. A detailed understanding of the long-term dissolution of scaffolds is vital for predicting their behaviour in clinical applications. Here, we explored the dissolution and reaction mechanisms of partly crystalline and glass–ceramic scaffolds based on the bioactive glasses S53P4 and 45S5 using a continuous flow-through method in Tris-buffer (Tris) and simulated body fluid (SBF) for up to 21 days. Granules of the parent glasses were used as references. The main crystalline phase in both scaffolds was sodium-calcium-silicate. The scaffolds’ dissolution suggested that the sodium-calcium-silicate crystals dissolved incongruently to yield hydrous silica. The silica phase then provided abundant nucleation sites for hydroxyapatite precipitation, resulting in fine-grained crystalline structures. When exposed to Tris, the scaffolds almost completely dissolved within the test period, leaving only highly porous remnant phases. For the 45S5 scaffolds, the calcium phosphate reaction layers that formed on their surfaces effectively slowed the dissolution in SBF. In contrast, this effect was less apparent for the S53P4 specimens. |
| Databáze: |
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