A Label‐Free Multitechnique Approach to Characterize the Interaction of Bioactive Compounds with Biomimetic Interfaces

Author:

Fernandes Eduarda1ORCID,Costa Rui R.2ORCID,Machado Raúl3ORCID,Reis Rui L.2ORCID,Pashkuleva Iva2ORCID,Lúcio Marlene4ORCID

Affiliation:

1. CF‐UM‐UP Centro de Física das Universidades do Minho e Porto Universidade do Minho 4710‐057 Braga Portugal

2. 3B's Research Group, I3Bs – Research Institute on Biomaterials, Biodegradables and Biomimetics University of Minho, Headquarters of the European Institute of Excellence on Tissue Engineering and Regenerative Medicine, AvePark, Parque de Ciência e Tecnologia, and ICVS/3B's, PT Government Associate Laboratory 4805‐017 Braga/Guimarães Portugal

3. CBMA Centro de Biologia Molecular e Ambiental/Aquatic Research Network (ARNET) Associate Laboratory, and IB‐S, Institute of Science and Innovation for Bio‐Sustainability Universidade do Minho Campus de Gualtar 4710‐057 Braga Portugal

4. CF‐UM‐UP, Centro de Física das Universidades do Minho e Porto, and CBMA Centro de Biologia Molecular e Ambiental Universidade do Minho 4710‐057 Braga Portugal

Abstract

Extensive research has been conducted on biomimetic interfaces mimicking the complex and diverse microenvironment of cell membranes to gain insights into bioactive compound interactions and membrane biophysics modulation. The present study proposes an innovative approach that combines five prospective label‐free methodologies (derivative spectroscopy, synchrotron small‐ and wide‐angle X‐Ray scattering, attenuated total reflection–Fourier‐transform infrared spectroscopy, quartz‐crystal microbalance with dissipation, and surface plasmon resonance) to showcase their synergistic capabilities and complementarity in investigating drug–membrane interactions. This multitechnique approach combines the real‐time monitoring of the adsorption process under continuous flow conditions with the steady‐state perspective of this process. As a proof of concept, the interaction of three bioactive compounds (caffeine, testosterone, and diclofenac) with two biomimetic membrane interfaces (multistacked lipid bilayers and supported lipid bilayers) mimicking the more ordered lipid transient phases, with and without cholesterol (lo and so), that are responsible for a variety of membrane‐associated biological activities, is investigated. The biophysical effects of the bioactives are discussed using complementary data from real‐time and steady‐state experiments, including membrane adsorption and distribution, predicted location, and induced changes in order and fluidity, encompassing bilayer thickness, hydration, and area per lipid molecule.

Funder

Fundação para a Ciência e a Tecnologia

Central European Research Infrastructure Consortium

European Regional Development Fund

Publisher

Wiley

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