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Lipid Nanoparticle Composition Drives mRNA Delivery to the Placenta

View ORCID ProfileRachel E. Young, View ORCID ProfileKatherine M. Nelson, Samuel I. Hofbauer, Tara Vijayakumar, View ORCID ProfileMohamad-Gabriel Alameh, View ORCID ProfileDrew Weissman, View ORCID ProfileCharalampos Papachristou, View ORCID ProfileJason P. Gleghorn, View ORCID ProfileRachel S. Riley
doi: https://doi.org/10.1101/2022.12.22.521490
Rachel E. Young
aDepartment of Biomedical Engineering, Henry M. Rowan College of Engineering, Rowan University, 201 Mullica Hill Rd, Glassboro, NJ 08028, United States
bSchool of Translational Biomedical Engineering & Sciences, Virtua College of Medicine & Life Sciences of Rowan University, 201 Mullica Hill Rd, Glassboro, NJ 08028, United States
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Katherine M. Nelson
cDepartment of Chemical and Biomolecular Engineering, College of Engineering, University of Delaware, 150 Academy Street, Newark, DE 19716, United States
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Samuel I. Hofbauer
aDepartment of Biomedical Engineering, Henry M. Rowan College of Engineering, Rowan University, 201 Mullica Hill Rd, Glassboro, NJ 08028, United States
bSchool of Translational Biomedical Engineering & Sciences, Virtua College of Medicine & Life Sciences of Rowan University, 201 Mullica Hill Rd, Glassboro, NJ 08028, United States
dCooper Medical School of Rowan University, Rowan University, 401 Broadway, Camden, NJ 08103, United States
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Tara Vijayakumar
aDepartment of Biomedical Engineering, Henry M. Rowan College of Engineering, Rowan University, 201 Mullica Hill Rd, Glassboro, NJ 08028, United States
bSchool of Translational Biomedical Engineering & Sciences, Virtua College of Medicine & Life Sciences of Rowan University, 201 Mullica Hill Rd, Glassboro, NJ 08028, United States
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Mohamad-Gabriel Alameh
ePerelman School of Medicine, University of Pennsylvania, 3400 Civic Center Blvd, Philadelphia, PA 19104, United States
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Drew Weissman
ePerelman School of Medicine, University of Pennsylvania, 3400 Civic Center Blvd, Philadelphia, PA 19104, United States
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Charalampos Papachristou
fDepartment of Mathematics, College of Science & Mathematics, Rowan University, 201 Mullica Hill Rd, Glassboro, NJ 08028, United States
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Jason P. Gleghorn
gDepartment of Biomedical Engineering, College of Engineering, University of Delaware, 590 Avenue 1743, Newark, DE 19713, United States
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Rachel S. Riley
aDepartment of Biomedical Engineering, Henry M. Rowan College of Engineering, Rowan University, 201 Mullica Hill Rd, Glassboro, NJ 08028, United States
bSchool of Translational Biomedical Engineering & Sciences, Virtua College of Medicine & Life Sciences of Rowan University, 201 Mullica Hill Rd, Glassboro, NJ 08028, United States
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  • For correspondence: rileyr@rowan.edu
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ABSTRACT

Ionizable lipid nanoparticles (LNPs) have gained attention as mRNA delivery platforms for vaccination against COVID-19 and for protein replacement therapies. LNPs enhance mRNA stability, circulation time, cellular uptake, and preferential delivery to specific tissues compared to mRNA with no carrier platform. However, LNPs have yet to be developed for safe and effective mRNA delivery to the placenta as a method to treat placental dysfunction. Here, we develop LNPs that enable high levels of mRNA delivery to trophoblasts in vitro and to the placenta in vivo with no toxicity. We conducted a Design of Experiments to explore how LNP composition, including the type and molar ratio of each lipid component, drives trophoblast and placental delivery. Our data revealed that a specific combination of ionizable lipid and phospholipid in the LNP design yields high transfection efficiency in vitro. Further, we present one LNP platform that exhibits highest delivery of placental growth factor mRNA to the placenta in pregnant mice, which demonstrates induced protein synthesis and secretion of a therapeutic protein. Lastly, our high-performing LNPs have no toxicity to both the pregnant mice and fetuses. Our results demonstrate the feasibility of LNPs as a platform for mRNA delivery to the placenta. Our top LNPs may provide a therapeutic platform to treat diseases that originate from placental dysfunction during pregnancy.

Competing Interest Statement

The authors have declared no competing interest.

  • ABBREVIATIONS

    LNP
    lipid nanoparticle
    PEG
    polyethylene glycol
    DOE
    design of experiments
    HELLP
    hemolysis, elevated liver enzymes, low platelet count
    sFlt-1
    soluble fms-like tyrosine kinase-1
    PlGF
    placental growth factor
    VEGFR1
    vascular endothelial growth factor receptor-1
    DSD
    definitive screening design
    DOPE
    1,2-dioleoyl-sn-glycero-3-phosphoethanolamine
    DSPC
    1,2 distearoyl-sn-glycero-3-phosphocholine
    DMPE-PEG
    1,2-dimyristoyl-sn-glycero-3-phosphoethanolamine-N-[methoxy(polyethylene glycol)-2000] (ammonium salt)
    TNS
    [6-(p-toluidinyl)naphthalene-2-sulfonic acid]
    ALT
    alanine aminotransferase
    AST
    aspartate aminotransferase
    IL-6
    interleukin-6
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    Posted December 22, 2022.
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    Lipid Nanoparticle Composition Drives mRNA Delivery to the Placenta
    Rachel E. Young, Katherine M. Nelson, Samuel I. Hofbauer, Tara Vijayakumar, Mohamad-Gabriel Alameh, Drew Weissman, Charalampos Papachristou, Jason P. Gleghorn, Rachel S. Riley
    bioRxiv 2022.12.22.521490; doi: https://doi.org/10.1101/2022.12.22.521490
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    Lipid Nanoparticle Composition Drives mRNA Delivery to the Placenta
    Rachel E. Young, Katherine M. Nelson, Samuel I. Hofbauer, Tara Vijayakumar, Mohamad-Gabriel Alameh, Drew Weissman, Charalampos Papachristou, Jason P. Gleghorn, Rachel S. Riley
    bioRxiv 2022.12.22.521490; doi: https://doi.org/10.1101/2022.12.22.521490

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