Author:
Ripoll Manon,Martin Elian,Enot Mathilde,Robbe Oscar,Rapisarda Chiara,Nicolai Marie-Claire,Deliot Aurélie,Tabeling Patrick,Authelin Jean-René,Nakach Mostafa,Wils Pierre
Abstract
AbstractLipid nanoparticles (LNPs) for RNA and DNA delivery have attracted considerable attention for their ability to treat a broad range of diseases and to vectorize mRNA for COVID vaccines. LNPs are produced by mixing biomolecules and lipids, which self-assemble to form the desired structure. In this domain, microfluidics shows clear advantages: high mixing quality, low-stress conditions, and fast preparation. Studies of LNPs produced in micromixers have revealed, in certain ranges of flow rates, a degradation in performance in terms of size, monodispersity and encapsulation efficiency. In this study, we focus on the ring micromixer, which is well adapted to high throughput. We reveal three regimes, side-by-side, transitional and highly mixed, that control the mixing performance of the device. Furthermore, using cryo-TEM and biochemical analysis, we show that the mixing performances are strongly correlated to the characteristics of the LNPs we produce. We emphasize the importance of the flow-rate ratio and propose a physical criterion based on the onset of temporal instabilities for producing LNPs with optimal characteristics in terms of geometry, monodispersity and encapsulation yield. These criteria are generally applicable.
Funder
SANOFI, France
École Supérieure de Physique et de Chimie Industrielles de la Ville de Paris
Centre National de la Recherche Scientifique
Publisher
Springer Science and Business Media LLC
Cited by
32 articles.
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