Inhalable exosomes outperform liposomes as mRNA and protein drug carriers to the lung

Kristen D. Popowski(North Carolina State University), Blanca López de Juan Abad(North Carolina State University), Arianna George(North Carolina State University), Dylan Silkstone(University of North Carolina at Chapel Hill), Elizabeth Belcher(University of North Carolina at Chapel Hill), Jae-Wook Chung(North Carolina State University), Asma Ghodsi(North Carolina State University), Halle Lutz(North Carolina State University), Jada Davenport(North Carolina State University), Mallory Flanagan(North Carolina State University), Jorge A. Piedrahita(North Carolina State University), Phuong‐Uyen Dinh(North Carolina State University), Ke Cheng(University of North Carolina at Chapel Hill)
Extracellular Vesicle
June 15, 2022
Cited by 151Open Access
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Abstract

Respiratory diseases are among the leading causes of morbidity and mortality worldwide, coupled with the ongoing coronavirus disease 2019 (COVID-19) pandemic. mRNA lipid nanoparticle (LNP) vaccines have been developed, but their intramuscular delivery limits pulmonary bioavailability. Inhalation of nanoparticle therapeutics offers localized drug delivery that minimizes off targeted adverse effects and has greater patient compliance. However, LNP platforms require extensive reformulation for inhaled delivery. Lung-derived extracellular vesicles (Lung-Exo) offer a biological nanoparticle alternative that is naturally optimized for mRNA translation and delivery to pulmonary cells. We compared the biodistribution of Lung-Exo against commercially standard biological extracellular vesicles (HEK-Exo) and LNPs (Lipo), where Lung-Exo exhibited superior mRNA and protein cargo distribution to and retention in the bronchioles and parenchyma following nebulization administration. This suggests that inhaled Lung-Exo can deliver mRNA and protein drugs with enhanced pulmonary bioavailability and therapeutic efficacy.


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