Thermosensitive chitosan-based hydrogel: A vehicle for overcoming the limitations of nose-to-brain cell therapy

Cell therapy is a promising strategy for treating neurological pathologies but requires invasive methods to bypass the blood–brain barrier restrictions. The nose-to-brain route has been presented as a direct and less invasive alternative to access the brain. The primary limitations of this route are...

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Veröffentlicht in:Acta biomaterialia 2024-10, Vol.188, p.157-168
Hauptverfasser: Ojeda-Hernández, Doddy Denise, Velasco-Lozano, Susana, Fraile, José M., Mateos-Díaz, J.C., Rojo, Francisco J., Benito-Martín, María Soledad, Selma-Calvo, Belén, Fuente-Martín, Sarah de la, García-Martín, Marina, Larriba-González, María Teresa, Hernández-Sapiéns, Mercedes Azucena, Canales-Aguirre, Alejandro A., Matias-Guiu, Jordi A., Matias-Guiu, Jorge, Gomez-Pinedo, Ulises
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Sprache:eng
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Zusammenfassung:Cell therapy is a promising strategy for treating neurological pathologies but requires invasive methods to bypass the blood–brain barrier restrictions. The nose-to-brain route has been presented as a direct and less invasive alternative to access the brain. The primary limitations of this route are low retention in the olfactory epithelium and poor cell survival in the harsh conditions of the nasal cavity. Thus, using chitosan-based hydrogel as a vehicle is proposed in this work to overcome the limitations of nose-to-brain cell administration. The hydrogelʼs design was driven to achieve gelification in response to body temperature and a mucosa-interacting chemical structure biocompatible with cells. The hydrogel showed a < 30 min gelation time at 37 °C and >95 % biocompatibility with 2D and 3D cultures of mesenchymal stromal cells. Additionally, the viability, stability, and migration capacity of oligodendrocyte precursor cells (OPCs) within the hydrogel were maintained in vitro for up to 72 h. After the intranasal administration of the OPCs-containing hydrogel, histological analysis showed the presence of viable cells in the nasal cavity for up to 72 h post-administration in healthy athymic mice. These results demonstrate the hydrogel's capacity to increase the residence time in the nasal cavity while providing the cells with a favorable environment for their viability. This study presents for the first time the use of thermosensitive hydrogels in nose-to-brain cell therapy, opening the possibility of increasing the delivery efficiency in future approaches in translational medicine. This work highlights the potential of biomaterials, specifically hydrogels, in improving the effectiveness of cell therapy administered through the nose. The nose-to-brain route has been suggested as a non-invasive way to directly access the brain. However, delivering stem cells through this route poses a challenge since their viability must be preserved and cells can be swept away by nasal mucus. Earlier attempts at intranasal cell therapy have shown low efficiency, but still hold promise to the future. The hydrogels designed for this study can provide stem cells with a biocompatible environment and adhesion to the nasal atrium, easing the successful migration of viable cells to the brain. [Display omitted]
ISSN:1742-7061
1878-7568
1878-7568
DOI:10.1016/j.actbio.2024.09.002