Effects of Histidine Oligomers in Lipid Nanoparticles on siRNA Delivery

Author:

Lee Hyeondo1,You Gayeon1,Yeo Sangho1,Lee Hyukjin2,Mok Hyejung1ORCID

Affiliation:

1. Department of Bioscience and Biotechnology Konkuk University Seoul 05029 Republic of Korea

2. College of Pharmacy Graduate School of Pharmaceutical Sciences Ewha Womans University Seoul 03760 Republic of Korea

Abstract

AbstractIn this study, histidine oligomer (oHis; 10mer)‐incorporating LNPs (H10LNPs) are developed as a novel carrier for efficient siRNA delivery. Notably, the unmodified oHis (10mer) is greatly incorporated within LNPs through ionic interaction with siRNAs, which serves as an endosome escape enhancer. H10LNPs with a size of ≈65 nm demonstrate a significantly enhanced extent of endosomal escape, as evidenced by calcein assay and confocal microscopy images of intracellular fluorescence, surpassing conventional LNPs. Furthermore, the half inhibitory concentration (IC50) of the human endogenous globotriaosylceramide synthase (Gb3 synthase) gene in H10LNPs‐treated cells exhibits a significant threefold decrease, compared to that in LNP‐treated cells. Notably, H10LNPs maintain comparable biocompatibility and biodistribution both in vitro and in vivo. Considering that the fabricated siRNA H10LNPs exhibit excellent biocompatibility and superior gene silencing activity over conventional LNPs, these particles can be harnessed for the safe delivery of therapeutic siRNAs. Additionally, this study introduces promising, feasible, simple, and alternative formulation processes for integrating unmodified functional cationic peptides into LNPs to enhance the delivery efficiency of a wide range of nucleic acid‐based drugs.

Funder

National Research Foundation of Korea

Ministry of Health and Welfare

Publisher

Wiley

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