Tuning Lipid Nanoparticles for RNA Delivery to Extrahepatic Organs

Author:

Song Donghui1ORCID,Zhao Yu1,Wang Zeyu1,Xu Qiaobing1ORCID

Affiliation:

1. Department of Biomedical Engineering Tufts University Medford MA 02155 USA

Abstract

AbstractRNA therapeutics have been successfully transitioned into clinical applications. Lipid nanoparticles (LNPs) are widely employed as nonviral delivery vehicles for RNA therapeutics in commercial vaccine and gene therapy products. However, the bottleneck in expanding the clinical applications of LNP‐based RNA therapeutics lies in the tendency of these nanoparticles to preferentially accumulate in the liver. This challenge underscores the need to design LNPs capable of delivering RNA to organs beyond the liver. In this perspective, recent progress is discussed in developing strategies for designing LNPs to deliver RNA to extrahepatic organs. Organ‐selective targeting capability is achieved by either altering the composition of the LNP formulation or chemically modifying the ionizable lipid component. Both approaches result in changes in the physicochemical properties of the LNPs, which subsequently alters the composition of the biomolecular corona that adsorbs onto its surface following administration. The biomolecular corona is a known mechanism that mediates organ‐selective LNP delivery. Furthermore, this perspective aims to provide an outlook on shaping the next‐generation LNP delivery platforms. Potential efforts include targeting specific cell types, improving the safety profile of LNPs, and developing strategies to overcome physiological barriers against organ‐specific delivery.

Funder

National Institutes of Health

Publisher

Wiley

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