| Literature DB >> 35633287 |
Christopher R Lucas1, Patrick D Halley2, Amjad A Chowdury2, Bonnie K Harrington3, Larry Beaver4, Rosa Lapalombella4, Amy J Johnson4, Erin K Hertlein4, Mitch A Phelps5, John C Byrd3, Carlos E Castro6.
Abstract
DNA origami (DO) nanotechnology enables the construction of precise nanostructures capable of functionalization with small molecule drugs, nucleic acids, and proteins, suggesting a promising platform for biomedical applications. Despite the potential for drug and vaccine delivery, the impact of DO vehicles on immunogenicity in vivo is not well understood. Here, two DO vehicles, a flat triangle and a nanorod, at varying concentrations are evaluated in vitro and with a repeated dosing regimen administered at a high dose in vivo to study early and late immunogenicity. The studies show normal CD11b+ myeloid cell populations preferentially internalize DO in vitro. DO structures distribute well systemically in vivo, elicit a modest pro-inflammatory immune response that diminishes over time and are nontoxic as shown by weight, histopathology, lack of cytokine storm, and a complete biochemistry panel at the day 10 end point. The results take critical steps to characterize the biological response to DO and suggest that DO vehicles represent a promising platform for drug delivery and vaccine development where immunogenicity should be a key consideration.Entities:
Keywords: DNA origami; biomedical nanotechnology; drug delivery; immunogenicity; in vivo
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Year: 2022 PMID: 35633287 PMCID: PMC9250639 DOI: 10.1002/smll.202108063
Source DB: PubMed Journal: Small ISSN: 1613-6810 Impact factor: 15.153