Modulating lipid nanoparticles with histidinamide-conjugated cholesterol for improved intracellular delivery of mRNA

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Title
Modulating lipid nanoparticles with histidinamide-conjugated cholesterol for improved intracellular delivery of mRNA
Author(s)
O Jung; Hye-Youn Jung; L T Thuy; M Choi; S Kim; Hae-Geun JeonJihyun Yang; Seok-Min Kim; Tae-Don Kim; E Lee; Yoonkyung Kim; J S Choi
Bibliographic Citation
Advanced Healthcare Materials, vol. 13, no. 14, pp. 2303857-2303857
Publication Year
2024
Abstract
Recently, mRNA-based therapeutics, including vaccines, have gained significant attention in the field of gene therapy for treating various diseases. Among the various mRNA delivery vehicles, lipid nanoparticles (LNPs) have emerged as promising vehicles for packaging and delivering mRNA with low immunogenicity. However, while mRNA delivery has several advantages, the delivery efficiency and stability of LNPs remain challenging for mRNA therapy. In this study, an ionizable helper cholesterol analog, 3β[L-histidinamide-carbamoyl] cholesterol (Hchol) lipid is developed and incorporated into LNPs instead of cholesterol to enhance the LNP potency. The pKa values of the Hchol-LNPs are ?6.03 and 6.61 in MC3- and SM102-based lipid formulations. Notably, the Hchol-LNPs significantly improve the delivery efficiency by enhancing the endosomal escape of mRNA. Additionally, the Hchol-LNPs are more effective in a red blood cell hemolysis at pH 5.5, indicating a synergistic effect of the protonated imidazole groups of Hchol and cholesterol on endosomal membrane destabilization. Furthermore, mRNA delivery is substantially enhanced in mice treated with Hchol-LNPs. Importantly, LNP-encapsulated SARS-CoV-2 spike mRNA vaccinations induce potent antigen-specific antibodies against SARS-CoV-2. Overall, incorporating Hchol into LNP formulations enables efficient endosomal escape and stability, leading to an mRNA delivery vehicle with a higher delivery efficiency.
ISSN
2192-2640
Publisher
Wiley
Full Text Link
http://dx.doi.org/10.1002/adhm.202303857
Type
Article
Appears in Collections:
Division of Research on National Challenges > Infectious Disease Research Center > 1. Journal Articles
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