Optimization of a lipid nanoparticle–based protocol for RNA transfection into primary mononuclear phagocytes

Author:

Zhang Yu1,Béland Louis-Charles1,Roussel Sabrina2,Bertrand Nicolas2,Hébert Sébastien S1,Vallières Luc1ORCID

Affiliation:

1. Neuroscience Unit, University Hospital Center of Quebec-Laval University , 2705 Laurier Boulevard, Quebec City, Quebec G1V 4G2 , Canada

2. Endocrinology and Nephrology Unit, University Hospital Center of Quebec-Laval University , 2705 Laurier Boulevard, Quebec City, Quebec G1V 4G2 , Canada

Abstract

Abstract The effective delivery of synthetic RNA into mononuclear phagocytes is a prerequisite for experimental research and therapeutic development. However, traditional methods are highly ineffective and toxic for these cells. Here, we aimed to optimize a transfection protocol for primary bone marrow–derived phagocytes, specifically dendritic cells and macrophages, using lipid nanoparticles generated by microfluidics. Our results show that a lipid mixture similar to that used in Moderna's COVID-19 messenger RNA vaccine outperforms the others tested. Improved messenger RNA transfection can be achieved by replacing uridine with methylpseudouridine but not methoxyuridine, which interferes with transfection. The addition of diphenyleneiodonium or apocynin can enhance transfection in a cell type–dependent manner without adverse effects, while apolipoprotein E provides no added value. These optimized transfection conditions can also be used for microRNA agonists and antagonists. In sum, this study offers a straightforward, highly efficient, reproducible, and nontoxic protocol to deliver RNA into different primary mononuclear phagocytes in culture.

Funder

Multiple Sclerosis Society of Canada

Canadian Institutes for Health Research

Natural Sciences and Engineering Research Council of Canada

CHU de Québec with its Neuroscience Unit

Laval University Joint Scholarship Program

Fonds de Recherche du Québec–Santé

Publisher

Oxford University Press (OUP)

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