Hybrid core-shell particles for mRNA systemic delivery

被引:28
作者
Andretto, Valentina [1 ]
Repellin, Mathieu [1 ]
Pujol, Marine [1 ]
Almouazen, Eyad [1 ]
Sidi-Boumedine, Jacqueline [1 ]
Granjon, Thierry [2 ]
Zhang, Heyang [3 ]
Remaut, Katrien [3 ]
Jordheim, Lars Petter [4 ]
Briancon, Stephanie [1 ]
Keil, Isabel Sofia [5 ]
Vascotto, Fulvia [5 ]
Walzer, Kerstin C. [6 ]
Sahin, Ugur [6 ]
Haas, Heinrich [6 ]
Kryza, David [1 ,7 ]
Lollo, Giovanna [1 ]
机构
[1] Univ Lyon, Univ Claude Bernard Lyon 1, CNRS, LAGEPP UMR 5007, 43 Blvd 11 Novembre 1918, F-69622 Villeurbanne, France
[2] Univ Lyon, Univ Lyon 1, Inst Chim & Biochim Mol & Supramol, ICBMS UMR 5246,CNRS, F-69622 Lyon, France
[3] Univ Ghent, Fac Pharmaceut Sci, Lab Gen Biochem & Phys Pharm, Ghent 9000, Belgium
[4] Univ Lyon, Univ Claude Bernard Lyon 1, Ctr Leon Berard, Ctr Rech Cancerol Lyon,NSERM 1052,CNRS 5286, F-69008 Lyon, France
[5] Johannes Gutenberg Univ gGmbH, TRON Translat Oncol Univ Med Ctr, Mainz, Germany
[6] BioNTech SE, Goldgrube 12, D-55131 Mainz, Germany
[7] Hosp Civils Lyon, F-69437 Lyon, France
关键词
Hybrid lipid-polymer nanoparticles; Core-shell nanoparticles; Lipoplexes; Hyaluronic acid; IVT mRNA; In vivo biodistribution; THERAPY; GENE; NANOPARTICLES; COMPLEXES; BINDING; CELLS;
D O I
10.1016/j.jconrel.2022.11.042
中图分类号
O6 [化学];
学科分类号
0703 ;
摘要
mRNA based infectious disease vaccines have opened the venue for development of novel nucleic acids-based therapeutics. For all mRNA therapeutics dedicated delivery systems are required, where different functionalities and targeting abilities need to be optimized for the respective applications. One option for advanced formulations with tailored properties are lipid-polymer hybrid nanoparticles with complex nanostructure, which allow to combine features of several already well described nucleic acid delivery systems. Here, we explored hyaluronic acid (HA) as coating of liposome-mRNA complexes (LRCs) to investigate effects of the coating on surface charge, physicochemical characteristics and biological activity. HA was electrostatically attached to positively charged complexes, forming hybrid LRCs (HLRCs). At different N/P ratios, physico-chemical characterization of the two sets of particles showed similarity in size (around 200 nm) and mRNA binding abilities, while the presence of the HA shell conferred a negative surface charge to otherwise positive complexes. High transfection efficiency of LRCs and HLRCs in vitro has been obtained in THP-1 and human monocytes derived from PBMC, an interesting target cell population for cancer and immune related pathologies. In mice, quantitative biodistribution of radiolabeled LRC and HLRC particles, coupled with bioluminescence studies to detect the protein translation sites, hinted towards both particles' accumulation in the hepatic reticuloendothelial system (RES). mRNA translated proteins though was found mainly in the spleen, a major source for immune cells, with preference for expression in macrophages. The results showed that surface modifications of liposome-mRNA complexes can be used to fine-tune nanoparticle physico-chemical characteristics. This provides a tool for assembly of stable and optimized nanoparticles, which are prerequisite for future therapeutic interventions using mRNA-based nanomedicines.
引用
收藏
页码:1037 / 1049
页数:13
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