Micellization of Lipopeptides Containing Toll-like Receptor Agonist and Integrin Binding Sequences

Short bioactive peptide sequences are of great interest in biomaterials development. We investigate the self-assembly of a lipopeptide containing both the highly cationic CSK4 toll-like receptor agonist hexapeptide sequence and RGDS integrin-binding motif, i.e., C16-CSK4RGDS, as well as the control...

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Bibliographic Details
Published in:ACS applied materials & interfaces 2024-12, Vol.16 (50), p.68713-68723
Main Authors: Castelletto, Valeria, de Mello, Lucas R., Seitsonen, Jani, Hamley, Ian W.
Format: Article
Language:English
Subjects:
Animals
Forum
Humans
Integrins - agonists
Integrins - chemistry
Integrins - metabolism
Lipopeptides - chemistry
Lipopeptides - pharmacology
Micelles
Molecular Dynamics Simulation
Oligopeptides - chemistry
Oligopeptides - pharmacology
Toll-Like Receptor Agonists
Toll-Like Receptors - agonists
Toll-Like Receptors - chemistry
Toll-Like Receptors - metabolism
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Summary:Short bioactive peptide sequences are of great interest in biomaterials development. We investigate the self-assembly of a lipopeptide containing both the highly cationic CSK4 toll-like receptor agonist hexapeptide sequence and RGDS integrin-binding motif, i.e., C16-CSK4RGDS, as well as the control containing a scrambled terminal sequence C16-CSK4GRDS. Both lipopeptides are found to form micelles, as revealed by small-angle X-ray scattering and cryogenic transmission electron microscopy, and modeled using atomistic molecular dynamics simulations. We carefully examined methods to probe the aggregation of the molecules, i.e. to obtain the critical micelle concentration (CMC). Fluorescent probe assays using 1-anilino-8-naphthalenesulfonate (ANS) reveal low CMC values, 1–2 μM, which contrast with consistent values more than 2 orders of magnitude larger obtained from surface tension and electrical conductivity as well as unexpected UV/vis absorption spectra discontinuities and fluoresccence probe assays using Nile red. The anomalous results obtained from an ANS fluorescence probe are ascribed to the effect of ANS binding to the cationic (lysine and arginine) residues in the lipopeptide, which leads to a conformational change, as shown by circular dichroism, even at low concentrations below the actual CMC. Despite the small change in the peptide sequence (swapping of G and R residues), there is surprisingly a significant difference in the aggregation propensity and association number, both of which are greater for C16-CSK4GRDS. Both lipopeptides are cytocompatible (with fibroblasts and myoblasts) at low concentration, although cytotoxicity is noted at higher concentration.
ISSN:1944-8244
1944-8252
1944-8252
DOI:10.1021/acsami.4c18165