Ionization and structural properties of mRNA lipid nanoparticles influence expression in intramuscular and intravascular administration

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作者
Manuel J. Carrasco
Suman Alishetty
Mohamad-Gabriel Alameh
Hooda Said
Lacey Wright
Mikell Paige
Ousamah Soliman
Drew Weissman
Thomas E. Cleveland
Alexander Grishaev
Michael D. Buschmann
机构
[1] George Mason University,Department of Bioengineering
[2] University of Pennsylvania,Perelman School of Medicine
[3] George Mason University,Department of Chemistry & Biochemistry
[4] University of Pennsylvania,Perelman School of Medicine
[5] Institute for Bioscience and Biotechnology Research National Institute of Standards and Technology,undefined
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Communications Biology | / 4卷
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摘要
Lipid Nanoparticles (LNPs) are used to deliver siRNA and COVID-19 mRNA vaccines. The main factor known to determine their delivery efficiency is the pKa of the LNP containing an ionizable lipid. Herein, we report a method that can predict the LNP pKa from the structure of the ionizable lipid. We used theoretical, NMR, fluorescent-dye binding, and electrophoretic mobility methods to comprehensively measure protonation of both the ionizable lipid and the formulated LNP. The pKa of the ionizable lipid was 2-3 units higher than the pKa of the LNP primarily due to proton solvation energy differences between the LNP and aqueous medium. We exploited these results to explain a wide range of delivery efficiencies in vitro and in vivo for intramuscular (IM) and intravascular (IV) administration of different ionizable lipids at escalating ionizable lipid-to-mRNA ratios in the LNP. In addition, we determined that more negatively charged LNPs exhibit higher off-target systemic expression of mRNA in the liver following IM administration. This undesirable systemic off-target expression of mRNA-LNP vaccines could be minimized through appropriate design of the ionizable lipid and LNP.
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