Repression by the H-NS/YmoA histone-like protein complex enables IscR dependent regulation of the Yersinia T3SS

The type III secretion system (T3SS) is an appendage used by many bacterial pathogens, such as pathogenic Yersinia, to subvert host defenses. However, because the T3SS is energetically costly and immunogenic, it must be tightly regulated in response to environmental cues to enable survival in the ho...

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Autores principales: Balderas, David, Ohanyan, Mané, Alvarez, Pablo A., Mettert, Erin, Tanner, Natasha, Kiley, Patricia J., Auerbuch, Victoria
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Public Library of Science 2022
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9362927/
https://www.ncbi.nlm.nih.gov/pubmed/35901167
http://dx.doi.org/10.1371/journal.pgen.1010321
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author Balderas, David
Ohanyan, Mané
Alvarez, Pablo A.
Mettert, Erin
Tanner, Natasha
Kiley, Patricia J.
Auerbuch, Victoria
author_facet Balderas, David
Ohanyan, Mané
Alvarez, Pablo A.
Mettert, Erin
Tanner, Natasha
Kiley, Patricia J.
Auerbuch, Victoria
author_sort Balderas, David
collection PubMed
description The type III secretion system (T3SS) is an appendage used by many bacterial pathogens, such as pathogenic Yersinia, to subvert host defenses. However, because the T3SS is energetically costly and immunogenic, it must be tightly regulated in response to environmental cues to enable survival in the host. Here we show that expression of the Yersinia Ysc T3SS master regulator, LcrF, is orchestrated by the opposing activities of the repressive H-NS/YmoA histone-like protein complex and induction by the iron and oxygen-regulated IscR transcription factor. While deletion of iscR or ymoA has been shown to decrease and increase LcrF expression and type III secretion, respectively, the role of H-NS in this system has not been definitively established because hns is an essential gene in Yersinia. Using CRISPRi knockdown of hns, we show that hns depletion causes derepression of lcrF. Furthermore, we find that while YmoA is dispensable for H-NS binding to the lcrF promoter, YmoA binding to H-NS is important for H-NS repressive activity. We bioinformatically identified three H-NS binding regions within the lcrF promoter and demonstrate binding of H-NS to these sites in vivo using chromatin immunoprecipitation. Using promoter truncation and binding site mutation analysis, we show that two of these H-NS binding regions are important for H-NS/YmoA-mediated repression of the lcrF promoter. Surprisingly, we find that IscR is dispensable for lcrF transcription in the absence of H-NS/YmoA. Indeed, IscR-dependent regulation of LcrF and type III secretion in response to changes in oxygen, such as those Yersinia is predicted to experience during host infection, only occurs in the presence of an H-NS/YmoA complex. These data suggest that, in the presence of host tissue cues that drive sufficient IscR expression, IscR can act as a roadblock to H-NS/YmoA-dependent repression of RNA polymerase at the lcrF promoter to turn on T3SS expression.
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spelling pubmed-93629272022-08-10 Repression by the H-NS/YmoA histone-like protein complex enables IscR dependent regulation of the Yersinia T3SS Balderas, David Ohanyan, Mané Alvarez, Pablo A. Mettert, Erin Tanner, Natasha Kiley, Patricia J. Auerbuch, Victoria PLoS Genet Research Article The type III secretion system (T3SS) is an appendage used by many bacterial pathogens, such as pathogenic Yersinia, to subvert host defenses. However, because the T3SS is energetically costly and immunogenic, it must be tightly regulated in response to environmental cues to enable survival in the host. Here we show that expression of the Yersinia Ysc T3SS master regulator, LcrF, is orchestrated by the opposing activities of the repressive H-NS/YmoA histone-like protein complex and induction by the iron and oxygen-regulated IscR transcription factor. While deletion of iscR or ymoA has been shown to decrease and increase LcrF expression and type III secretion, respectively, the role of H-NS in this system has not been definitively established because hns is an essential gene in Yersinia. Using CRISPRi knockdown of hns, we show that hns depletion causes derepression of lcrF. Furthermore, we find that while YmoA is dispensable for H-NS binding to the lcrF promoter, YmoA binding to H-NS is important for H-NS repressive activity. We bioinformatically identified three H-NS binding regions within the lcrF promoter and demonstrate binding of H-NS to these sites in vivo using chromatin immunoprecipitation. Using promoter truncation and binding site mutation analysis, we show that two of these H-NS binding regions are important for H-NS/YmoA-mediated repression of the lcrF promoter. Surprisingly, we find that IscR is dispensable for lcrF transcription in the absence of H-NS/YmoA. Indeed, IscR-dependent regulation of LcrF and type III secretion in response to changes in oxygen, such as those Yersinia is predicted to experience during host infection, only occurs in the presence of an H-NS/YmoA complex. These data suggest that, in the presence of host tissue cues that drive sufficient IscR expression, IscR can act as a roadblock to H-NS/YmoA-dependent repression of RNA polymerase at the lcrF promoter to turn on T3SS expression. Public Library of Science 2022-07-28 /pmc/articles/PMC9362927/ /pubmed/35901167 http://dx.doi.org/10.1371/journal.pgen.1010321 Text en © 2022 Balderas 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
Balderas, David
Ohanyan, Mané
Alvarez, Pablo A.
Mettert, Erin
Tanner, Natasha
Kiley, Patricia J.
Auerbuch, Victoria
Repression by the H-NS/YmoA histone-like protein complex enables IscR dependent regulation of the Yersinia T3SS
title Repression by the H-NS/YmoA histone-like protein complex enables IscR dependent regulation of the Yersinia T3SS
title_full Repression by the H-NS/YmoA histone-like protein complex enables IscR dependent regulation of the Yersinia T3SS
title_fullStr Repression by the H-NS/YmoA histone-like protein complex enables IscR dependent regulation of the Yersinia T3SS
title_full_unstemmed Repression by the H-NS/YmoA histone-like protein complex enables IscR dependent regulation of the Yersinia T3SS
title_short Repression by the H-NS/YmoA histone-like protein complex enables IscR dependent regulation of the Yersinia T3SS
title_sort repression by the h-ns/ymoa histone-like protein complex enables iscr dependent regulation of the yersinia t3ss
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9362927/
https://www.ncbi.nlm.nih.gov/pubmed/35901167
http://dx.doi.org/10.1371/journal.pgen.1010321
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