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AhpA is a peroxidase expressed during biofilm formation in Bacillus subtilis

Organisms growing aerobically generate reactive oxygen species such as hydrogen peroxide. These reactive oxygen molecules damage enzymes and DNA, potentially causing cell death. In response, Bacillus subtilis produces at least nine potential peroxide‐scavenging enzymes; two belong to the alkylhydrop...

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Autores principales: Zwick, Joelie V., Noble, Sarah, Ellaicy, Yasser K., Coe, Gabrielle Dierker, Hakey, Dylan J., King, Alyssa N., Sadauskas, Alex J., Faulkner, Melinda J.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: John Wiley and Sons Inc. 2016
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5300871/
https://www.ncbi.nlm.nih.gov/pubmed/27683249
http://dx.doi.org/10.1002/mbo3.403
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author Zwick, Joelie V.
Noble, Sarah
Ellaicy, Yasser K.
Coe, Gabrielle Dierker
Hakey, Dylan J.
King, Alyssa N.
Sadauskas, Alex J.
Faulkner, Melinda J.
author_facet Zwick, Joelie V.
Noble, Sarah
Ellaicy, Yasser K.
Coe, Gabrielle Dierker
Hakey, Dylan J.
King, Alyssa N.
Sadauskas, Alex J.
Faulkner, Melinda J.
author_sort Zwick, Joelie V.
collection PubMed
description Organisms growing aerobically generate reactive oxygen species such as hydrogen peroxide. These reactive oxygen molecules damage enzymes and DNA, potentially causing cell death. In response, Bacillus subtilis produces at least nine potential peroxide‐scavenging enzymes; two belong to the alkylhydroperoxide reductase (Ahp) class of peroxidases. Here, we explore the role of one of these Ahp homologs, AhpA. While previous studies demonstrated that AhpA can scavenge peroxides and thus defend cells against peroxides, they did not clarify when during growth the cell produces AhpA. The results presented here show that the expression of ahpA is regulated in a manner distinct from that of the other peroxide‐scavenging enzymes in B. subtilis. While the primary Ahp, AhpC, is expressed during exponential growth and stationary phase, these studies demonstrate that the expression of ahpA is dependent on the transition‐state regulator AbrB and the sporulation and biofilm formation transcription factor Spo0A. Furthermore, these results show that ahpA is specifically expressed during biofilm formation, and not during sporulation or stationary phase, suggesting that derepression of ahpA by AbrB requires a signal other than those present upon entry into stationary phase. Despite this expression pattern, ahpA mutant strains still form and maintain robust biofilms, even in the presence of peroxides. Thus, the role of AhpA with regard to protecting cells within biofilms from environmental stresses is still uncertain. These studies highlight the need to further study the Ahp homologs to better understand how they differ from one another and the unique roles they may play in oxidative stress resistance.
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spelling pubmed-53008712017-02-13 AhpA is a peroxidase expressed during biofilm formation in Bacillus subtilis Zwick, Joelie V. Noble, Sarah Ellaicy, Yasser K. Coe, Gabrielle Dierker Hakey, Dylan J. King, Alyssa N. Sadauskas, Alex J. Faulkner, Melinda J. Microbiologyopen Original Research Organisms growing aerobically generate reactive oxygen species such as hydrogen peroxide. These reactive oxygen molecules damage enzymes and DNA, potentially causing cell death. In response, Bacillus subtilis produces at least nine potential peroxide‐scavenging enzymes; two belong to the alkylhydroperoxide reductase (Ahp) class of peroxidases. Here, we explore the role of one of these Ahp homologs, AhpA. While previous studies demonstrated that AhpA can scavenge peroxides and thus defend cells against peroxides, they did not clarify when during growth the cell produces AhpA. The results presented here show that the expression of ahpA is regulated in a manner distinct from that of the other peroxide‐scavenging enzymes in B. subtilis. While the primary Ahp, AhpC, is expressed during exponential growth and stationary phase, these studies demonstrate that the expression of ahpA is dependent on the transition‐state regulator AbrB and the sporulation and biofilm formation transcription factor Spo0A. Furthermore, these results show that ahpA is specifically expressed during biofilm formation, and not during sporulation or stationary phase, suggesting that derepression of ahpA by AbrB requires a signal other than those present upon entry into stationary phase. Despite this expression pattern, ahpA mutant strains still form and maintain robust biofilms, even in the presence of peroxides. Thus, the role of AhpA with regard to protecting cells within biofilms from environmental stresses is still uncertain. These studies highlight the need to further study the Ahp homologs to better understand how they differ from one another and the unique roles they may play in oxidative stress resistance. John Wiley and Sons Inc. 2016-09-28 /pmc/articles/PMC5300871/ /pubmed/27683249 http://dx.doi.org/10.1002/mbo3.403 Text en © 2016 The Authors. MicrobiologyOpen published by John Wiley & Sons Ltd. This is an open access article under the terms of the Creative Commons Attribution (http://creativecommons.org/licenses/by/4.0/) License, which permits use, distribution and reproduction in any medium, provided the original work is properly cited.
spellingShingle Original Research
Zwick, Joelie V.
Noble, Sarah
Ellaicy, Yasser K.
Coe, Gabrielle Dierker
Hakey, Dylan J.
King, Alyssa N.
Sadauskas, Alex J.
Faulkner, Melinda J.
AhpA is a peroxidase expressed during biofilm formation in Bacillus subtilis
title AhpA is a peroxidase expressed during biofilm formation in Bacillus subtilis
title_full AhpA is a peroxidase expressed during biofilm formation in Bacillus subtilis
title_fullStr AhpA is a peroxidase expressed during biofilm formation in Bacillus subtilis
title_full_unstemmed AhpA is a peroxidase expressed during biofilm formation in Bacillus subtilis
title_short AhpA is a peroxidase expressed during biofilm formation in Bacillus subtilis
title_sort ahpa is a peroxidase expressed during biofilm formation in bacillus subtilis
topic Original Research
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5300871/
https://www.ncbi.nlm.nih.gov/pubmed/27683249
http://dx.doi.org/10.1002/mbo3.403
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