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Your search keyword '"Simonsen, Jens B."' showing total 4 results
Start Over Author "Simonsen, Jens B." Topic drug delivery
4 results on '"Simonsen, Jens B."'

2. A systematic review of the biodistribution of biomimetic high-density lipoproteins in mice.

Author

Pedersbæk, Dennis and Simonsen, Jens B.

Subjects
*LIPOPROTEINS, *MICE, *DRUG administration, *DRUG delivery devices, *DRUG abuse, *LIPIDS
Abstract

For the past two decades, biomimetic high-density lipoproteins (b-HDL) have been used for various drug delivery applications. The b-HDL mimic the endogenous HDL, and therefore possess many attractive features for drug delivery, including high biocompatibility, biodegradability, and ability to transport and deliver their cargo (e.g. drugs and/or imaging agents) to specific cells and tissues that are recognized by HDL. The b-HDL designs reported in the literature often differ in size, shape, composition, and type of incorporated cargo. However, there exists only limited insight into how the b-HDL design dictates their biodistribution. To fill this gap, we conducted a comprehensive systematic literature search of biodistribution studies using various designs of apolipoprotein A-I (apoA-I)-based b-HDL (i.e. b-HDL with apoA-I, apoA-I mutants, or apoA-I mimicking peptides). We carefully screened 679 papers (search hits) for b-HDL biodistribution studies in mice, and ended up with 24 relevant biodistribution profiles that we compared according to b-HDL design. We show similarities between b-HDL biodistribution studies irrespectively of the b-HDL design, whereas the biodistribution of the b-HDL components (lipids and scaffold) differ significantly. The b-HDL lipids primarily accumulate in liver, while the b-HDL scaffold primarily accumulates in the kidney. Furthermore, both b-HDL lipids and scaffold accumulate well in the tumor tissue in tumor-bearing mice. Finally, we present essential considerations and strategies for b-HDL labeling, and discuss how the b-HDL biodistribution can be tuned through particle design and administration route. Our meta-analysis and discussions provide a detailed overview of the fate of b-HDL in mice that is highly relevant when applying b-HDL for drug delivery or in vivo imaging applications. Unlabelled Image • Biomimetic HDL (b-HDL) used for drug delivery vary in size, shape and composition • The biodistribution of the b-HDL variants is to a large extent similar • The b-HDL lipids accumulate primarily in the liver (and tumor) • The b-HDL scaffold accumulates primarily in the kidney and liver (and tumor) • The b-HDL biodistribution is tunable via particle design and administration route [ABSTRACT FROM AUTHOR]

Published
2020
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3. Deciphering the monocyte-targeting mechanisms of PEGylated cationic liposomes by investigating the biomolecular corona.

Author

Münter, Rasmus, Bak, Martin, Thomsen, Mikkel E., Parhamifar, Ladan, Stensballe, Allan, Simonsen, Jens B., Kristensen, Kasper, and Andresen, Thomas L.

Subjects
*CATIONIC lipids, *LIPOSOMES, *BLOOD proteins, *BLOOD plasma, *PROTEOGLYCANS, *CELLULAR signal transduction, *GLYCOSAMINOGLYCANS, *CD44 antigen
Abstract

[Display omitted] Cationic liposomes specifically target monocytes in blood, rendering them promising drug-delivery tools for cancer immunotherapy, vaccines, and therapies for monocytic leukaemia. The mechanism behind this monocyte targeting ability is, however, not understood, but may involve plasma proteins adsorbed on the liposomal surfaces. To shed light on this, we investigated the biomolecular corona of three different types of PEGylated cationic liposomes, finding all of them to adsorb hyaluronan-associated proteins and proteoglycans upon incubation in human blood plasma. This prompted us to study the role of the TLR4 co-receptors CD44 and CD14, both involved in signalling and uptake pathways of proteoglycans and glycosaminoglycans. We found that separate inhibition of each of these receptors hampered the monocyte uptake of the liposomes in whole human blood. Based on clues from the biomolecular corona, we have thus identified two receptors involved in the targeting and uptake of cationic liposomes in monocytes, in turn suggesting that certain proteoglycans and glycosaminoglycans may serve as monocyte-targeting opsonins. This mechanistic knowledge may pave the way for rational design of future monocyte-targeting drug-delivery platforms. [ABSTRACT FROM AUTHOR]

Published
2024
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4. The role of lipid components in lipid nanoparticles for vaccines and gene therapy.

Author

Hald Albertsen, Camilla, Kulkarni, Jayesh A., Witzigmann, Dominik, Lind, Marianne, Petersson, Karsten, and Simonsen, Jens B.

Subjects
*DNA vaccines, *GENE therapy, *LIPIDS, *NUCLEIC acids, *NANOPARTICLES
Abstract

[Display omitted] Lipid nanoparticles (LNPs) play an important role in mRNA vaccines against COVID-19. In addition, many preclinical and clinical studies, including the siRNA-LNP product, Onpattro®, highlight that LNPs unlock the potential of nucleic acid-based therapies and vaccines. To understand what is key to the success of LNPs, we need to understand the role of the building blocks that constitute them. In this Review , we discuss what each lipid component adds to the LNP delivery platform in terms of size, structure, stability, apparent pK a , nucleic acid encapsulation efficiency, cellular uptake, and endosomal escape. To explore this, we present findings from the liposome field as well as from landmark and recent articles in the LNP literature. We also discuss challenges and strategies related to in vitro/in vivo studies of LNPs based on fluorescence readouts, immunogenicity/reactogenicity, and LNP delivery beyond the liver. How these fundamental challenges are pursued, including what lipid components are added and combined, will likely determine the scope of LNP-based gene therapies and vaccines for treating various diseases. [ABSTRACT FROM AUTHOR]

Published
2022
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