| Literature DB >> 29331806 |
Sushma M Bhosle1, Kristin H Loomis1, Jonathan L Kirschman1, Emmeline L Blanchard1, Daryll A Vanover1, Chiara Zurla1, Damien Habrant2, Darin Edwards3, Patrick Baumhof4, Bruno Pitard5, Philip J Santangelo6.
Abstract
The translational efficiency of an in vitro transcribed (IVT) mRNA was measured upon delivery to primary skeletal muscle cells and to a mouse model system, towards the development of a predictive in vitro assay for the screening and validation of intramuscular mRNA-based vaccines. When IVT mRNA was delivered either naked or complexed with novel aminoglycoside-based delivery vehicles, significant differences in protein expression in vitro and in vivo were observed. We hypothesized that this previously anticipated discrepancy was due to differences in the mechanism of IVT mRNA endosomal entry and release following delivery. To address this, IVT mRNA was fluorescently labeled prior to delivery, to visualize its distribution. Colocalization with endosomal markers indicated that different entry pathways were utilized in vivo and in vitro, depending on the delivery vehicle, resulting in variations in protein expression levels. Since extracellular matrix stiffness (ECM) influences mRNA entry, trafficking and release, the effect of mechanotransduction on mRNA expression was investigated in vitro upon delivery of IVT mRNA alone, and complexed with delivery vehicles to skeletal muscle cells grown on ∼10 kPa hydrogels. This in vitro hydrogel model more accurately recapitulated the results obtained in vivo upon IM injection, indicating that this approach may assist in the characterization of mRNA based vaccines.Entities:
Keywords: ECM protein; Hydrogels; Mechanotransduction; Nanoparticles; Skeletalmuscle cells; mRNA delivery
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Year: 2018 PMID: 29331806 DOI: 10.1016/j.biomaterials.2018.01.010
Source DB: PubMed Journal: Biomaterials ISSN: 0142-9612 Impact factor: 12.479