TRPM8 channel inhibitor-encapsulated hydrogel as a tunable surface for bone tissue engineering

A major limitation in the bio-medical sector is the availability of materials suitable for bone tissue engineering using stem cells and methodology converting the stochastic biological events towards definitive as well as efficient bio-mineralization. We show that osteoblasts and Bone Marrow-derived...

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Veröffentlicht in:Scientific reports 2021-02, Vol.11 (1), p.3730-3730, Article 3730
Hauptverfasser: Acharya, Tusar Kanta, Kumar, Satish, Tiwari, Nikhil, Ghosh, Arijit, Tiwari, Ankit, Pal, Subhashis, Majhi, Rakesh Kumar, Kumar, Ashutosh, Das, Rashmita, Singh, Abhishek, Maji, Pradip K., Chattopadhyay, Naibedya, Goswami, Luna, Goswami, Chandan
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Sprache:eng
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Zusammenfassung:A major limitation in the bio-medical sector is the availability of materials suitable for bone tissue engineering using stem cells and methodology converting the stochastic biological events towards definitive as well as efficient bio-mineralization. We show that osteoblasts and Bone Marrow-derived Mesenchymal Stem Cell Pools (BM-MSCP) express TRPM8, a Ca 2+ -ion channel critical for bone-mineralization. TRPM8 inhibition triggers up-regulation of key osteogenesis factors; and increases mineralization by osteoblasts. We utilized CMT:HEMA, a carbohydrate polymer-based hydrogel that has nanofiber-like structure suitable for optimum delivery of TRPM8-specific activators or inhibitors. This hydrogel is ideal for proper adhesion, growth, and differentiation of osteoblast cell lines, primary osteoblasts, and BM-MSCP. CMT:HEMA coated with AMTB (TRPM8 inhibitor) induces differentiation of BM-MSCP into osteoblasts and subsequent mineralization in a dose-dependent manner. Prolonged and optimum inhibition of TRPM8 by AMTB released from the gels results in upregulation of osteogenic markers. We propose that AMTB-coated CMT:HEMA can be used as a tunable surface for bone tissue engineering. These findings may have broad implications in different bio-medical sectors.
ISSN:2045-2322
2045-2322
DOI:10.1038/s41598-021-81041-w