| Literature DB >> 30748040 |
Kalina Paunovska1, Alejandro J Da Silva Sanchez1, Cory D Sago1, Zubao Gan1, Melissa P Lokugamage1, Fatima Z Islam1, Sujay Kalathoor1, Brandon R Krupczak1, James E Dahlman1.
Abstract
Using mRNA to produce therapeutic proteins is a promising approach to treat genetic diseases. However, systemically delivering mRNA to cell types besides hepatocytes remains challenging. Fast identification of nanoparticle delivery (FIND) is a DNA barcode-based system designed to measure how over 100 lipid nanoparticles (LNPs) deliver mRNA that functions in the cytoplasm of target cells in a single mouse. By using FIND to quantify how 75 chemically distinct LNPs delivered mRNA to 28 cell types in vivo, it is found that an LNP formulated with oxidized cholesterol and no targeting ligand delivers Cre mRNA, which edits DNA in hepatic endothelial cells and Kupffer cells at 0.05 mg kg-1 . Notably, the LNP targets liver microenvironmental cells fivefold more potently than hepatocytes. The structure of the oxidized cholesterols added to the LNP is systematically varied to show that the position of the oxidative modification may be important; cholesterols modified on the hydrocarbon tail associated with sterol ring D tend to outperform cholesterols modified on sterol ring B. These data suggest that LNPs formulated with modified cholesterols can deliver gene-editing mRNA to the liver microenvironment at clinically relevant doses.Entities:
Keywords: Cre; DNA barcodes; barcoded nanoparticles; cholesterol; drug delivery; gene editing; mRNA
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Year: 2019 PMID: 30748040 PMCID: PMC6445717 DOI: 10.1002/adma.201807748
Source DB: PubMed Journal: Adv Mater ISSN: 0935-9648 Impact factor: 30.849