Issue 30, 2024

Fragment-based approach to study fungicide-biomimetic membrane interactions

Abstract

In this study, the molecular interactions of the allylamine-type fungicide butenafine and a set of substructures (“fragments”) with liposomes mimicking biological membranes were studied to gain a better understanding of the structural factors governing membrane affinity and perturbation. Specifically, drug/fragment-membrane interactions were investigated using an interdisciplinary approach involving micro differential scanning calorimetry, open-tubular capillary electrochromatography, nanoplasmonic sensing, and quartz crystal microbalance. By incubating the drug and the fragment compounds with liposomes with varying lipid composition or by externally adding the compounds to preformed liposomes, a detailed mechanistic picture on the underlying drug/fragment-membrane interactions was obtained. The nature and the degree of ionisation of polar head groups of the lipids had a major influence on the nature of drug-membrane interactions, and so had the presence and relative concentration of cholesterol within the membranes. The in-depth understanding of drug/fragment-membranes interactions established by the presented interdisciplinary fragment-based approach may be useful in guiding the design and early-stage evaluation of prospective antifungal drug candidates, and the discovery of agents with improved membrane penetrating characteristics in general.

Graphical abstract: Fragment-based approach to study fungicide-biomimetic membrane interactions

Supplementary files

Article information

Article type
Paper
Submitted
28 May 2024
Accepted
10 Jul 2024
First published
10 Jul 2024
This article is Open Access
Creative Commons BY license

Soft Matter, 2024,20, 5954-5968

Fragment-based approach to study fungicide-biomimetic membrane interactions

S. Jaikishan, M. Lavainne, H. K. Ravald, K. Scobbie, F. Dusa, R. Maheswari, J. Turpeinen, I. Eikemans, R. Chen, J. Rantala, V. Aseyev, N. N. Maier and S. K. Wiedmer, Soft Matter, 2024, 20, 5954 DOI: 10.1039/D4SM00648H

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