Publication | Closed Access
Lipid Nanoparticle Delivery of Chemically Modified NGF<sup>R100W</sup> mRNA Alleviates Peripheral Neuropathy
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Citations
38
References
2022
Year
Messenger RNA (mRNA) carries genetic instructions to the cell machinery for the transient production of antigens or therapeutic proteins and shows enormous potential in vaccine development, cancer immunotherapy, protein replacement therapy, and genome engineering. Here, the synthesis of chemically modified nerve growth factor mutant (NGF<sup>R100W</sup> ) mRNA through in vitro transcription is described. After the replacement of the original signal peptide sequence with the Ig Kappa leader sequence, codon-optimized NGF<sup>R100W</sup> mRNA yielded high secretion of mature NGF<sup>R100W</sup> , which promotes axon growth in PC12 cells. Using lipid nanoparticle (LNP)-delivery of N1-methylpseudouridine-modified mRNA in mice, NGF<sup>R100W</sup> -mRNA-LNPs result in the successful expression of NGF<sup>R100W</sup> protein, which significantly reduces nociceptive activity compared to that of NGF<sup>WT</sup> . This indicates that NGF<sup>R100W</sup> derived from exogenous mRNA elicited "painless" neuroprotective activity. Additionally, the therapeutic value of NGF<sup>R100W</sup> mRNA is established in a paclitaxel-induced peripheral neuropathy model by demonstrating the rapid recovery of intraepidermal nerve fibers. The results show that in vitro-transcribed mRNA has significant flexibility in sequence design and fast in vivo functional validation of target proteins. Furthermore, the results highlight the therapeutic potential of mRNA as a supplement to beneficial proteins for preventing or reversing some chronic medical conditions, such as peripheral neuropathy.
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