A Novel Mechanism for Protein Delivery by the Type 3 Secretion System for Extracellularly Secreted Proteins

The type 3 secretion system (T3SS) is essential for bacterial virulence through delivering effector proteins directly into the host cytosol. Here, we identified an alternative delivery mechanism of virulence factors mediated by the T3SS, which consists of the association of extracellularly secreted...

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Main Authors: Farid Tejeda-Dominguez, Jazmin Huerta-Cantillo, Lucia Chavez-Dueñas, Fernando Navarro-Garcia, Vanessa Sperandio
Format: Article
Language:English
Published: American Society for Microbiology 2017-03-01
Series:mBio
Online Access:http://mbio.asm.org/cgi/content/full/8/2/e00184-17
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spelling doaj-b773a6b5d9464815af97c70687ef17e92021-07-02T01:46:53ZengAmerican Society for MicrobiologymBio2150-75112017-03-0182e00184-1710.1128/mBio.00184-17A Novel Mechanism for Protein Delivery by the Type 3 Secretion System for Extracellularly Secreted ProteinsFarid Tejeda-DominguezJazmin Huerta-CantilloLucia Chavez-DueñasFernando Navarro-GarciaVanessa SperandioThe type 3 secretion system (T3SS) is essential for bacterial virulence through delivering effector proteins directly into the host cytosol. Here, we identified an alternative delivery mechanism of virulence factors mediated by the T3SS, which consists of the association of extracellularly secreted proteins from bacteria with the T3SS to gain access to the host cytosol. Both EspC, a protein secreted as an enteropathogenic Escherichia coli (EPEC) autotransporter, and YopH, a protein detected on the surface of Yersinia, require a functional T3SS for host cell internalization; here we provide biophysical and molecular evidence to support the concept of the EspC translocation mechanism, which requires (i) an interaction between EspA and an EspC middle segment, (ii) an EspC translocation motif (21 residues that are shared with the YopH translocation motif), (iii) increases in the association and dissociation rates of EspC mediated by EspA interacting with EspD, and (iv) an interaction of EspC with the EspD/EspB translocon pore. Interestingly, this novel mechanism does not exclude the injection model (i.e., EspF) operating through the T3SS conduit; therefore, T3SS can be functioning as an internal conduit or as an external railway, which can be used to reach the translocator pore, and this mechanism appears to be conserved among different T3SS-dependent pathogens.http://mbio.asm.org/cgi/content/full/8/2/e00184-17
collection DOAJ
language English
format Article
sources DOAJ
author Farid Tejeda-Dominguez
Jazmin Huerta-Cantillo
Lucia Chavez-Dueñas
Fernando Navarro-Garcia
Vanessa Sperandio
spellingShingle Farid Tejeda-Dominguez
Jazmin Huerta-Cantillo
Lucia Chavez-Dueñas
Fernando Navarro-Garcia
Vanessa Sperandio
A Novel Mechanism for Protein Delivery by the Type 3 Secretion System for Extracellularly Secreted Proteins
mBio
author_facet Farid Tejeda-Dominguez
Jazmin Huerta-Cantillo
Lucia Chavez-Dueñas
Fernando Navarro-Garcia
Vanessa Sperandio
author_sort Farid Tejeda-Dominguez
title A Novel Mechanism for Protein Delivery by the Type 3 Secretion System for Extracellularly Secreted Proteins
title_short A Novel Mechanism for Protein Delivery by the Type 3 Secretion System for Extracellularly Secreted Proteins
title_full A Novel Mechanism for Protein Delivery by the Type 3 Secretion System for Extracellularly Secreted Proteins
title_fullStr A Novel Mechanism for Protein Delivery by the Type 3 Secretion System for Extracellularly Secreted Proteins
title_full_unstemmed A Novel Mechanism for Protein Delivery by the Type 3 Secretion System for Extracellularly Secreted Proteins
title_sort novel mechanism for protein delivery by the type 3 secretion system for extracellularly secreted proteins
publisher American Society for Microbiology
series mBio
issn 2150-7511
publishDate 2017-03-01
description The type 3 secretion system (T3SS) is essential for bacterial virulence through delivering effector proteins directly into the host cytosol. Here, we identified an alternative delivery mechanism of virulence factors mediated by the T3SS, which consists of the association of extracellularly secreted proteins from bacteria with the T3SS to gain access to the host cytosol. Both EspC, a protein secreted as an enteropathogenic Escherichia coli (EPEC) autotransporter, and YopH, a protein detected on the surface of Yersinia, require a functional T3SS for host cell internalization; here we provide biophysical and molecular evidence to support the concept of the EspC translocation mechanism, which requires (i) an interaction between EspA and an EspC middle segment, (ii) an EspC translocation motif (21 residues that are shared with the YopH translocation motif), (iii) increases in the association and dissociation rates of EspC mediated by EspA interacting with EspD, and (iv) an interaction of EspC with the EspD/EspB translocon pore. Interestingly, this novel mechanism does not exclude the injection model (i.e., EspF) operating through the T3SS conduit; therefore, T3SS can be functioning as an internal conduit or as an external railway, which can be used to reach the translocator pore, and this mechanism appears to be conserved among different T3SS-dependent pathogens.
url http://mbio.asm.org/cgi/content/full/8/2/e00184-17
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