α-Helices in the Type III Secretion Effectors: A Prevalent Feature with Versatile Roles

Type III Secretion Systems (T3SSs) are multicomponent nanomachines located at the cell envelope of Gram-negative bacteria. Their main function is to transport bacterial proteins either extracellularly or directly into the eukaryotic host cell cytoplasm. Type III Secretion effectors (T3SEs), latest to be secreted T3S substrates, are destined to act at the eukaryotic host cell cytoplasm and occasionally at the nucleus, hijacking cellular processes through mimicking eukaryotic proteins. A broad range of functions is attributed to T3SEs, ranging from the manipulation of the host cell’s metabolism for the benefit of the bacterium to bypassing the host’s defense mechanisms. To perform this broad range of manipulations, T3SEs have evolved numerous novel folds that are compatible with some basic requirements: they should be able to easily unfold, pass through the narrow T3SS channel, and refold to an active form when on the other side. In this review, the various folds of T3SEs are presented with the emphasis placed on the functional and structural importance of α-helices and helical domains.

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Identification ofChlamydia trachomatisCT621, a protein delivered through the type III secretion system to the host cell cytoplasm and nucleus

FEMS Immunology & Medical Microbiology ◽

10.1111/j.1574-695x.2009.00581.x ◽

2009 ◽

Vol 57 (1) ◽

pp. 46-58 ◽

Cited By ~ 33

Author(s):

Anne-Sofie Hobolt-Pedersen ◽

Gunna Christiansen ◽

Evy Timmerman ◽

Kris Gevaert ◽

Svend Birkelund

Keyword(s):

Host Cell ◽

Type Iii Secretion ◽

Type Iii Secretion System ◽

Secretion System ◽

Cell Cytoplasm ◽

Type Iii ◽

Host Cell Cytoplasm

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Eukaryotic Cell Permeabilisation to Identify New Putative Chlamydial Type III Secretion System Effectors Secreted within Host Cell Cytoplasm

Microorganisms ◽

10.3390/microorganisms8030361 ◽

2020 ◽

Vol 8 (3) ◽

pp. 361 ◽

Cited By ~ 1

Author(s):

Carole Kebbi-Beghdadi ◽

Ludovic Pilloux ◽

Virginie Martin ◽

Gilbert Greub

Keyword(s):

Host Cell ◽

Type Iii Secretion ◽

Plasma Membranes ◽

Type Iii Secretion System ◽

Secretion System ◽

Effector Proteins ◽

Cell Cytoplasm ◽

Type Iii ◽

Host Cell Cytoplasm ◽

Adverse Pregnancy

Chlamydia trachomatis and Waddlia chondrophila are strict intracellular bacteria belonging to the Chlamydiales order. C. trachomatis is the most frequent bacterial cause of genital and ocular infections whereas W. chondrophila is an opportunistic pathogen associated with adverse pregnancy outcomes and respiratory infections. Being strictly intracellular, these bacteria are engaged in a complex interplay with their hosts to modulate their environment and create optimal conditions for completing their life cycle. For this purpose, they possess several secretion pathways and, in particular, a Type III Secretion System (T3SS) devoted to the delivery of effector proteins in the host cell cytosol. Identifying these effectors is a crucial step in understanding the molecular basis of bacterial pathogenesis. Following incubation of infected cells with perfringolysin O, a pore-forming toxin that binds cholesterol present in plasma membranes, we analysed by mass spectrometry the protein content of the host cell cytoplasm. We identified 13 putative effectors secreted by C. trachomatis and 19 secreted by W. chondrophila. Using Y. enterocolitica as a heterologous expression and secretion system, we confirmed that four of these identified proteins are secreted by the T3SS. Two W. chondrophila T3SS effectors (hypothetical proteins Wcw_0499 and Wcw_1706) were further characterised and demonstrated to be early/mid-cycle effectors. In addition, Wcw_1706 is associated with a tetratricopeptide domain-containing protein homologous to C. trachomatis class II chaperone. Furthermore, we identified a novel C. trachomatis effector, CT460 that localises in the eukaryotic nucleus when ectopically expressed in 293 T cells.

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Identification of Novel Host Interactors of Effectors Secreted by Salmonella and Citrobacter

mSystems ◽

10.1128/msystems.00032-15 ◽

2016 ◽

Vol 1 (4) ◽

Cited By ~ 9

Author(s):

Ryan L. Sontag ◽

Ernesto S. Nakayasu ◽

Roslyn N. Brown ◽

George S. Niemann ◽

Michael A. Sydor ◽

...

Keyword(s):

Host Cell ◽

Type Iii Secretion ◽

Defense Mechanisms ◽

Pathogenic Bacteria ◽

Effector Proteins ◽

Host Cells ◽

Secretion Systems ◽

Type Iii ◽

Cell Cytosol ◽

Host Cell Cytosol

ABSTRACT During infection, pathogenic bacteria face an adverse environment of factors driven by both cellular and humoral defense mechanisms. To help evade the immune response and ultimately proliferate inside the host, many bacteria evolved specialized secretion systems to deliver effector proteins directly into host cells. Translocated effector proteins function to subvert host defense mechanisms. Numerous pathogenic bacteria use a specialized secretion system called type III secretion to deliver effectors into the host cell cytosol. Here, we identified 75 new host targets of Salmonella and Citrobacter effectors, which will help elucidate their mechanisms of action. Many pathogenic bacteria of the family Enterobacteriaceae use type III secretion systems to inject virulence proteins, termed “effectors,” into the host cell cytosol. Although host-cellular activities of several effectors have been demonstrated, the function and host-targeted pathways of most of the effectors identified to date are largely undetermined. To gain insight into host proteins targeted by bacterial effectors, we performed coaffinity purification of host proteins from cell lysates using recombinant effectors from the Enterobacteriaceae intracellular pathogens Salmonella enterica serovar Typhimurium and Citrobacter rodentium. We identified 54 high-confidence host interactors for the Salmonella effectors GogA, GtgA, GtgE, SpvC, SrfH, SseL, SspH1, and SssB collectively and 21 interactors for the Citrobacter effectors EspT, NleA, NleG1, and NleK. We biochemically validated the interaction between the SrfH Salmonella protein and the extracellular signal-regulated kinase 2 (ERK2) host protein kinase, which revealed a role for this effector in regulating phosphorylation levels of this enzyme, which plays a central role in signal transduction. IMPORTANCE During infection, pathogenic bacteria face an adverse environment of factors driven by both cellular and humoral defense mechanisms. To help evade the immune response and ultimately proliferate inside the host, many bacteria evolved specialized secretion systems to deliver effector proteins directly into host cells. Translocated effector proteins function to subvert host defense mechanisms. Numerous pathogenic bacteria use a specialized secretion system called type III secretion to deliver effectors into the host cell cytosol. Here, we identified 75 new host targets of Salmonella and Citrobacter effectors, which will help elucidate their mechanisms of action.

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Type III Secretion Systems and Disease

Clinical Microbiology Reviews ◽

10.1128/cmr.00013-07 ◽

2007 ◽

Vol 20 (4) ◽

pp. 535-549 ◽

Cited By ~ 294

Author(s):

Bryan Coburn ◽

Inna Sekirov ◽

B. Brett Finlay

Keyword(s):

Host Cell ◽

Type Iii Secretion ◽

Human Infection ◽

Effector Proteins ◽

Secretion Systems ◽

Barrier Dysfunction ◽

Type Iii ◽

Extracellular Milieu ◽

Host Cell Cytoplasm ◽

Type Iii Secretion Systems

SUMMARY Type III secretion systems (T3SSs) are complex bacterial structures that provide gram-negative pathogens with a unique virulence mechanism enabling them to inject bacterial effector proteins directly into the host cell cytoplasm, bypassing the extracellular milieu. Although the effector proteins vary among different T3SS pathogens, common pathogenic mechanisms emerge, including interference with the host cell cytoskeleton to promote attachment and invasion, interference with cellular trafficking processes, cytotoxicity and barrier dysfunction, and immune system subversion. The activity of the T3SSs correlates closely with infection progression and outcome, both in animal models and in human infection. Therefore, to facilitate patient care and improve outcomes, it is important to understand the T3SS-mediated virulence processes and to target T3SSs in therapeutic and prophylactic development efforts.

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The EspB Protein of EnteropathogenicEscherichia coli Is Targeted to the Cytoplasm of Infected HeLa Cells

Infection and Immunity ◽

10.1128/iai.66.11.5501-5507.1998 ◽

1998 ◽

Vol 66 (11) ◽

pp. 5501-5507 ◽

Cited By ~ 78

Author(s):

Kathleen A. Taylor ◽

Colin B. O’Connell ◽

Paul W. Luther ◽

Michael S. Donnenberg

Keyword(s):

Host Cell ◽

Hela Cells ◽

Type Iii Secretion ◽

Laser Scanning ◽

Laser Scanning Microscopy ◽

Confocal Laser ◽

Cell Cytoplasm ◽

Type Iii ◽

Host Cell Cytoplasm ◽

Infected Cells

ABSTRACT The EspB protein of enteropathogenic Escherichia coli(EPEC) is exported via a type III secretion apparatus. EspB is critical for signaling the host cell and for the development of the attaching and effacing lesion characteristic of EPEC infection. We used cellular fractionation and confocal laser scanning microscopy to determine the cellular location of EspB during infection of HeLa cells. Both methods indicated that EspB is targeted to the cytoplasm of infected cells. Using mutants, we found that EspB targeting to the host cell cytoplasm requires the type III secretion apparatus and the secreted proteins EspA and EspD, but not intimin. These results provide insights into the function of the type III secretion apparatus of EPEC and the functions of the Esp proteins.

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Identification of a Family of Effectors Secreted by the Type III Secretion System That Are Conserved in Pathogenic Chlamydiae

Infection and Immunity ◽

10.1128/iai.00825-10 ◽

2010 ◽

Vol 79 (2) ◽

pp. 571-580 ◽

Cited By ~ 23

Author(s):

Sandra Muschiol ◽

Gaelle Boncompain ◽

François Vromman ◽

Pierre Dehoux ◽

Staffan Normark ◽

...

Keyword(s):

Host Cell ◽

Type Iii Secretion ◽

Effector Proteins ◽

Main Process ◽

Cell Cytoplasm ◽

Type Iii ◽

Amino Terminal ◽

Cell Functions ◽

Host Cell Cytoplasm ◽

Infectious Cycle

ABSTRACTChlamydiae are Gram-negative, obligate intracellular pathogens that replicate within a membrane-bounded compartment termed an inclusion. Throughout their development, they actively modify the eukaryotic environment. The type III secretion (TTS) system is the main process by which the bacteria translocate effector proteins into the inclusion membrane and the host cell cytoplasm. Here we describe a family of type III secreted effectors that are present in all pathogenic chlamydiae and absent in the environment-related species. It is defined by a common domain of unknown function, DUF582, that is present in four or five proteins in eachChlamydiaceaespecies. We show that the amino-terminal extremity of DUF582 proteins functions as a TTS signal. DUF582 proteins fromC. trachomatisCT620, CT621, and CT711 are expressed at the middle and late phases of the infectious cycle. Immunolocalization further revealed that CT620 and CT621 are secreted into the host cell cytoplasm, as well as within the lumen of the inclusion, where they do not associate with bacterial markers. Finally, we show that DUF582 proteins are present in nuclei of infected cells, suggesting that members of the DUF582 family of effector proteins may target nuclear cell functions. The expansion of this family of proteins in pathogenic chlamydiae and their conservation among the different species suggest that they play important roles in the infectious cycle.

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The Type III Pseudomonal Exotoxin U Activates the c-Jun NH2-Terminal Kinase Pathway and Increases Human Epithelial Interleukin-8 Production

Infection and Immunity ◽

10.1128/iai.02045-05 ◽

2006 ◽

Vol 74 (7) ◽

pp. 4104-4113 ◽

Cited By ~ 25

Author(s):

Alayne Cuzick ◽

Fiona R. Stirling ◽

Susan L. Lindsay ◽

Thomas J. Evans

Keyword(s):

Inflammatory Response ◽

Host Cell ◽

Type Iii Secretion ◽

Interleukin 8 ◽

Specific Gene ◽

Secretion Systems ◽

Type Iii ◽

Host Inflammatory Response ◽

Kinase Pathway ◽

Bacterial Type

ABSTRACT Microbial interactions with host cell signaling pathways are key determinants of the host cell response to infection. Many toxins secreted by bacterial type III secretion systems either stimulate or inhibit the host inflammatory response. We investigated the role of type III secreted toxins of the lung pathogen Pseudomonas aeruginosa in the inflammatory response of human respiratory epithelial cells to infection. Using bacteria with specific gene deletions, we found that interleukin-8 production by these cells was almost entirely dependent on bacterial type III secretion of exotoxin U (ExoU), a phospholipase, although other bacterial factors are involved. ExoU activated the c-Jun NH2-terminal kinase pathway, stimulating the phosphorylation and activation of mitogen-activated kinase kinase 4, c-Jun NH2-terminal kinase, and c-Jun. This in turn increased levels of transcriptionally competent activator protein-1. Although this pathway was dependent on the lipase activity of ExoU, it was independent of cell death. Activation of mitogen-activated kinase signaling by ExoU in this fashion is a novel mechanism by which a bacterial product can initiate a host inflammatory response, and it may result in increased epithelial permeability and bacterial spread.

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Effect of the O-Antigen Length of Lipopolysaccharide on the Functions of Type III Secretion Systems in Salmonella enterica

Infection and Immunity ◽

10.1128/iai.00871-09 ◽

2009 ◽

Vol 77 (12) ◽

pp. 5458-5470 ◽

Cited By ~ 50

Author(s):

Stefanie U. Hölzer ◽

Markus C. Schlumberger ◽

Daniela Jäckel ◽

Michael Hensel

Keyword(s):

Type Iii Secretion ◽

Salmonella Enterica ◽

Defense Mechanisms ◽

Host Cells ◽

Effector Protein ◽

Secretion Systems ◽

Type Iii ◽

O Antigen ◽

T3ss Effector ◽

Type Iii Secretion Systems

ABSTRACT The virulence of Salmonella enterica critically depends on the functions of two type III secretion systems (T3SS), with the Salmonella pathogenicity island 1 (SPI1)-encoded T3SS required for host cell invasion and the SPI2-T3SS enabling Salmonella to proliferate within host cells. A further T3SS is required for the assembly of the flagella. Most serovars of Salmonella also possess a lipopolysaccharide with a complex O-antigen (OAg) structure. The number of OAg units attached to the core polysaccharide varies between 16 and more than 100 repeats, with a trimodal distribution. This work investigated the correlation of the OAg length with the functions of the SPI1-T3SS and the SPI2-T3SS. We observed that the number of repeats of OAg units had no effect on bacterial motility. The interaction of Salmonella with epithelial cells was altered if the OAg structure was changed by mutations in regulators of OAg. Strains defective in synthesis of very long or long and very long OAg species showed increased translocation of a SPI1-T3SS effector protein and increased invasion. Invasion of a strain entirely lacking OAg was increased, but this mutant strain also showed increased adhesion. In contrast, translocation of a SPI2-T3SS effector protein and intracellular replication were not affected by modification of the OAg length. Mutant strains lacking the entire OAg or long and very long OAg were highly susceptible to complement killing. These observations indicate that the architecture of the outer membrane of Salmonella is balanced to permit sufficient T3SS function but also to confer optimal protection against antimicrobial defense mechanisms.

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Identification of a Specific Chaperone for SptP, a Substrate of the Centisome 63 Type III Secretion System ofSalmonella typhimurium

Journal of Bacteriology ◽

10.1128/jb.180.13.3393-3399.1998 ◽

1998 ◽

Vol 180 (13) ◽

pp. 3393-3399 ◽

Cited By ~ 73

Author(s):

Yixin Fu ◽

Jorge E. Galán

Keyword(s):

Actin Cytoskeleton ◽

Host Cell ◽

Type Iii Secretion ◽

Tyrosine Phosphatase ◽

Secretion System ◽

Effector Proteins ◽

Loss Of Function ◽

Secretion Systems ◽

Type Iii ◽

Type Iii Protein Secretion

ABSTRACT Salmonella typhimurium uses of a type III protein secretion system encoded at centisome 63 of its chromosome to deliver effector molecules into the host cell. These proteins stimulate host cell responses such as reorganization of the actin cytoskeleton and activation of transcription factors. One of these effector proteins is SptP, a tyrosine phosphatase that causes disruption of the host cell actin cytoskeleton. A characteristic feature of many substrates of type III secretion systems is their association with specific cytoplasmic chaperones which appears to be required for secretion and/or translocation of these proteins into the host cell. We report here the identification of SicP, a 13-kDa acidic polypeptide that is encoded immediately upstream of sptP. A loss-of-function mutation in sicP resulted in drastically reduced levels of SptP but did not affect sptP expression, indicating that SicP exerts its effect posttranscriptionally. Pulse-chase experiments demonstrated that the loss of SicP leads to increased degradation of SptP. In addition, we show that SicP binds to SptP directly and that the binding site is located between residues 15 and 100 of the tyrosine phosphatase. Taken together, these results indicate that SicP acts as a specific chaperone for SptP.

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Type III Protein Secretion Systems in Bacterial Pathogens of Animals and Plants

Microbiology and Molecular Biology Reviews ◽

10.1128/mmbr.62.2.379-433.1998 ◽

1998 ◽

Vol 62 (2) ◽

pp. 379-433 ◽

Cited By ~ 1674

Author(s):

Christoph J. Hueck

Keyword(s):

Host Cell ◽

Protein Secretion ◽

Type Iii Secretion ◽

Plant Pathogens ◽

Host Cells ◽

Secretion Systems ◽

Type Iii ◽

Type Iii Secretion Systems ◽

Animal Pathogens ◽

Type Iii Protein Secretion

SUMMARY Various gram-negative animal and plant pathogens use a novel, sec-independent protein secretion system as a basic virulence mechanism. It is becoming increasingly clear that these so-called type III secretion systems inject (translocate) proteins into the cytosol of eukaryotic cells, where the translocated proteins facilitate bacterial pathogenesis by specifically interfering with host cell signal transduction and other cellular processes. Accordingly, some type III secretion systems are activated by bacterial contact with host cell surfaces. Individual type III secretion systems direct the secretion and translocation of a variety of unrelated proteins, which account for species-specific pathogenesis phenotypes. In contrast to the secreted virulence factors, most of the 15 to 20 membrane-associated proteins which constitute the type III secretion apparatus are conserved among different pathogens. Most of the inner membrane components of the type III secretion apparatus show additional homologies to flagellar biosynthetic proteins, while a conserved outer membrane factor is similar to secretins from type II and other secretion pathways. Structurally conserved chaperones which specifically bind to individual secreted proteins play an important role in type III protein secretion, apparently by preventing premature interactions of the secreted factors with other proteins. The genes encoding type III secretion systems are clustered, and various pieces of evidence suggest that these systems have been acquired by horizontal genetic transfer during evolution. Expression of type III secretion systems is coordinately regulated in response to host environmental stimuli by networks of transcription factors. This review comprises a comparison of the structure, function, regulation, and impact on host cells of the type III secretion systems in the animal pathogens Yersinia spp., Pseudomonas aeruginosa, Shigella flexneri, Salmonella typhimurium, enteropathogenic Escherichia coli, and Chlamydia spp. and the plant pathogens Pseudomonas syringae, Erwinia spp., Ralstonia solanacearum, Xanthomonas campestris, and Rhizobium spp.

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