Pheromone Recognition and Selectivity by ComR Proteins among Streptococcus Species

Natural transformation, or competence, is an ability inherent to bacteria for the uptake of extracellular DNA. This process is central to bacterial evolution and allows for the rapid acquirement of new traits, such as antibiotic resistance in pathogenic microorganisms. For the Gram-positive bacteria...

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Published in:PLoS pathogens Vol. 12; no. 12; p. e1005979
Main Authors: Shanker, Erin, Morrison, Donald A, Talagas, Antoine, Nessler, Sylvie, Federle, Michael J, Prehna, Gerd
Format: Journal Article
Language:English
Published: United States Public Library of Science 01-12-2016
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Abstract Natural transformation, or competence, is an ability inherent to bacteria for the uptake of extracellular DNA. This process is central to bacterial evolution and allows for the rapid acquirement of new traits, such as antibiotic resistance in pathogenic microorganisms. For the Gram-positive bacteria genus Streptococcus, genes required for competence are under the regulation of quorum sensing (QS) mediated by peptide pheromones. One such system, ComRS, consists of a peptide (ComS) that is processed (XIP), secreted, and later imported into the cytoplasm, where it binds and activates the transcription factor ComR. ComR then engages in a positive feedback loop for the expression of ComS and the alternative sigma-factor SigX. Although ComRS are present in the majority of Streptococcus species, the sequence of both ComS/XIP and ComR diverge significantly, suggesting a mechanism for species-specific communication. To study possible cross-talk between streptococcal species in the regulation of competence, and to explore in detail the molecular interaction between ComR and XIP we undertook an interdisciplinary approach. We developed a 'test-bed' assay to measure the activity of different ComR proteins in response to cognate and heterologous XIP peptides in vivo, revealing distinct ComR classes of strict, intermediate, and promiscuous specificity among species. We then solved an X-ray crystal structure of ComR from S. suis to further understand the interaction with XIP and to search for structural features in ComR proteins that may explain XIP recognition. Using the structure as a guide, we probed the apo conformation of the XIP-binding pocket by site-directed mutagenesis, both in test-bed cultures and biochemically in vitro. In alignments with ComR proteins from other species, we find that the pocket is lined by a variable and a conserved face, where residues of the conserved face contribute to ligand binding and the variable face discriminate among XIP peptides. Together, our results not only provide a model for XIP recognition and specificity, but also allow for the prediction of novel XIP peptides that induce ComR activity.
AbstractList Natural transformation, or competence, is an ability inherent to bacteria for the uptake of extracellular DNA. This process is central to bacterial evolution and allows for the rapid acquirement of new traits, such as antibiotic resistance in pathogenic microorganisms. For the Gram-positive bacteria genus Streptococcus, genes required for competence are under the regulation of quorum sensing (QS) mediated by peptide pheromones. One such system, ComRS, consists of a peptide (ComS) that is processed (XIP), secreted, and later imported into the cytoplasm, where it binds and activates the transcription factor ComR. ComR then engages in a positive feedback loop for the expression of ComS and the alternative sigma-factor SigX. Although ComRS are present in the majority of Streptococcus species, the sequence of both ComS/XIP and ComR diverge significantly, suggesting a mechanism for species-specific communication. To study possible cross-talk between streptococcal species in the regulation of competence, and to explore in detail the molecular interaction between ComR and XIP we undertook an interdisciplinary approach. We developed a ‘test-bed’ assay to measure the activity of different ComR proteins in response to cognate and heterologous XIP peptides in vivo, revealing distinct ComR classes of strict, intermediate, and promiscuous specificity among species. We then solved an X-ray crystal structure of ComR from S. suis to further understand the interaction with XIP and to search for structural features in ComR proteins that may explain XIP recognition. Using the structure as a guide, we probed the apo conformation of the XIP-binding pocket by site-directed mutagenesis, both in test-bed cultures and biochemically in vitro. In alignments with ComR proteins from other species, we find that the pocket is lined by a variable and a conserved face, where residues of the conserved face contribute to ligand binding and the variable face discriminate among XIP peptides. Together, our results not only provide a model for XIP recognition and specificity, but also allow for the prediction of novel XIP peptides that induce ComR activity.
Natural transformation, or competence, is an ability inherent to bacteria for the uptake of extracellular DNA. This process is central to bacterial evolution and allows for the rapid acquirement of new traits, such as antibiotic resistance in pathogenic microorganisms. For the Gram-positive bacteria genus Streptococcus , genes required for competence are under the regulation of quorum sensing (QS) mediated by peptide pheromones. One such system, ComRS, consists of a peptide (ComS) that is processed (XIP), secreted, and later imported into the cytoplasm, where it binds and activates the transcription factor ComR. ComR then engages in a positive feedback loop for the expression of ComS and the alternative sigma-factor SigX. Although ComRS are present in the majority of Streptococcus species, the sequence of both ComS/XIP and ComR diverge significantly, suggesting a mechanism for species-specific communication. To study possible cross-talk between streptococcal species in the regulation of competence, and to explore in detail the molecular interaction between ComR and XIP we undertook an interdisciplinary approach. We developed a ‘test-bed’ assay to measure the activity of different ComR proteins in response to cognate and heterologous XIP peptides in vivo , revealing distinct ComR classes of strict, intermediate, and promiscuous specificity among species. We then solved an X-ray crystal structure of ComR from S . suis to further understand the interaction with XIP and to search for structural features in ComR proteins that may explain XIP recognition. Using the structure as a guide, we probed the apo conformation of the XIP-binding pocket by site-directed mutagenesis, both in test-bed cultures and biochemically in vitro . In alignments with ComR proteins from other species, we find that the pocket is lined by a variable and a conserved face, where residues of the conserved face contribute to ligand binding and the variable face discriminate among XIP peptides. Together, our results not only provide a model for XIP recognition and specificity, but also allow for the prediction of novel XIP peptides that induce ComR activity. Bacteria transmit chemical signals to each other in a process known as quorum sensing. This adaptation is central to pathogenesis as it allows bacteria to coordinate a group response, such as when to form a biofilm, secrete virulence factors, or uptake new DNA. Quorum sensing in many species of Gram-positive bacteria utilizes secreted short peptide signals that are sensed by protein receptors that alter gene expression. The ComR-ComS receptor-signal pair is a regulator of competence for genetic transformation that is broadly conserved in a majority of Streptococcus species, including those pathogenic in humans and animals. Despite this conservation, we observe sequence diversity among ComRS orthologs that raises questions relating to sensory specificity and the molecular mechanism of peptide recognition. To address this, we directly tested the possibility for signaling cross-talk and identified three general categories of ComR receptors displaying strict, intermediate, and promiscuous responses to heterologous peptides. To elucidate the molecular mechanism of receptor specificity we determined an X-ray crystal structure of ComR from S . suis . We observe a conserved face of the ligand pocket important for peptide binding and a variable face that functions in peptide specificity. Finally, basic criteria necessary for peptide responses were used to redesign active peptides from inactive templates.
Audience Academic
Author Shanker, Erin
Nessler, Sylvie
Talagas, Antoine
Federle, Michael J
Prehna, Gerd
Morrison, Donald A
AuthorAffiliation 1 Department of Medicinal Chemistry and Pharmacognosy, University of Illinois at Chicago, Chicago, IL, United States of America
6 Department of Microbiology and Immunology, University of Illinois at Chicago, Chicago, IL, United States of America
2 Center for Biomolecular Science, University of Illinois at Chicago, Chicago, IL, United States of America
3 Department of Biological Sciences, University of Illinois at Chicago, Chicago, IL, United States of America
4 Institute of Integrative Biology of the Cell (I2BC), CEA, CNRS, Univ Paris-Sud, Université Paris-Saclay, France
5 Center for Structural Biology, Research Resources Center, University of Illinois at Chicago, Chicago, IL, United States of America
National Jewish Health, UNITED STATES
AuthorAffiliation_xml – name: 3 Department of Biological Sciences, University of Illinois at Chicago, Chicago, IL, United States of America
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– name: 1 Department of Medicinal Chemistry and Pharmacognosy, University of Illinois at Chicago, Chicago, IL, United States of America
– name: 6 Department of Microbiology and Immunology, University of Illinois at Chicago, Chicago, IL, United States of America
– name: 4 Institute of Integrative Biology of the Cell (I2BC), CEA, CNRS, Univ Paris-Sud, Université Paris-Saclay, France
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2016 Shanker et al 2016 Shanker et al
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Notes PMCID: PMC5131902
Michigan Technology Tri-Corridor
AC02-06CH11357; AI091779; 5F30AI110080; 085P1000817
USDOE Office of Science (SC)
National Inst. of Health
Michigan Economic Development Corp.
Burroughs Wellcome Fund
Conceived and designed the experiments: ES GP. Performed the experiments: ES GP. Analyzed the data: ES DAM AT SN MJF GP. Contributed reagents/materials/analysis tools: DAM MJF GP. Wrote the paper: ES DAM AT SN MJF GP.
The authors have declared that no competing interests exist.
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SSID ssj0041316
Score 2.4450579
Snippet Natural transformation, or competence, is an ability inherent to bacteria for the uptake of extracellular DNA. This process is central to bacterial evolution...
SourceID doaj
pubmedcentral
osti
hal
gale
crossref
pubmed
SourceType Open Website
Open Access Repository
Aggregation Database
Index Database
StartPage e1005979
SubjectTerms Bacterial proteins
Bacterial Proteins - metabolism
BASIC BIOLOGICAL SCIENCES
Biology and Life Sciences
Calorimetry
Circular Dichroism
crystal structure
DNA Transformation Competence - physiology
face recognition
Gene Expression Regulation, Bacterial - physiology
Life Sciences
Medicine and Health Sciences
Pheromones
Physical Sciences
Physiological aspects
Properties
Quorum sensing
Quorum Sensing - physiology
Research and Analysis Methods
sequence motif analysis
Social Sciences
Streptococcus - physiology
Streptococcus agalactiae
Streptococcus mutans
Streptococcus pyogenes
Streptococcus suis
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Title Pheromone Recognition and Selectivity by ComR Proteins among Streptococcus Species
URI https://www.ncbi.nlm.nih.gov/pubmed/27907154
https://hal.science/hal-01451053
https://www.osti.gov/servlets/purl/1498415
https://pubmed.ncbi.nlm.nih.gov/PMC5131902
https://doaj.org/article/18a3368349644be5b36992b171df49fd
Volume 12
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