Please use this identifier to cite or link to this item: https://hdl.handle.net/10356/168944
Title: Unraveling how cholesterol affects multivalency-induced membrane deformation of sub-100 nm lipid vesicles
Authors: Park, Hyeonjin
Sut, Tun Naw
Yoon, Bo Kyeong
Zhdanov, Vladimir P.
Cho, Nam-Joon
Jackman, Joshua A.
Keywords: Engineering::Materials
Issue Date: 2022
Source: Park, H., Sut, T. N., Yoon, B. K., Zhdanov, V. P., Cho, N. & Jackman, J. A. (2022). Unraveling how cholesterol affects multivalency-induced membrane deformation of sub-100 nm lipid vesicles. Langmuir, 38(51), 15950-15959. https://dx.doi.org/10.1021/acs.langmuir.2c02252
Journal: Langmuir
Abstract: Cholesterol plays a critical role in modulating the lipid membrane properties of biological and biomimetic systems and recent attention has focused on its role in the functions of sub-100 nm lipid vesicles and lipid nanoparticles. These functions often rely on multivalent ligand-receptor interactions involving membrane attachment and dynamic shape transformations while the extent to which cholesterol can influence such interaction processes is largely unknown. To address this question, herein, we investigated the attachment of sub-100 nm lipid vesicles containing varying cholesterol fractions (0-45 mol %) to membrane-mimicking supported lipid bilayer (SLB) platforms. Biotinylated lipids and streptavidin proteins were used as model ligands and receptors, respectively, while the localized surface plasmon resonance sensing technique was employed to track vesicle attachment kinetics in combination with analytical modeling of vesicle shape changes. Across various conditions mimicking low and high multivalency, our findings revealed that cholesterol-containing vesicles could bind to receptor-functionalized membranes but underwent appreciably less multivalency-induced shape deformation than vesicles without cholesterol, which can be explained by a cholesterol-mediated increase in membrane bending rigidity. Interestingly, the extent of vesicle deformation that occurred in response to increasingly strong multivalent interactions was less pronounced for vesicles with greater cholesterol fraction. The latter trend was rationalized by taking into account the strong dependence of the membrane bending energy on the area of the vesicle-SLB contact region and such insights can aid the engineering of membrane-enveloped nanoparticles with tailored biophysical properties.
URI: https://hdl.handle.net/10356/168944
ISSN: 0743-7463
DOI: 10.1021/acs.langmuir.2c02252
Schools: School of Materials Science and Engineering 
Rights: © 2022 American Chemical Society. All rights reserved.
Fulltext Permission: none
Fulltext Availability: No Fulltext
Appears in Collections:MSE Journal Articles

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