Crosstalk between the HpArsRS two-component system and HpNikR is necessary for maximal activation of urease transcription

Helicobacter pylori NikR (HpNikR) is a nickel dependent transcription factor that directly regulates a number of genes in this important gastric pathogen. One key gene that is regulated by HpNikR is ureA, which encodes for the urease enzyme. In vitro DNA binding studies of HpNikR with the ureA promo...

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Autores principales: Carpenter, Beth M., West, Abby L., Gancz, Hanan, Servetas, Stephanie L., Pich, Oscar Q., Gilbreath, Jeremy J., Hallinger, Daniel R., Forsyth, Mark H., Merrell, D. Scott, Michel, Sarah L. J.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Frontiers Media S.A. 2015
Materias:
Microbiology
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4464171/
https://www.ncbi.nlm.nih.gov/pubmed/26124751
http://dx.doi.org/10.3389/fmicb.2015.00558
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author Carpenter, Beth M.
West, Abby L.
Gancz, Hanan
Servetas, Stephanie L.
Pich, Oscar Q.
Gilbreath, Jeremy J.
Hallinger, Daniel R.
Forsyth, Mark H.
Merrell, D. Scott
Michel, Sarah L. J.
author_facet Carpenter, Beth M.
West, Abby L.
Gancz, Hanan
Servetas, Stephanie L.
Pich, Oscar Q.
Gilbreath, Jeremy J.
Hallinger, Daniel R.
Forsyth, Mark H.
Merrell, D. Scott
Michel, Sarah L. J.
author_sort Carpenter, Beth M.
collection PubMed
description Helicobacter pylori NikR (HpNikR) is a nickel dependent transcription factor that directly regulates a number of genes in this important gastric pathogen. One key gene that is regulated by HpNikR is ureA, which encodes for the urease enzyme. In vitro DNA binding studies of HpNikR with the ureA promoter (P(ureA)) previously identified a recognition site that is required for high affinity protein/DNA binding. As a means to determine the in vivo significance of this recognition site and to identify the key DNA sequence determinants required for ureA transcription, herein, we have translated these in vitro results to analysis directly within H. pylori. Using a series of GFP reporter constructs in which the P(ureA) DNA target was altered, in combination with mutant H. pylori strains deficient in key regulatory proteins, we confirmed the importance of the previously identified HpNikR recognition sequence for HpNikR-dependent ureA transcription. Moreover, we identified a second factor, the HpArsRS two-component system that was required for maximum transcription of ureA. While HpArsRS is known to regulate ureA in response to acid shock, it was previously thought to function independently of HpNikR and to have no role at neutral pH. However, our qPCR analysis of ureA expression in wildtype, ΔnikR and ΔarsS single mutants as well as a ΔarsS/nikR double mutant strain background showed reduced basal level expression of ureA when arsS was absent. Additionally, we determined that both HpNikR and HpArsRS were necessary for maximal expression of ureA under nickel, low pH and combined nickel and low pH stresses. In vitro studies of HpArsR-P with the P(ureA) DNA target using florescence anisotropy confirmed a direct protein/DNA binding interaction. Together, these data support a model in which HpArsRS and HpNikR cooperatively interact to regulate ureA transcription under various environmental conditions. This is the first time that direct “cross-talk” between HpArsRS and HpNikR at neutral pH has been demonstrated.
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spelling pubmed-44641712015-06-29 Crosstalk between the HpArsRS two-component system and HpNikR is necessary for maximal activation of urease transcription Carpenter, Beth M. West, Abby L. Gancz, Hanan Servetas, Stephanie L. Pich, Oscar Q. Gilbreath, Jeremy J. Hallinger, Daniel R. Forsyth, Mark H. Merrell, D. Scott Michel, Sarah L. J. Front Microbiol Microbiology Helicobacter pylori NikR (HpNikR) is a nickel dependent transcription factor that directly regulates a number of genes in this important gastric pathogen. One key gene that is regulated by HpNikR is ureA, which encodes for the urease enzyme. In vitro DNA binding studies of HpNikR with the ureA promoter (P(ureA)) previously identified a recognition site that is required for high affinity protein/DNA binding. As a means to determine the in vivo significance of this recognition site and to identify the key DNA sequence determinants required for ureA transcription, herein, we have translated these in vitro results to analysis directly within H. pylori. Using a series of GFP reporter constructs in which the P(ureA) DNA target was altered, in combination with mutant H. pylori strains deficient in key regulatory proteins, we confirmed the importance of the previously identified HpNikR recognition sequence for HpNikR-dependent ureA transcription. Moreover, we identified a second factor, the HpArsRS two-component system that was required for maximum transcription of ureA. While HpArsRS is known to regulate ureA in response to acid shock, it was previously thought to function independently of HpNikR and to have no role at neutral pH. However, our qPCR analysis of ureA expression in wildtype, ΔnikR and ΔarsS single mutants as well as a ΔarsS/nikR double mutant strain background showed reduced basal level expression of ureA when arsS was absent. Additionally, we determined that both HpNikR and HpArsRS were necessary for maximal expression of ureA under nickel, low pH and combined nickel and low pH stresses. In vitro studies of HpArsR-P with the P(ureA) DNA target using florescence anisotropy confirmed a direct protein/DNA binding interaction. Together, these data support a model in which HpArsRS and HpNikR cooperatively interact to regulate ureA transcription under various environmental conditions. This is the first time that direct “cross-talk” between HpArsRS and HpNikR at neutral pH has been demonstrated. Frontiers Media S.A. 2015-06-12 /pmc/articles/PMC4464171/ /pubmed/26124751 http://dx.doi.org/10.3389/fmicb.2015.00558 Text en Copyright © 2015 Carpenter, West, Gancz, Servetas, Pich, Gilbreath, Hallinger, Forsyth, Merrell and Michel. http://creativecommons.org/licenses/by/4.0/ This is an open-access article distributed under the terms of the Creative Commons Attribution License (CC BY). The use, distribution or reproduction in other forums is permitted, provided the original author(s) or licensor are credited and that the original publication in this journal is cited, in accordance with accepted academic practice. No use, distribution or reproduction is permitted which does not comply with these terms.
spellingShingle Microbiology
Carpenter, Beth M.
West, Abby L.
Gancz, Hanan
Servetas, Stephanie L.
Pich, Oscar Q.
Gilbreath, Jeremy J.
Hallinger, Daniel R.
Forsyth, Mark H.
Merrell, D. Scott
Michel, Sarah L. J.
Crosstalk between the HpArsRS two-component system and HpNikR is necessary for maximal activation of urease transcription
title Crosstalk between the HpArsRS two-component system and HpNikR is necessary for maximal activation of urease transcription
title_full Crosstalk between the HpArsRS two-component system and HpNikR is necessary for maximal activation of urease transcription
title_fullStr Crosstalk between the HpArsRS two-component system and HpNikR is necessary for maximal activation of urease transcription
title_full_unstemmed Crosstalk between the HpArsRS two-component system and HpNikR is necessary for maximal activation of urease transcription
title_short Crosstalk between the HpArsRS two-component system and HpNikR is necessary for maximal activation of urease transcription
title_sort crosstalk between the hparsrs two-component system and hpnikr is necessary for maximal activation of urease transcription
topic Microbiology
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4464171/
https://www.ncbi.nlm.nih.gov/pubmed/26124751
http://dx.doi.org/10.3389/fmicb.2015.00558
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