Loss of YhcB results in dysregulation of coordinated peptidoglycan, LPS and phospholipid synthesis during Escherichia coli cell growth

The cell envelope is essential for viability in all domains of life. It retains enzymes and substrates within a confined space while providing a protective barrier to the external environment. Destabilising the envelope of bacterial pathogens is a common strategy employed by antimicrobial treatment....

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Autores principales: Goodall, Emily C. A., Isom, Georgia L., Rooke, Jessica L., Pullela, Karthik, Icke, Christopher, Yang, Zihao, Boelter, Gabriela, Jones, Alun, Warner, Isabel, Da Costa, Rochelle, Zhang, Bing, Rae, James, Tan, Wee Boon, Winkle, Matthias, Delhaye, Antoine, Heinz, Eva, Collet, Jean-Francois, Cunningham, Adam F., Blaskovich, Mark A., Parton, Robert G., Cole, Jeff A., Banzhaf, Manuel, Chng, Shu-Sin, Vollmer, Waldemar, Bryant, Jack A., Henderson, Ian R.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Public Library of Science 2021
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8741058/
https://www.ncbi.nlm.nih.gov/pubmed/34941903
http://dx.doi.org/10.1371/journal.pgen.1009586
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author Goodall, Emily C. A.
Isom, Georgia L.
Rooke, Jessica L.
Pullela, Karthik
Icke, Christopher
Yang, Zihao
Boelter, Gabriela
Jones, Alun
Warner, Isabel
Da Costa, Rochelle
Zhang, Bing
Rae, James
Tan, Wee Boon
Winkle, Matthias
Delhaye, Antoine
Heinz, Eva
Collet, Jean-Francois
Cunningham, Adam F.
Blaskovich, Mark A.
Parton, Robert G.
Cole, Jeff A.
Banzhaf, Manuel
Chng, Shu-Sin
Vollmer, Waldemar
Bryant, Jack A.
Henderson, Ian R.
author_facet Goodall, Emily C. A.
Isom, Georgia L.
Rooke, Jessica L.
Pullela, Karthik
Icke, Christopher
Yang, Zihao
Boelter, Gabriela
Jones, Alun
Warner, Isabel
Da Costa, Rochelle
Zhang, Bing
Rae, James
Tan, Wee Boon
Winkle, Matthias
Delhaye, Antoine
Heinz, Eva
Collet, Jean-Francois
Cunningham, Adam F.
Blaskovich, Mark A.
Parton, Robert G.
Cole, Jeff A.
Banzhaf, Manuel
Chng, Shu-Sin
Vollmer, Waldemar
Bryant, Jack A.
Henderson, Ian R.
author_sort Goodall, Emily C. A.
collection PubMed
description The cell envelope is essential for viability in all domains of life. It retains enzymes and substrates within a confined space while providing a protective barrier to the external environment. Destabilising the envelope of bacterial pathogens is a common strategy employed by antimicrobial treatment. However, even in one of the best studied organisms, Escherichia coli, there remain gaps in our understanding of how the synthesis of the successive layers of the cell envelope are coordinated during growth and cell division. Here, we used a whole-genome phenotypic screen to identify mutants with a defective cell envelope. We report that loss of yhcB, a conserved gene of unknown function, results in loss of envelope stability, increased cell permeability and dysregulated control of cell size. Using whole genome transposon mutagenesis strategies, we report the comprehensive genetic interaction network of yhcB, revealing all genes with a synthetic negative and a synthetic positive relationship. These genes include those previously reported to have a role in cell envelope biogenesis. Surprisingly, we identified genes previously annotated as essential that became non-essential in a ΔyhcB background. Subsequent analyses suggest that YhcB functions at the junction of several envelope biosynthetic pathways coordinating the spatiotemporal growth of the cell, highlighting YhcB as an as yet unexplored antimicrobial target.
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spelling pubmed-87410582022-01-08 Loss of YhcB results in dysregulation of coordinated peptidoglycan, LPS and phospholipid synthesis during Escherichia coli cell growth Goodall, Emily C. A. Isom, Georgia L. Rooke, Jessica L. Pullela, Karthik Icke, Christopher Yang, Zihao Boelter, Gabriela Jones, Alun Warner, Isabel Da Costa, Rochelle Zhang, Bing Rae, James Tan, Wee Boon Winkle, Matthias Delhaye, Antoine Heinz, Eva Collet, Jean-Francois Cunningham, Adam F. Blaskovich, Mark A. Parton, Robert G. Cole, Jeff A. Banzhaf, Manuel Chng, Shu-Sin Vollmer, Waldemar Bryant, Jack A. Henderson, Ian R. PLoS Genet Research Article The cell envelope is essential for viability in all domains of life. It retains enzymes and substrates within a confined space while providing a protective barrier to the external environment. Destabilising the envelope of bacterial pathogens is a common strategy employed by antimicrobial treatment. However, even in one of the best studied organisms, Escherichia coli, there remain gaps in our understanding of how the synthesis of the successive layers of the cell envelope are coordinated during growth and cell division. Here, we used a whole-genome phenotypic screen to identify mutants with a defective cell envelope. We report that loss of yhcB, a conserved gene of unknown function, results in loss of envelope stability, increased cell permeability and dysregulated control of cell size. Using whole genome transposon mutagenesis strategies, we report the comprehensive genetic interaction network of yhcB, revealing all genes with a synthetic negative and a synthetic positive relationship. These genes include those previously reported to have a role in cell envelope biogenesis. Surprisingly, we identified genes previously annotated as essential that became non-essential in a ΔyhcB background. Subsequent analyses suggest that YhcB functions at the junction of several envelope biosynthetic pathways coordinating the spatiotemporal growth of the cell, highlighting YhcB as an as yet unexplored antimicrobial target. Public Library of Science 2021-12-23 /pmc/articles/PMC8741058/ /pubmed/34941903 http://dx.doi.org/10.1371/journal.pgen.1009586 Text en © 2021 Goodall et al https://creativecommons.org/licenses/by/4.0/This is an open access article distributed under the terms of the Creative Commons Attribution License (https://creativecommons.org/licenses/by/4.0/) , which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are credited.
spellingShingle Research Article
Goodall, Emily C. A.
Isom, Georgia L.
Rooke, Jessica L.
Pullela, Karthik
Icke, Christopher
Yang, Zihao
Boelter, Gabriela
Jones, Alun
Warner, Isabel
Da Costa, Rochelle
Zhang, Bing
Rae, James
Tan, Wee Boon
Winkle, Matthias
Delhaye, Antoine
Heinz, Eva
Collet, Jean-Francois
Cunningham, Adam F.
Blaskovich, Mark A.
Parton, Robert G.
Cole, Jeff A.
Banzhaf, Manuel
Chng, Shu-Sin
Vollmer, Waldemar
Bryant, Jack A.
Henderson, Ian R.
Loss of YhcB results in dysregulation of coordinated peptidoglycan, LPS and phospholipid synthesis during Escherichia coli cell growth
title Loss of YhcB results in dysregulation of coordinated peptidoglycan, LPS and phospholipid synthesis during Escherichia coli cell growth
title_full Loss of YhcB results in dysregulation of coordinated peptidoglycan, LPS and phospholipid synthesis during Escherichia coli cell growth
title_fullStr Loss of YhcB results in dysregulation of coordinated peptidoglycan, LPS and phospholipid synthesis during Escherichia coli cell growth
title_full_unstemmed Loss of YhcB results in dysregulation of coordinated peptidoglycan, LPS and phospholipid synthesis during Escherichia coli cell growth
title_short Loss of YhcB results in dysregulation of coordinated peptidoglycan, LPS and phospholipid synthesis during Escherichia coli cell growth
title_sort loss of yhcb results in dysregulation of coordinated peptidoglycan, lps and phospholipid synthesis during escherichia coli cell growth
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8741058/
https://www.ncbi.nlm.nih.gov/pubmed/34941903
http://dx.doi.org/10.1371/journal.pgen.1009586
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