Structural basis of DSF recognition by its receptor RpfR and its regulatory interaction with the DSF synthase RpfF

The diffusible signal factors (DSFs) are a family of quorum-sensing autoinducers (AIs) produced and detected by numerous gram-negative bacteria. The DSF family AIs are fatty acids, differing in their acyl chain length, branching, and substitution but having in common a cis-2 double bond that is requ...

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Autores principales: Waldron, Evan J., Snyder, Daniel, Fernandez, Nicolas L., Sileo, Emily, Inoyama, Daigo, Freundlich, Joel S., Waters, Christopher M., Cooper, Vaughn S., Neiditch, Matthew B.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Public Library of Science 2019
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6361424/
https://www.ncbi.nlm.nih.gov/pubmed/30716063
http://dx.doi.org/10.1371/journal.pbio.3000123
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author Waldron, Evan J.
Snyder, Daniel
Fernandez, Nicolas L.
Sileo, Emily
Inoyama, Daigo
Freundlich, Joel S.
Waters, Christopher M.
Cooper, Vaughn S.
Neiditch, Matthew B.
author_facet Waldron, Evan J.
Snyder, Daniel
Fernandez, Nicolas L.
Sileo, Emily
Inoyama, Daigo
Freundlich, Joel S.
Waters, Christopher M.
Cooper, Vaughn S.
Neiditch, Matthew B.
author_sort Waldron, Evan J.
collection PubMed
description The diffusible signal factors (DSFs) are a family of quorum-sensing autoinducers (AIs) produced and detected by numerous gram-negative bacteria. The DSF family AIs are fatty acids, differing in their acyl chain length, branching, and substitution but having in common a cis-2 double bond that is required for their activity. In both human and plant pathogens, DSFs regulate diverse phenotypes, including virulence factor expression, antibiotic resistance, and biofilm dispersal. Despite their widespread relevance to both human health and agriculture, the molecular basis of DSF recognition by their cellular receptors remained a mystery. Here, we report the first structure–function studies of the DSF receptor regulation of pathogenicity factor R (RpfR). We present the X-ray crystal structure of the RpfR DSF-binding domain in complex with the Burkholderia DSF (BDSF), which to our knowledge is the first structure of a DSF receptor in complex with its AI. To begin to understand the mechanistic role of the BDSF–RpfR contacts observed in the biologically important complex, we have also determined the X-ray crystal structure of the RpfR DSF-binding domain in complex with the inactive, saturated isomer of BDSF, dodecanoic acid (C12:0). In addition to these ligand–receptor complex structures, we report the discovery of a previously overlooked RpfR domain and show that it binds to and negatively regulates the DSF synthase regulation of pathogenicity factor F (RpfF). We have named this RpfR region the RpfF interaction (FI) domain, and we have determined its X-ray crystal structure alone and in complex with RpfF. These X-ray crystal structures, together with extensive complementary in vivo and in vitro functional studies, reveal the molecular basis of DSF recognition and the importance of the cis-2 double bond to DSF function. Finally, we show that throughout cellular growth, the production of BDSF by RpfF is post-translationally controlled by the RpfR N-terminal FI domain, affecting the cellular concentration of the bacterial second messenger bis-(3′-5′)-cyclic dimeric guanosine monophosphate (c-di-GMP). Thus, in addition to describing the molecular basis for the binding and specificity of a DSF for its receptor, we describe a receptor–synthase interaction regulating bacterial quorum-sensing signaling and second messenger signal transduction.
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spelling pubmed-63614242019-02-15 Structural basis of DSF recognition by its receptor RpfR and its regulatory interaction with the DSF synthase RpfF Waldron, Evan J. Snyder, Daniel Fernandez, Nicolas L. Sileo, Emily Inoyama, Daigo Freundlich, Joel S. Waters, Christopher M. Cooper, Vaughn S. Neiditch, Matthew B. PLoS Biol Research Article The diffusible signal factors (DSFs) are a family of quorum-sensing autoinducers (AIs) produced and detected by numerous gram-negative bacteria. The DSF family AIs are fatty acids, differing in their acyl chain length, branching, and substitution but having in common a cis-2 double bond that is required for their activity. In both human and plant pathogens, DSFs regulate diverse phenotypes, including virulence factor expression, antibiotic resistance, and biofilm dispersal. Despite their widespread relevance to both human health and agriculture, the molecular basis of DSF recognition by their cellular receptors remained a mystery. Here, we report the first structure–function studies of the DSF receptor regulation of pathogenicity factor R (RpfR). We present the X-ray crystal structure of the RpfR DSF-binding domain in complex with the Burkholderia DSF (BDSF), which to our knowledge is the first structure of a DSF receptor in complex with its AI. To begin to understand the mechanistic role of the BDSF–RpfR contacts observed in the biologically important complex, we have also determined the X-ray crystal structure of the RpfR DSF-binding domain in complex with the inactive, saturated isomer of BDSF, dodecanoic acid (C12:0). In addition to these ligand–receptor complex structures, we report the discovery of a previously overlooked RpfR domain and show that it binds to and negatively regulates the DSF synthase regulation of pathogenicity factor F (RpfF). We have named this RpfR region the RpfF interaction (FI) domain, and we have determined its X-ray crystal structure alone and in complex with RpfF. These X-ray crystal structures, together with extensive complementary in vivo and in vitro functional studies, reveal the molecular basis of DSF recognition and the importance of the cis-2 double bond to DSF function. Finally, we show that throughout cellular growth, the production of BDSF by RpfF is post-translationally controlled by the RpfR N-terminal FI domain, affecting the cellular concentration of the bacterial second messenger bis-(3′-5′)-cyclic dimeric guanosine monophosphate (c-di-GMP). Thus, in addition to describing the molecular basis for the binding and specificity of a DSF for its receptor, we describe a receptor–synthase interaction regulating bacterial quorum-sensing signaling and second messenger signal transduction. Public Library of Science 2019-02-04 /pmc/articles/PMC6361424/ /pubmed/30716063 http://dx.doi.org/10.1371/journal.pbio.3000123 Text en © 2019 Waldron et al http://creativecommons.org/licenses/by/4.0/ This is an open access article distributed under the terms of the Creative Commons Attribution License (http://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
Waldron, Evan J.
Snyder, Daniel
Fernandez, Nicolas L.
Sileo, Emily
Inoyama, Daigo
Freundlich, Joel S.
Waters, Christopher M.
Cooper, Vaughn S.
Neiditch, Matthew B.
Structural basis of DSF recognition by its receptor RpfR and its regulatory interaction with the DSF synthase RpfF
title Structural basis of DSF recognition by its receptor RpfR and its regulatory interaction with the DSF synthase RpfF
title_full Structural basis of DSF recognition by its receptor RpfR and its regulatory interaction with the DSF synthase RpfF
title_fullStr Structural basis of DSF recognition by its receptor RpfR and its regulatory interaction with the DSF synthase RpfF
title_full_unstemmed Structural basis of DSF recognition by its receptor RpfR and its regulatory interaction with the DSF synthase RpfF
title_short Structural basis of DSF recognition by its receptor RpfR and its regulatory interaction with the DSF synthase RpfF
title_sort structural basis of dsf recognition by its receptor rpfr and its regulatory interaction with the dsf synthase rpff
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6361424/
https://www.ncbi.nlm.nih.gov/pubmed/30716063
http://dx.doi.org/10.1371/journal.pbio.3000123
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