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Dual-Uptake Mode of the Antibiotic Phazolicin Prevents Resistance Acquisition by Gram-Negative Bacteria

Phazolicin (PHZ) is a peptide antibiotic exhibiting narrow-spectrum activity against rhizobia closely related to its producer, Rhizobium sp. strain Pop5. Here, we show that the frequency of spontaneous PHZ-resistant mutants in Sinorhizobium meliloti is below the detection limit. We find that PHZ can...

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Autores principales: Travin, Dmitrii Y., Jouan, Romain, Vigouroux, Armelle, Inaba-Inoue, Satomi, Lachat, Joy, Haq, Fazal, Timchenko, Tatiana, Sutormin, Dmitry, Dubiley, Svetlana, Beis, Konstantinos, Moréra, Solange, Severinov, Konstantin, Mergaert, Peter
Formato: Online Artículo Texto
Lenguaje:English
Publicado: American Society for Microbiology 2023
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC10128002/
https://www.ncbi.nlm.nih.gov/pubmed/36802165
http://dx.doi.org/10.1128/mbio.00217-23
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author Travin, Dmitrii Y.
Jouan, Romain
Vigouroux, Armelle
Inaba-Inoue, Satomi
Lachat, Joy
Haq, Fazal
Timchenko, Tatiana
Sutormin, Dmitry
Dubiley, Svetlana
Beis, Konstantinos
Moréra, Solange
Severinov, Konstantin
Mergaert, Peter
author_facet Travin, Dmitrii Y.
Jouan, Romain
Vigouroux, Armelle
Inaba-Inoue, Satomi
Lachat, Joy
Haq, Fazal
Timchenko, Tatiana
Sutormin, Dmitry
Dubiley, Svetlana
Beis, Konstantinos
Moréra, Solange
Severinov, Konstantin
Mergaert, Peter
author_sort Travin, Dmitrii Y.
collection PubMed
description Phazolicin (PHZ) is a peptide antibiotic exhibiting narrow-spectrum activity against rhizobia closely related to its producer, Rhizobium sp. strain Pop5. Here, we show that the frequency of spontaneous PHZ-resistant mutants in Sinorhizobium meliloti is below the detection limit. We find that PHZ can enter S. meliloti cells through two distinct promiscuous peptide transporters, BacA and YejABEF, which belong to the SLiPT (SbmA-like peptide transporter) and ABC (ATP-binding cassette) transporter families, respectively. The dual-uptake mode explains the lack of observed resistance acquisition because the simultaneous inactivation of both transporters is necessary for resistance to PHZ. Since both BacA and YejABEF are essential for the development of functional symbiosis of S. meliloti with leguminous plants, the unlikely acquisition of PHZ resistance via the inactivation of these transporters is further disfavored. A whole-genome transposon sequencing screen did not reveal additional genes that can provide strong PHZ resistance when inactivated. However, it was found that the capsular polysaccharide KPS, the novel putative envelope polysaccharide PPP (PHZ-protecting polysaccharide), as well as the peptidoglycan layer jointly contribute to the sensitivity of S. meliloti to PHZ, most likely serving as barriers that reduce the amount of PHZ transported inside the cell.
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spelling pubmed-101280022023-04-26 Dual-Uptake Mode of the Antibiotic Phazolicin Prevents Resistance Acquisition by Gram-Negative Bacteria Travin, Dmitrii Y. Jouan, Romain Vigouroux, Armelle Inaba-Inoue, Satomi Lachat, Joy Haq, Fazal Timchenko, Tatiana Sutormin, Dmitry Dubiley, Svetlana Beis, Konstantinos Moréra, Solange Severinov, Konstantin Mergaert, Peter mBio Research Article Phazolicin (PHZ) is a peptide antibiotic exhibiting narrow-spectrum activity against rhizobia closely related to its producer, Rhizobium sp. strain Pop5. Here, we show that the frequency of spontaneous PHZ-resistant mutants in Sinorhizobium meliloti is below the detection limit. We find that PHZ can enter S. meliloti cells through two distinct promiscuous peptide transporters, BacA and YejABEF, which belong to the SLiPT (SbmA-like peptide transporter) and ABC (ATP-binding cassette) transporter families, respectively. The dual-uptake mode explains the lack of observed resistance acquisition because the simultaneous inactivation of both transporters is necessary for resistance to PHZ. Since both BacA and YejABEF are essential for the development of functional symbiosis of S. meliloti with leguminous plants, the unlikely acquisition of PHZ resistance via the inactivation of these transporters is further disfavored. A whole-genome transposon sequencing screen did not reveal additional genes that can provide strong PHZ resistance when inactivated. However, it was found that the capsular polysaccharide KPS, the novel putative envelope polysaccharide PPP (PHZ-protecting polysaccharide), as well as the peptidoglycan layer jointly contribute to the sensitivity of S. meliloti to PHZ, most likely serving as barriers that reduce the amount of PHZ transported inside the cell. American Society for Microbiology 2023-02-21 /pmc/articles/PMC10128002/ /pubmed/36802165 http://dx.doi.org/10.1128/mbio.00217-23 Text en Copyright © 2023 Travin et al. https://creativecommons.org/licenses/by/4.0/This is an open-access article distributed under the terms of the Creative Commons Attribution 4.0 International license (https://creativecommons.org/licenses/by/4.0/) .
spellingShingle Research Article
Travin, Dmitrii Y.
Jouan, Romain
Vigouroux, Armelle
Inaba-Inoue, Satomi
Lachat, Joy
Haq, Fazal
Timchenko, Tatiana
Sutormin, Dmitry
Dubiley, Svetlana
Beis, Konstantinos
Moréra, Solange
Severinov, Konstantin
Mergaert, Peter
Dual-Uptake Mode of the Antibiotic Phazolicin Prevents Resistance Acquisition by Gram-Negative Bacteria
title Dual-Uptake Mode of the Antibiotic Phazolicin Prevents Resistance Acquisition by Gram-Negative Bacteria
title_full Dual-Uptake Mode of the Antibiotic Phazolicin Prevents Resistance Acquisition by Gram-Negative Bacteria
title_fullStr Dual-Uptake Mode of the Antibiotic Phazolicin Prevents Resistance Acquisition by Gram-Negative Bacteria
title_full_unstemmed Dual-Uptake Mode of the Antibiotic Phazolicin Prevents Resistance Acquisition by Gram-Negative Bacteria
title_short Dual-Uptake Mode of the Antibiotic Phazolicin Prevents Resistance Acquisition by Gram-Negative Bacteria
title_sort dual-uptake mode of the antibiotic phazolicin prevents resistance acquisition by gram-negative bacteria
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC10128002/
https://www.ncbi.nlm.nih.gov/pubmed/36802165
http://dx.doi.org/10.1128/mbio.00217-23
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