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Nanoprobes to investigate nonspecific interactions in lipid bilayers: from defect-mediated adhesion to membrane disruption

When a lipid membrane approaches a material/nanomaterial, nonspecific adhesion may occur. The interactions responsible for nonspecific adhesion can either preserve the membrane integrity or lead to its disruption. Despite the importance of the phenomenon, there is still a lack of clear understanding...

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Autores principales: Razza, Nicolò, Lavino, Alessio D., Fadda, Giulia, Lairez, Didier, Impagnatiello, Andrea, Marchisio, Daniele, Sangermano, Marco, Rizza, Giancarlo
Formato: Online Artículo Texto
Lenguaje:English
Publicado: RSC 2021
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9418973/
https://www.ncbi.nlm.nih.gov/pubmed/36132337
http://dx.doi.org/10.1039/d1na00360g
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author Razza, Nicolò
Lavino, Alessio D.
Fadda, Giulia
Lairez, Didier
Impagnatiello, Andrea
Marchisio, Daniele
Sangermano, Marco
Rizza, Giancarlo
author_facet Razza, Nicolò
Lavino, Alessio D.
Fadda, Giulia
Lairez, Didier
Impagnatiello, Andrea
Marchisio, Daniele
Sangermano, Marco
Rizza, Giancarlo
author_sort Razza, Nicolò
collection PubMed
description When a lipid membrane approaches a material/nanomaterial, nonspecific adhesion may occur. The interactions responsible for nonspecific adhesion can either preserve the membrane integrity or lead to its disruption. Despite the importance of the phenomenon, there is still a lack of clear understanding of how and why nonspecific adhesion may originate different resulting scenarios and how these interaction scenarios can be investigated. This work aims at bridging this gap by investigating the role of the interplay between cationic electrostatic and hydrophobic interactions in modulating the membrane stability during nonspecific adhesion phenomena. Here, the stability of the membrane has been studied employing anisotropic nanoprobes in zwitterionic lipid membranes with the support of coarse-grained molecular dynamics simulations to interpret the experimental observations. Lipid membrane electrical measurements and nanoscale visualization in combination with molecular dynamics simulations revealed the phenomena driving nonspecific adhesion. Any interaction with the lipidic bilayer is defect-mediated involving cationic electrostatically driven lipid extraction and hydrophobically-driven chain protrusion, whose interplay determines the existence of a thermodynamic optimum for the membrane structural integrity. These findings unlock unexplored routes to exploit nonspecific adhesion in lipid membranes. The proposed platform can act as a straightforward probing tool to locally investigate interactions between synthetic materials and lipid membranes for the design of antibacterials, antivirals, and scaffolds for tissue engineering.
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spelling pubmed-94189732022-09-20 Nanoprobes to investigate nonspecific interactions in lipid bilayers: from defect-mediated adhesion to membrane disruption Razza, Nicolò Lavino, Alessio D. Fadda, Giulia Lairez, Didier Impagnatiello, Andrea Marchisio, Daniele Sangermano, Marco Rizza, Giancarlo Nanoscale Adv Chemistry When a lipid membrane approaches a material/nanomaterial, nonspecific adhesion may occur. The interactions responsible for nonspecific adhesion can either preserve the membrane integrity or lead to its disruption. Despite the importance of the phenomenon, there is still a lack of clear understanding of how and why nonspecific adhesion may originate different resulting scenarios and how these interaction scenarios can be investigated. This work aims at bridging this gap by investigating the role of the interplay between cationic electrostatic and hydrophobic interactions in modulating the membrane stability during nonspecific adhesion phenomena. Here, the stability of the membrane has been studied employing anisotropic nanoprobes in zwitterionic lipid membranes with the support of coarse-grained molecular dynamics simulations to interpret the experimental observations. Lipid membrane electrical measurements and nanoscale visualization in combination with molecular dynamics simulations revealed the phenomena driving nonspecific adhesion. Any interaction with the lipidic bilayer is defect-mediated involving cationic electrostatically driven lipid extraction and hydrophobically-driven chain protrusion, whose interplay determines the existence of a thermodynamic optimum for the membrane structural integrity. These findings unlock unexplored routes to exploit nonspecific adhesion in lipid membranes. The proposed platform can act as a straightforward probing tool to locally investigate interactions between synthetic materials and lipid membranes for the design of antibacterials, antivirals, and scaffolds for tissue engineering. RSC 2021-07-08 /pmc/articles/PMC9418973/ /pubmed/36132337 http://dx.doi.org/10.1039/d1na00360g Text en This journal is © The Royal Society of Chemistry https://creativecommons.org/licenses/by-nc/3.0/
spellingShingle Chemistry
Razza, Nicolò
Lavino, Alessio D.
Fadda, Giulia
Lairez, Didier
Impagnatiello, Andrea
Marchisio, Daniele
Sangermano, Marco
Rizza, Giancarlo
Nanoprobes to investigate nonspecific interactions in lipid bilayers: from defect-mediated adhesion to membrane disruption
title Nanoprobes to investigate nonspecific interactions in lipid bilayers: from defect-mediated adhesion to membrane disruption
title_full Nanoprobes to investigate nonspecific interactions in lipid bilayers: from defect-mediated adhesion to membrane disruption
title_fullStr Nanoprobes to investigate nonspecific interactions in lipid bilayers: from defect-mediated adhesion to membrane disruption
title_full_unstemmed Nanoprobes to investigate nonspecific interactions in lipid bilayers: from defect-mediated adhesion to membrane disruption
title_short Nanoprobes to investigate nonspecific interactions in lipid bilayers: from defect-mediated adhesion to membrane disruption
title_sort nanoprobes to investigate nonspecific interactions in lipid bilayers: from defect-mediated adhesion to membrane disruption
topic Chemistry
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9418973/
https://www.ncbi.nlm.nih.gov/pubmed/36132337
http://dx.doi.org/10.1039/d1na00360g
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