A Novel Growth-Based Selection Strategy Identifies New Constitutively Active Variants of the Major Virulence Regulator PrfA in Listeria monocytogenes

Listeria monocytogenes is a Gram-positive pathogen able to cause severe human infections. Its major virulence regulator is the transcriptional activator PrfA, a member of the Crp/Fnr family of transcriptional regulators. To establish a successful L. monocytogenes infection, the PrfA protein needs to...

Descripción completa

Detalles Bibliográficos
Autores principales: Hansen, Sabine, Hall, Michael, Grundström, Christin, Brännström, Kristoffer, Sauer-Eriksson, A. Elisabeth, Johansson, Jörgen
Formato: Online Artículo Texto
Lenguaje:English
Publicado: American Society for Microbiology 2020
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7221254/
https://www.ncbi.nlm.nih.gov/pubmed/32179627
http://dx.doi.org/10.1128/JB.00115-20
_version_ 1783533333344419840
author Hansen, Sabine
Hall, Michael
Grundström, Christin
Brännström, Kristoffer
Sauer-Eriksson, A. Elisabeth
Johansson, Jörgen
author_facet Hansen, Sabine
Hall, Michael
Grundström, Christin
Brännström, Kristoffer
Sauer-Eriksson, A. Elisabeth
Johansson, Jörgen
author_sort Hansen, Sabine
collection PubMed
description Listeria monocytogenes is a Gram-positive pathogen able to cause severe human infections. Its major virulence regulator is the transcriptional activator PrfA, a member of the Crp/Fnr family of transcriptional regulators. To establish a successful L. monocytogenes infection, the PrfA protein needs to be in an active conformation, either by binding the cognate inducer glutathione (GSH) or by possessing amino acid substitutions rendering the protein constitutively active (PrfA*). By a yet unknown mechanism, phosphotransferase system (PTS) sugars repress the activity of PrfA. We therefore took a transposon-based approach to identify the mechanism by which PTS sugars repress PrfA activity. For this, we screened a transposon mutant bank to identify clones able to grow in the presence of glucose-6-phosphate as the sole carbon source. Surprisingly, most of the isolated transposon mutants also carried amino acid substitutions in PrfA. In transposon-free strains, the PrfA amino acid substitution mutants displayed growth, virulence factor expression, infectivity, and DNA binding, agreeing with previously identified PrfA* mutants. Hence, the initial growth phenotype observed in the isolated clone was due to the amino acid substitution in PrfA and unrelated to the loci inactivated by the transposon mutant. Finally, we provide structural evidence for the existence of an intermediately activated PrfA state, which gives new insights into PrfA protein activation. IMPORTANCE The Gram-positive bacterium Listeria monocytogenes is a human pathogen affecting mainly the elderly, immunocompromised people, and pregnant women. It can lead to meningoencephalitis, septicemia, and abortion. The major virulence regulator in L. monocytogenes is the PrfA protein, a transcriptional activator. Using a growth-based selection strategy, we identified mutations in the PrfA protein leading to constitutively active virulence factor expression. We provide structural evidence for the existence of an intermediately activated PrfA state, which gives new insights into PrfA protein activation.
format Online
Article
Text
id pubmed-7221254
institution National Center for Biotechnology Information
language English
publishDate 2020
publisher American Society for Microbiology
record_format MEDLINE/PubMed
spelling pubmed-72212542020-05-20 A Novel Growth-Based Selection Strategy Identifies New Constitutively Active Variants of the Major Virulence Regulator PrfA in Listeria monocytogenes Hansen, Sabine Hall, Michael Grundström, Christin Brännström, Kristoffer Sauer-Eriksson, A. Elisabeth Johansson, Jörgen J Bacteriol Research Article Listeria monocytogenes is a Gram-positive pathogen able to cause severe human infections. Its major virulence regulator is the transcriptional activator PrfA, a member of the Crp/Fnr family of transcriptional regulators. To establish a successful L. monocytogenes infection, the PrfA protein needs to be in an active conformation, either by binding the cognate inducer glutathione (GSH) or by possessing amino acid substitutions rendering the protein constitutively active (PrfA*). By a yet unknown mechanism, phosphotransferase system (PTS) sugars repress the activity of PrfA. We therefore took a transposon-based approach to identify the mechanism by which PTS sugars repress PrfA activity. For this, we screened a transposon mutant bank to identify clones able to grow in the presence of glucose-6-phosphate as the sole carbon source. Surprisingly, most of the isolated transposon mutants also carried amino acid substitutions in PrfA. In transposon-free strains, the PrfA amino acid substitution mutants displayed growth, virulence factor expression, infectivity, and DNA binding, agreeing with previously identified PrfA* mutants. Hence, the initial growth phenotype observed in the isolated clone was due to the amino acid substitution in PrfA and unrelated to the loci inactivated by the transposon mutant. Finally, we provide structural evidence for the existence of an intermediately activated PrfA state, which gives new insights into PrfA protein activation. IMPORTANCE The Gram-positive bacterium Listeria monocytogenes is a human pathogen affecting mainly the elderly, immunocompromised people, and pregnant women. It can lead to meningoencephalitis, septicemia, and abortion. The major virulence regulator in L. monocytogenes is the PrfA protein, a transcriptional activator. Using a growth-based selection strategy, we identified mutations in the PrfA protein leading to constitutively active virulence factor expression. We provide structural evidence for the existence of an intermediately activated PrfA state, which gives new insights into PrfA protein activation. American Society for Microbiology 2020-05-11 /pmc/articles/PMC7221254/ /pubmed/32179627 http://dx.doi.org/10.1128/JB.00115-20 Text en Copyright © 2020 Hansen 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
Hansen, Sabine
Hall, Michael
Grundström, Christin
Brännström, Kristoffer
Sauer-Eriksson, A. Elisabeth
Johansson, Jörgen
A Novel Growth-Based Selection Strategy Identifies New Constitutively Active Variants of the Major Virulence Regulator PrfA in Listeria monocytogenes
title A Novel Growth-Based Selection Strategy Identifies New Constitutively Active Variants of the Major Virulence Regulator PrfA in Listeria monocytogenes
title_full A Novel Growth-Based Selection Strategy Identifies New Constitutively Active Variants of the Major Virulence Regulator PrfA in Listeria monocytogenes
title_fullStr A Novel Growth-Based Selection Strategy Identifies New Constitutively Active Variants of the Major Virulence Regulator PrfA in Listeria monocytogenes
title_full_unstemmed A Novel Growth-Based Selection Strategy Identifies New Constitutively Active Variants of the Major Virulence Regulator PrfA in Listeria monocytogenes
title_short A Novel Growth-Based Selection Strategy Identifies New Constitutively Active Variants of the Major Virulence Regulator PrfA in Listeria monocytogenes
title_sort novel growth-based selection strategy identifies new constitutively active variants of the major virulence regulator prfa in listeria monocytogenes
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7221254/
https://www.ncbi.nlm.nih.gov/pubmed/32179627
http://dx.doi.org/10.1128/JB.00115-20
work_keys_str_mv AT hansensabine anovelgrowthbasedselectionstrategyidentifiesnewconstitutivelyactivevariantsofthemajorvirulenceregulatorprfainlisteriamonocytogenes
AT hallmichael anovelgrowthbasedselectionstrategyidentifiesnewconstitutivelyactivevariantsofthemajorvirulenceregulatorprfainlisteriamonocytogenes
AT grundstromchristin anovelgrowthbasedselectionstrategyidentifiesnewconstitutivelyactivevariantsofthemajorvirulenceregulatorprfainlisteriamonocytogenes
AT brannstromkristoffer anovelgrowthbasedselectionstrategyidentifiesnewconstitutivelyactivevariantsofthemajorvirulenceregulatorprfainlisteriamonocytogenes
AT sauererikssonaelisabeth anovelgrowthbasedselectionstrategyidentifiesnewconstitutivelyactivevariantsofthemajorvirulenceregulatorprfainlisteriamonocytogenes
AT johanssonjorgen anovelgrowthbasedselectionstrategyidentifiesnewconstitutivelyactivevariantsofthemajorvirulenceregulatorprfainlisteriamonocytogenes
AT hansensabine novelgrowthbasedselectionstrategyidentifiesnewconstitutivelyactivevariantsofthemajorvirulenceregulatorprfainlisteriamonocytogenes
AT hallmichael novelgrowthbasedselectionstrategyidentifiesnewconstitutivelyactivevariantsofthemajorvirulenceregulatorprfainlisteriamonocytogenes
AT grundstromchristin novelgrowthbasedselectionstrategyidentifiesnewconstitutivelyactivevariantsofthemajorvirulenceregulatorprfainlisteriamonocytogenes
AT brannstromkristoffer novelgrowthbasedselectionstrategyidentifiesnewconstitutivelyactivevariantsofthemajorvirulenceregulatorprfainlisteriamonocytogenes
AT sauererikssonaelisabeth novelgrowthbasedselectionstrategyidentifiesnewconstitutivelyactivevariantsofthemajorvirulenceregulatorprfainlisteriamonocytogenes
AT johanssonjorgen novelgrowthbasedselectionstrategyidentifiesnewconstitutivelyactivevariantsofthemajorvirulenceregulatorprfainlisteriamonocytogenes

Ejemplares similares