Combinatorial Screening of Biscarbamate Ionizable Lipids Identifies a Low Reactogenicity Lipid for Lipid Nanoparticle mRNA Delivery

Author:

De Lombaerde Emily1,Chen Yong1,Ye Tingting1,Deckers Julie23,Mencarelli Giulia4,De Swarte Kim23,Lauwers Heleen1,De Coen Ruben5,Kasmi Sabah5,Bevers Sanne5,Kuchmiy Anna5,Bogaert Bram5,Baekens Lies5,Zhong Zifu1,Lamoot Alexander1,Sanders Niek N.6,Lambrecht Bart N.23,Baptista Antonio P.23,De Koker Stefaan5,De Geest Bruno G.1ORCID

Affiliation:

1. Department of Pharmaceutics Ghent University Ghent 9000 Belgium

2. Laboratory of Mucosal Immunology VIB‐UGent Center for Inflammation Research Ghent University Ghent 9052 Belgium

3. Department of Internal Medicine and Pediatrics Faculty of Medicine and Health Sciences Ghent University Ghent 9000 Belgium

4. Department of Experimental Medicine and Biochemical Sciences University of Perugia Perugia 06132 Italy

5. etherna Niel 2845 Belgium

6. Laboratory of Gene Therapy Department of Veterinary and Biosciences Faculty of Veterinary Medicine Ghent University Merelbeke 9820 Belgium

Abstract

AbstractMessenger RNA (mRNA) has emerged as a promising therapeutic modality for various diseases. However, efficient delivery of mRNA into target cells remains a significant challenge. In this study, the combinatorial synthesis and characterization of a novel series of ionizable biscarbamate lipids (IBLs) for mRNA lipid nanoparticle (LNP) delivery are reported. A simplified and scalable method is developed, resulting in IBLs suitable for formulating mRNA into stable LNPs. Two generations of IBLs are synthesized and evaluated for their mRNA transfection capacity in vitro, using eGFP as a reporter protein, leading to the identification of S‐Ac7‐DOG as a lead IBL. Upon intramuscular vaccination, S‐Ac7‐DOG LNPs instigated robust antigen‐specific CD8+ T cell responses against an mRNA encoded viral oncoprotein and a tumor neo‐antigen. In comparison to MC3 LNPs, which are used as a benchmark, S‐Ac7‐DOG LNPs exhibit low reactogenicity, robust mRNA transfection, and a distinct biodistribution, with higher accumulation in draining lymph nodes and spleen. These findings highlight the potential of IBLs as a novel and promising class of ionizable lipids for mRNA delivery in vaccines and beyond.

Funder

H2020 European Research Council

Publisher

Wiley

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