4.8 Article

MiRNA 24-3p-rich exosomes functionalized DEGMA-modified hyaluronic acid hydrogels for corneal epithelial healing

Journal

BIOACTIVE MATERIALS
Volume 25, Issue -, Pages 640-656

Publisher

KEAI PUBLISHING LTD
DOI: 10.1016/j.bioactmat.2022.07.011

Keywords

miRNA 24-3p; Exosome; Corneal epithelium; Cell migration; Thermosensitive hydrogel

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Damage to the corneal epithelium can cause irreversible corneal opacities and blindness. The migration rate of corneal epithelial cells directly affects corneal repair. Using exosomes extracted from adipose-derived mesenchymal stem cells loaded with miRNA 24-3p, researchers have found that it can promote rabbit corneal epithelial cell migration and corneal repair.
The damage of corneal epithelium may lead to the formation of irreversible corneal opacities and even blindness. The migration rate of corneal epithelial cells directly affects corneal repair. Here, we explored ocu-microRNA 24-3p (miRNA 24-3p) that can promote rabbit corneal epithelial cells migration and cornea repair. Exosomes, an excellent transport carrier, were exacted from adipose derived mesenchymal stem cells for loading with miRNA 24-3p to prepare miRNA 24-3p-rich exosomes (Exos-miRNA 24-3p). It can accelerate corneal epithelial migration in vitro and in vivo. For application in cornea alkali burns, we further modified hyaluronic acid with di(ethylene glycol) monomethyl ether methacrylate (DEGMA) to obtain a thermosensitive hydrogel, also reported a ther-mosensitive DEGMA-modified hyaluronic acid hydrogel (THH) for the controlled release of Exos-miRNA 24-3p. It formed a highly uniform and clear thin layer on the ocular surface to resist clearance from blinking and extended the drug-ocular-epithelium contact time. The use of THH-3/Exos-miRNA 24-3p for 28 days after alkali burn injury accelerated corneal epithelial defect healing and epithelial maturation. It also reduced corneal stromal fibrosis and macrophage activation. MiRNA 24-3p-rich exosomes functionalized DEGMA-modified hyaluronic acid hydrogel as a multilevel delivery strategy has a potential use for cell-free therapy of corneal epithelial regeneration.

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