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Reformulating lipid nanoparticles for organ-targeted mRNA accumulation and translation

Kexin Su, Lu Shi, Tao Sheng, Xinxin Yan, Lixin Lin, Chaoyang Meng, Shiqi Wu, Yuxuan Chen, Yao Zhang, Chaorong Wang, Zichuan Wang, Junjie Qiu, Jiahui Zhao, Tengfei Xu, Ping Yuan, Zhen Gu, Shuai Liu

2024Nature Communications224 citationsDOIOpen Access PDF

Abstract

Fully targeted mRNA therapeutics necessitate simultaneous organ-specific accumulation and effective translation. Despite some progress, delivery systems are still unable to fully achieve this. Here, we reformulate lipid nanoparticles (LNPs) through adjustments in lipid material structures and compositions to systematically achieve the pulmonary and hepatic (respectively) targeted mRNA distribution and expression. A combinatorial library of degradable-core based ionizable cationic lipids is designed, following by optimisation of LNP compositions. Contrary to current LNP paradigms, our findings demonstrate that cholesterol and phospholipid are dispensable for LNP functionality. Specifically, cholesterol-removal addresses the persistent challenge of preventing nanoparticle accumulation in hepatic tissues. By modulating and simplifying intrinsic LNP components, concurrent mRNA accumulation and translation is achieved in the lung and liver, respectively. This targeting strategy is applicable to existing LNP systems with potential to expand the progress of precise mRNA therapy for diverse diseases.

Topics & Concepts

Translation (biology)Messenger RNAComputational biologyChemistryPhospholipidCell biologyNanotechnologyBiologyBiochemistryMaterials scienceGeneMembraneRNA Interference and Gene DeliveryRNA Research and SplicingRNA and protein synthesis mechanisms
Reformulating lipid nanoparticles for organ-targeted mRNA accumulation and translation | Litcius