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Complex Size and Surface Charge Determine Nucleic Acid Transfer by Fusogenic Liposomes

Marco Hoffmann, Nils Hersch, S. Gerlach, Georg Dreissen, Ronald Springer, Rudolf Merkel, Ágnes Csiszár, Bernd Hoffmann

2020International Journal of Molecular Sciences32 citationsDOIOpen Access PDF

Abstract

Highly efficient, biocompatible, and fast nucleic acid delivery methods are essential for biomedical applications and research. At present, two main strategies are used to this end. In non-viral transfection liposome- or polymer-based formulations are used to transfer cargo into cells via endocytosis, whereas viral carriers enable direct nucleic acid delivery into the cell cytoplasm. Here, we introduce a new generation of liposomes for nucleic acid delivery, which immediately fuse with the cellular plasma membrane upon contact to transfer the functional nucleic acid directly into the cell cytoplasm. For maximum fusion efficiency combined with high cargo transfer, nucleic acids had to be complexed and partially neutralized before incorporation into fusogenic liposomes. Among the various neutralization agents tested, small, linear, and positively charged polymers yielded the best complex properties. Systematic variation of liposomal composition and nucleic acid complexation identified surface charge as well as particle size as essential parameters for cargo-liposome interaction and subsequent fusion induction. Optimized protocols were tested for the efficient transfer of different kinds of nucleic acids like plasmid DNA, messenger RNA, and short-interfering RNA into various mammalian cells in culture and into primary tissues.

Topics & Concepts

Nucleic acidLiposomeEndocytosisCytoplasmSmall interfering RNATransfectionBiophysicsDNARNABiochemistryChemistryBiologyCellGeneRNA Interference and Gene DeliveryAdvanced biosensing and bioanalysis techniquesVirus-based gene therapy research
Complex Size and Surface Charge Determine Nucleic Acid Transfer by Fusogenic Liposomes | Litcius