Development of a local controlled release system for therapeutic proteins in the treatment of skeletal muscle injuries and diseases.
Rachel LevOrit Bar-AmGalit SaarOmbretta GuardiolaGabriella MinchiottiEli PeledDror SeliktarPublished in: Cell death & disease (2024)
The present study aims to develop and characterize a controlled-release delivery system for protein therapeutics in skeletal muscle regeneration following an acute injury. The therapeutic protein, a membrane-GPI anchored protein called Cripto, was immobilized in an injectable hydrogel delivery vehicle for local administration and sustained release. The hydrogel was made of poly(ethylene glycol)-fibrinogen (PEG-Fibrinogen, PF), in the form of injectable microspheres. The PF microspheres exhibited a spherical morphology with an average diameter of approximately 100 micrometers, and the Cripto protein was uniformly entrapped within them. The release rate of Cripto from the PF microspheres was controlled by tuning the crosslinking density of the hydrogel, which was varied by changing the concentration of poly(ethylene glycol) diacrylate (PEG-DA) crosslinker. In vitro experiments confirmed a sustained-release profile of Cripto from the PF microspheres for up to 27 days. The released Cripto was biologically active and promoted the in vitro proliferation of mouse myoblasts. The therapeutic effect of PF-mediated delivery of Cripto in vivo was tested in a cardiotoxin (CTX)-induced muscle injury model in mice. The Cripto caused an increase in the in vivo expression of the myogenic markers Pax7, the differentiation makers eMHC and Desmin, higher numbers of centro-nucleated myofibers and greater areas of regenerated muscle tissue. Collectively, these results establish the PF microspheres as a potential delivery system for the localized, sustained release of therapeutic proteins toward the accelerated repair of damaged muscle tissue following acute injuries.
Keyphrases
- skeletal muscle
- drug delivery
- hyaluronic acid
- insulin resistance
- protein protein
- molecularly imprinted
- liver failure
- binding protein
- stem cells
- tissue engineering
- wound healing
- drug induced
- respiratory failure
- amino acid
- type diabetes
- metabolic syndrome
- escherichia coli
- diabetic rats
- adipose tissue
- extracorporeal membrane oxygenation
- long non coding rna
- ionic liquid
- multidrug resistant
- acute respiratory distress syndrome
- cord blood
- combination therapy
- capillary electrophoresis