PURPOSE: We describe a nucleation-based method which allows for the generation of monodisperse lipid nanoparticles over a range of diameters. Using a set of novel zwitterionic lipids and inverse phosphocholine lipids with pKas ranging from 2 to 5, we showed how the hydrodynamic diameter of lipid nanoparticles can be systematically manipulated over a 60 nm to 500 nm size range. METHOD: Lipid nanoparticles were prepared by adding an anti-solvent, such as water, to the organic phase containing the lipid components. This led to super-saturation and the spontaneous formation of particles. RESULTS: The growth and final particle size was controlled by the ratio of the components in the ternary system: lipid, organic solvent and aqueous phase. Particles with diameter below 125 nm were formed under conditions where the super-saturation coefficient was between 2.3 and 20. PEG-lipid served as an efficient growth inhibitor except at very high and low lipid concentrations. Encapsulation efficiency of siRNA into lipid nanoparticles was shown to be pH-dependent and requires the protonation of the anionic carboxylate groups of the zwitterionic lipids, emphasizing the importance of electrostatic forces. CONCLUSION: This process enables high encapsulation efficiency of nucleic acids and allows the size of lipid nanoparticles to be controlled.
PURPOSE: We describe a nucleation-based method which allows for the generation of monodisperse lipid nanoparticles over a range of diameters. Using a set of novel zwitterionic lipids and inverse phosphocholinelipids with pKas ranging from 2 to 5, we showed how the hydrodynamic diameter of lipid nanoparticles can be systematically manipulated over a 60 nm to 500 nm size range. METHOD:Lipid nanoparticles were prepared by adding an anti-solvent, such as water, to the organic phase containing the lipid components. This led to super-saturation and the spontaneous formation of particles. RESULTS: The growth and final particle size was controlled by the ratio of the components in the ternary system: lipid, organic solvent and aqueous phase. Particles with diameter below 125 nm were formed under conditions where the super-saturation coefficient was between 2.3 and 20. PEG-lipid served as an efficient growth inhibitor except at very high and low lipid concentrations. Encapsulation efficiency of siRNA into lipid nanoparticles was shown to be pH-dependent and requires the protonation of the anionic carboxylate groups of the zwitterionic lipids, emphasizing the importance of electrostatic forces. CONCLUSION: This process enables high encapsulation efficiency of nucleic acids and allows the size of lipid nanoparticles to be controlled.
Authors: Abraham D Stroock; Stephan K W Dertinger; Armand Ajdari; Igor Mezic; Howard A Stone; George M Whitesides Journal: Science Date: 2002-01-25 Impact factor: 47.728
Authors: Vincent J Venditto; Aaron Dolor; Aditya Kohli; Stefan Salentinig; Ben J Boyd; Francis C Szoka Journal: Chem Commun (Camb) Date: 2014-08-21 Impact factor: 6.222
Authors: Shaza Abdulnasser Harfoush; Matthias Hannig; Duc Dung Le; Sebastian Heck; Maximilian Leitner; Albert Joachim Omlor; Isabella Tavernaro; Annette Kraegeloh; Ralf Kautenburger; Guido Kickelbick; Andreas Beilhack; Markus Bischoff; Juliane Nguyen; Martina Sester; Robert Bals; Quoc Thai Dinh Journal: Respir Res Date: 2020-07-02