Electrospun fiber-mediated delivery of neurotrophin-3 mRNA for neural tissue engineering applications

Aligned electrospun fibers provide topographical cues and local therapeutic delivery to facilitate robust peripheral nerve regeneration. mRNA delivery enables transient expression of desired proteins that promote axonal regeneration. However, no prior work delivers mRNA from electrospun fibers for peripheral nerve regeneration applications. Here, we developed the first aligned electrospun fibers to deliver pseudouridine-modified (Psi) neurotrophin-3 (NT-3) mRNA (Psi NT-3mRNA) to primary Schwann cells and assessed NT-3 secretion and bioactivity. We first electrospun aligned poly(L-lactic acid) (PLLA) fibers and coated them with the anionic substrates dextran sulfate sodium salt (DSS) or poly(3,4-dihydroxy-L-phenylalanine) (pDOPA). Cationic lipoplexes containing Psi NT-3mRNA complexed to JetMESSENGER (R) were then immobilized to the fibers, resulting in detectable Psi NT-3mRNA release for 28 days from all fiber groups investigated (PLLA +mRNA, 0.5DSS4h +mRNA, and 2pDOPA4h +mRNA). The 2pDOPA4h +mRNA group significantly increased Schwann cell secretion of NT-3 for 21 days compared to control PLLA fibers ( p < 0.001-0.05) and, on average, increased Schwann cell secretion of NT-3 by >= 2-fold compared to bo-us mRNA delivery from the 1 mu gBolus+mRNA and 3 mu gBolus+mRNA groups. The 2pDOPA4h +mRNA fibers supported Schwann cell secretion of NT-3 at levels that significantly increased dorsal root ganglia (DRG) neurite extension by 44% ( p < 0.0 0 01) and neurite area by 64% ( p < 0.001) compared to control PLLA fibers. The data show that the 2pDOPA4h + mRNA fibers enhance the ability of Schwann cells to promote neurite growth from DRG, demonstrating this platform's potential capability to improve peripheral nerve regeneration. Statement of significance Aligned electrospun fibers enhance axonal regeneration by providing structural support and guidance cues, but further therapeutic stimulation is necessary to improve functional outcomes. mRNA delivery enables the transient expression of therapeutic proteins, yet achieving local, sustained delivery remains challenging. Previous work shows that genetic material delivery from electrospun fibers improves regeneration; however, mRNA delivery has not been explored. Here, we examine mRNA delivery from aligned electrospun fibers to enhance neurite outgrowth. We show that immobilization of NT-3mRNA/JetMESSENGER (R) lipoplexes to aligned electrospun fibers functionalized with pDOPA enables local, sustained NT-3mRNA delivery to Schwann cells, increasing Schwann cell secretion of NT-3 and enhancing DRG neurite outgrowth. This study displays the potential benefits of electrospun fiber-mediated mRNA delivery platforms for neural tissue engineering. Published by Elsevier Ltd on behalf of Acta Materialia Inc.