Modulating Noncovalent and Covalent Forces to Control Inverse Phosphocholine Lipid Self-Assembly on Inorganic Surfaces

07 March 2022, Version 1
This content is a preprint and has not undergone peer review at the time of posting.

Abstract

While noncovalent forces typically drive lipid vesicle adsorption and rupture to form supported lipid bilayer (SLB) coatings on inorganic surfaces, this strategy only works on a few materials with suitable energetics such as SiO2. The use of coordination chemistry between inverse-phosphocholine (PC) lipid headgroups and surfaces has emerged as a promising strategy to enable SLB formation on other materials such as TiO2 based on covalent forces. However, until now, a cohesive picture of how noncovalent and covalent forces jointly contribute to the latter SLB formation process has been lacking. Herein, we investigated inverse-PC lipid vesicle adsorption onto TiO2 and SiO2 surfaces and discovered how adsorption pathways can be controlled by tuning the balance of noncovalent and covalent forces. On TiO2, SLB formation depended on two key factors: (1) favorable noncovalent forces to facilitate initial vesicle adsorption; and (2) a critical density of lipid-TiO2 coordinate bonds to enable sufficient vesicle deformation triggering fusion and rupture. In other cases, either no adsorption or intact vesicle adsorption without rupture occurred even when coordinate bonds were present. Conversely, on SiO2, conditions were identified to support inverse-PC lipid adsorption whereas vesicles were repelled otherwise. The experimental results were supported by interfacial force modeling and our findings demonstrate how a subtle interplay of noncovalent and covalent forces plays a deterministic role in modulating lipid self-assembly pathways.

Keywords

vesicle
adsorption
supported lipid bilayer
phospholipid
noncovalent
coordinate bonding
interfacial forces

Supplementary materials

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Supporting Information
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Additional experimental details and results, including materials and methods, vesicle size and zeta potential characterization, and analysis of vesicle deformation as well as details of interfacial force modeling calculations.
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