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Mechanistic aspects of maltotriose-conjugate translocation to the Gram-negative bacteria cytoplasm

Small molecule accumulation in Gram-negative bacteria is a key challenge to discover novel antibiotics, because of their two membranes and efflux pumps expelling toxic molecules. An approach to overcome this challenge is to hijack uptake pathways so that bacterial transporters shuttle the antibiotic...

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Autores principales: Dumont, Estelle, Vergalli, Julia, Pajovic, Jelena, Bhamidimarri, Satya P, Morante, Koldo, Wang, Jiajun, Lubriks, Dmitrijs, Suna, Edgars, Stavenger, Robert A, Winterhalter, Mathias, Réfrégiers, Matthieu, Pagès, Jean-Marie
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Life Science Alliance LLC 2018
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6311466/
https://www.ncbi.nlm.nih.gov/pubmed/30620010
http://dx.doi.org/10.26508/lsa.201800242
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author Dumont, Estelle
Vergalli, Julia
Pajovic, Jelena
Bhamidimarri, Satya P
Morante, Koldo
Wang, Jiajun
Lubriks, Dmitrijs
Suna, Edgars
Stavenger, Robert A
Winterhalter, Mathias
Réfrégiers, Matthieu
Pagès, Jean-Marie
author_facet Dumont, Estelle
Vergalli, Julia
Pajovic, Jelena
Bhamidimarri, Satya P
Morante, Koldo
Wang, Jiajun
Lubriks, Dmitrijs
Suna, Edgars
Stavenger, Robert A
Winterhalter, Mathias
Réfrégiers, Matthieu
Pagès, Jean-Marie
author_sort Dumont, Estelle
collection PubMed
description Small molecule accumulation in Gram-negative bacteria is a key challenge to discover novel antibiotics, because of their two membranes and efflux pumps expelling toxic molecules. An approach to overcome this challenge is to hijack uptake pathways so that bacterial transporters shuttle the antibiotic to the cytoplasm. Here, we have characterized maltodextrin–fluorophore conjugates that can pass through both the outer and inner membranes mediated by components of the Escherichia coli maltose regulon. Single-channel electrophysiology recording demonstrated that the compounds permeate across the LamB channel leading to accumulation in the periplasm. We have also demonstrated that a maltotriose conjugate distributes into both the periplasm and cytoplasm. In the cytoplasm, the molecule activates the maltose regulon and triggers the expression of maltose binding protein in the periplasmic space indicating that the complete maltose entry pathway is induced. This maltotriose conjugate can (i) reach the periplasmic and cytoplasmic compartments to significant internal concentrations and (ii) auto-induce its own entry pathway via the activation of the maltose regulon, representing an interesting prototype to deliver molecules to the cytoplasm of Gram-negative bacteria.
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spelling pubmed-63114662019-01-07 Mechanistic aspects of maltotriose-conjugate translocation to the Gram-negative bacteria cytoplasm Dumont, Estelle Vergalli, Julia Pajovic, Jelena Bhamidimarri, Satya P Morante, Koldo Wang, Jiajun Lubriks, Dmitrijs Suna, Edgars Stavenger, Robert A Winterhalter, Mathias Réfrégiers, Matthieu Pagès, Jean-Marie Life Sci Alliance Research Articles Small molecule accumulation in Gram-negative bacteria is a key challenge to discover novel antibiotics, because of their two membranes and efflux pumps expelling toxic molecules. An approach to overcome this challenge is to hijack uptake pathways so that bacterial transporters shuttle the antibiotic to the cytoplasm. Here, we have characterized maltodextrin–fluorophore conjugates that can pass through both the outer and inner membranes mediated by components of the Escherichia coli maltose regulon. Single-channel electrophysiology recording demonstrated that the compounds permeate across the LamB channel leading to accumulation in the periplasm. We have also demonstrated that a maltotriose conjugate distributes into both the periplasm and cytoplasm. In the cytoplasm, the molecule activates the maltose regulon and triggers the expression of maltose binding protein in the periplasmic space indicating that the complete maltose entry pathway is induced. This maltotriose conjugate can (i) reach the periplasmic and cytoplasmic compartments to significant internal concentrations and (ii) auto-induce its own entry pathway via the activation of the maltose regulon, representing an interesting prototype to deliver molecules to the cytoplasm of Gram-negative bacteria. Life Science Alliance LLC 2018-12-28 /pmc/articles/PMC6311466/ /pubmed/30620010 http://dx.doi.org/10.26508/lsa.201800242 Text en © 2018 Dumont et al. https://creativecommons.org/licenses/by/4.0/This article is available under a Creative Commons License (Attribution 4.0 International, as described at https://creativecommons.org/licenses/by/4.0/).
spellingShingle Research Articles
Dumont, Estelle
Vergalli, Julia
Pajovic, Jelena
Bhamidimarri, Satya P
Morante, Koldo
Wang, Jiajun
Lubriks, Dmitrijs
Suna, Edgars
Stavenger, Robert A
Winterhalter, Mathias
Réfrégiers, Matthieu
Pagès, Jean-Marie
Mechanistic aspects of maltotriose-conjugate translocation to the Gram-negative bacteria cytoplasm
title Mechanistic aspects of maltotriose-conjugate translocation to the Gram-negative bacteria cytoplasm
title_full Mechanistic aspects of maltotriose-conjugate translocation to the Gram-negative bacteria cytoplasm
title_fullStr Mechanistic aspects of maltotriose-conjugate translocation to the Gram-negative bacteria cytoplasm
title_full_unstemmed Mechanistic aspects of maltotriose-conjugate translocation to the Gram-negative bacteria cytoplasm
title_short Mechanistic aspects of maltotriose-conjugate translocation to the Gram-negative bacteria cytoplasm
title_sort mechanistic aspects of maltotriose-conjugate translocation to the gram-negative bacteria cytoplasm
topic Research Articles
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6311466/
https://www.ncbi.nlm.nih.gov/pubmed/30620010
http://dx.doi.org/10.26508/lsa.201800242
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