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The battle for silver binding: How the interplay between the SilE, SilF, and SilB proteins contributes to the silver efflux pump mechanism

The resistance of gram-negative bacteria to silver ions is mediated by a silver efflux pump, which mainly relies on a tripartite efflux complex SilCBA, a metallochaperone SilF and an intrinsically disordered protein SilE. However, the precise mechanism by which silver ions are extruded from the cell...

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Autores principales: Arrault, Cyrielle, Monneau, Yoan Rocky, Martin, Marie, Cantrelle, François-Xavier, Boll, Emmanuelle, Chirot, Fabien, Comby Zerbino, Clothilde, Walker, Olivier, Hologne, Maggy
Formato: Online Artículo Texto
Lenguaje:English
Publicado: American Society for Biochemistry and Molecular Biology 2023
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC10407283/
https://www.ncbi.nlm.nih.gov/pubmed/37394004
http://dx.doi.org/10.1016/j.jbc.2023.105004
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author Arrault, Cyrielle
Monneau, Yoan Rocky
Martin, Marie
Cantrelle, François-Xavier
Boll, Emmanuelle
Chirot, Fabien
Comby Zerbino, Clothilde
Walker, Olivier
Hologne, Maggy
author_facet Arrault, Cyrielle
Monneau, Yoan Rocky
Martin, Marie
Cantrelle, François-Xavier
Boll, Emmanuelle
Chirot, Fabien
Comby Zerbino, Clothilde
Walker, Olivier
Hologne, Maggy
author_sort Arrault, Cyrielle
collection PubMed
description The resistance of gram-negative bacteria to silver ions is mediated by a silver efflux pump, which mainly relies on a tripartite efflux complex SilCBA, a metallochaperone SilF and an intrinsically disordered protein SilE. However, the precise mechanism by which silver ions are extruded from the cell and the different roles of SilB, SilF, and SilE remain poorly understood. To address these questions, we employed nuclear magnetic resonance and mass spectrometry to investigate the interplay between these proteins. We first solved the solution structures of SilF in its free and Ag(+)-bound forms, and we demonstrated that SilB exhibits two silver binding sites in its N and C termini. Conversely to the homologous Cus system, we determined that SilF and SilB interact without the presence of silver ions and that the rate of silver dissociation is eight times faster when SilF is bound to SilB, indicating the formation of a SilF–Ag–SilB intermediate complex. Finally, we have shown that SilE does not bind to either SilF or SilB, regardless of the presence or absence of silver ions, further corroborating that it merely acts as a regulator that prevents the cell from being overloaded with silver. Collectively, we have provided further insights into protein interactions within the sil system that contribute to bacterial resistance to silver ions.
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spelling pubmed-104072832023-08-09 The battle for silver binding: How the interplay between the SilE, SilF, and SilB proteins contributes to the silver efflux pump mechanism Arrault, Cyrielle Monneau, Yoan Rocky Martin, Marie Cantrelle, François-Xavier Boll, Emmanuelle Chirot, Fabien Comby Zerbino, Clothilde Walker, Olivier Hologne, Maggy J Biol Chem Research Article The resistance of gram-negative bacteria to silver ions is mediated by a silver efflux pump, which mainly relies on a tripartite efflux complex SilCBA, a metallochaperone SilF and an intrinsically disordered protein SilE. However, the precise mechanism by which silver ions are extruded from the cell and the different roles of SilB, SilF, and SilE remain poorly understood. To address these questions, we employed nuclear magnetic resonance and mass spectrometry to investigate the interplay between these proteins. We first solved the solution structures of SilF in its free and Ag(+)-bound forms, and we demonstrated that SilB exhibits two silver binding sites in its N and C termini. Conversely to the homologous Cus system, we determined that SilF and SilB interact without the presence of silver ions and that the rate of silver dissociation is eight times faster when SilF is bound to SilB, indicating the formation of a SilF–Ag–SilB intermediate complex. Finally, we have shown that SilE does not bind to either SilF or SilB, regardless of the presence or absence of silver ions, further corroborating that it merely acts as a regulator that prevents the cell from being overloaded with silver. Collectively, we have provided further insights into protein interactions within the sil system that contribute to bacterial resistance to silver ions. American Society for Biochemistry and Molecular Biology 2023-07-01 /pmc/articles/PMC10407283/ /pubmed/37394004 http://dx.doi.org/10.1016/j.jbc.2023.105004 Text en © 2023 The Authors https://creativecommons.org/licenses/by-nc-nd/4.0/This is an open access article under the CC BY-NC-ND license (http://creativecommons.org/licenses/by-nc-nd/4.0/).
spellingShingle Research Article
Arrault, Cyrielle
Monneau, Yoan Rocky
Martin, Marie
Cantrelle, François-Xavier
Boll, Emmanuelle
Chirot, Fabien
Comby Zerbino, Clothilde
Walker, Olivier
Hologne, Maggy
The battle for silver binding: How the interplay between the SilE, SilF, and SilB proteins contributes to the silver efflux pump mechanism
title The battle for silver binding: How the interplay between the SilE, SilF, and SilB proteins contributes to the silver efflux pump mechanism
title_full The battle for silver binding: How the interplay between the SilE, SilF, and SilB proteins contributes to the silver efflux pump mechanism
title_fullStr The battle for silver binding: How the interplay between the SilE, SilF, and SilB proteins contributes to the silver efflux pump mechanism
title_full_unstemmed The battle for silver binding: How the interplay between the SilE, SilF, and SilB proteins contributes to the silver efflux pump mechanism
title_short The battle for silver binding: How the interplay between the SilE, SilF, and SilB proteins contributes to the silver efflux pump mechanism
title_sort battle for silver binding: how the interplay between the sile, silf, and silb proteins contributes to the silver efflux pump mechanism
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC10407283/
https://www.ncbi.nlm.nih.gov/pubmed/37394004
http://dx.doi.org/10.1016/j.jbc.2023.105004
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