Your search keyword '"Coombes, Brian K."' showing total 13 results

1. NleG Type 3 Effectors from Enterohaemorrhagic Escherichia coli Are U-Box E3 Ubiquitin Ligases.

Author

Bin Wu, Skarina, Tatiana, Yee, Adelinda, Jobin, Marie-Claude, DiLeo, Rosa, Semesi, Anthony, Fares, Christophe, Lemak, Alexander, Coombes, Brian K., Arrowsmith, Cheryl H., Singer, Alexander U., and Savchenko, Alexei

Subjects

ESCHERICHIA coli, PATHOGENIC microorganisms, HOMOLOGY (Biology), MICROBIOLOGICAL assay, EUKARYOTIC cells, UBIQUITIN, MUTAGENESIS

Abstract

NleG homologues constitute the largest family of type 3 effectors delivered by pathogenic E. coli, with fourteen members in the enterohaemorrhagic (EHEC) O157:H7 strain alone. Identified recently as part of the non-LEE-encoded (Nle) effector set, this family remained uncharacterised and shared no sequence homology to other proteins including those of known function. The C-terminal domain of NleG2-3 (residues 90 to 191) is the most conserved region in NleG proteins and was solved by NMR. Structural analysis of this structure revealed the presence of a RING finger/U-box motif. Functional assays demonstrated that NleG2-3 as well as NleG5-1, NleG6-2 and NleG9′ family members exhibited a strong autoubiquitination activity in vitro; a characteristic usually expressed by eukaryotic ubiquitin E3 ligases. When screened for activity against a panel of 30 human E2 enzymes, the NleG2-3 and NleG5-1 homologues showed an identical profile with only UBE2E2, UBE2E3 and UBE2D2 enzymes supporting NleG activity. Fluorescence polarization analysis yielded a binding affinity constant of 56 ± μM for the UBE2D2/NleG5-1 interaction, a value comparable with previous studies on E2/E3 affinities. The UBE2D2 interaction interface on NleG2-3 defined by NMR chemical shift perturbation and mutagenesis was shown to be generally similar to that characterised for human RING finger ubiquitin ligases. The alanine substitutions of UBE2D2 residues Arg5 and Lys63, critical for activation of eukaryotic E3 ligases, also significantly decreased both NleG binding and autoubiquitination activity. These results demonstrate that bacteria-encoded NleG effectors are E3 ubiquitin ligases analogous to RING finger and U-box enzymes in eukaryotes. [ABSTRACT FROM AUTHOR]

Published

2010

2. Structural and Biochemical Characterization of SrcA, a Multi-Cargo Type III Secretion Chaperone in Salmonella Required for Pathogenic Association with a Host.

Author

Cooper, Colin A., Kun Zhang, Andres, Sara N., Yuan Fang, Kaniuk, Natalia A., Hannemann, Mandy, Brumell, John H., Foster, Leonard J., Junop, Murray S., and Coombes, Brian K.

Subjects

REGULATION of secretion, BIOMARKERS, MOLECULAR chaperones, PATHOGENIC microorganisms, GRAM-negative bacteria, PATHOGENIC bacteria

Abstract

Many Gram-negative bacteria colonize and exploit host niches using a protein apparatus called a type III secretion system (T3SS) that translocates bacterial effector proteins into host cells where their functions are essential for pathogenesis. A suite of T3SS-associated chaperone proteins bind cargo in the bacterial cytosol, establishing protein interaction networks needed for effector translocation into host cells. In Salmonella enterica serovar Typhimurium, a T3SS encoded in a large genomic island (SPI-2) is required for intracellular infection, but the chaperone complement required for effector translocation by this system is not known. Using a reverse genetics approach, we identified a multi-cargo secretion chaperone that is functionally integrated with the SPI-2-encoded T3SS and required for systemic infection in mice. Crystallographic analysis of SrcA at a resolution of 2.5 Å revealed a dimer similar to the CesT chaperone from enteropathogenic E. coli but lacking a 17-amino acid extension at the carboxyl terminus. Further biochemical and quantitative proteomics data revealed three protein interactions with SrcA, including two effector cargos (SseL and PipB2) and the type III-associated ATPase, SsaN, that increases the efficiency of effector translocation. Using competitive infections in mice we show that SrcA increases bacterial fitness during host infection, highlighting the in vivo importance of effector chaperones for the SPI-2 T3SS. [ABSTRACT FROM AUTHOR]

Published

2010

3. Pathogenic adaptation of intracellular bacteria by rewiring a cis-regulatory input function.

Author

Osborne, Suzanne E., Walthers, Don, Tomljenovic, Ana M., Mulder, David T., Silphaduang, Uma, Duong, Nancy, Lowden, Michael J., Wickham, Mark E., Waller, Ross F., Kenney, Linda J., and Coombes, Brian K.

Subjects

DNA, GENETIC transformation, BACTERIA, ENDEMIC flea-borne typhus, SALMONELLA, GENETIC mutation, PATHOGENIC microorganisms, BINDING sites

Abstract

The acquisition of DNA by horizontal gene transfer enables bacteria to adapt to previously unexploited ecological niches. Although horizontal gene transfer and mutation of protein-coding sequences are well-recognized forms of pathogen evolution, the evolutionary significance of cis-regulatory mutations in creating phenotypic diversity through altered transcriptional outputs is not known. We show the significance of regulatory mutation for pathogen evolution by mapping and then rewiring a cis-regulatory module controlling a gene required for murine typhoid. Acquisition of a binding site for the Salmonella pathogenicity island-2 regulator, SsrB, enabled the srfN gene, ancestral to the Salmonella genus, to play a role in pathoadaptation of S. typhimurium to a host animal. We identified the evolved cis-regulatory module and quantified the fitness gain that this regulatory output accrues for the bacterium using competitive infections of host animals. Our findings highlight a mechanism of pathogen evolution involving regulatory mutation that is selected because of the fitness advantage the new regulatory output provides the incipient clones. [ABSTRACT FROM AUTHOR]

Published

2009

4. FimH Adhesin of Type 1 Fimbriae Is a Potent Inducer of Innate Antimicrobial Responses Which Requires TLR4 and Type 1 Interferon Signalling.

Author

Ashkar, Ali A., Mossman, Karen L., Coombes, Brian K., Gyles, Carlton L., and Mackenzie, Randy

Subjects

IMMUNITY, PILI (Microbiology), ANTIVIRAL agents, IMMUNE response, PATHOGENIC microorganisms

Abstract

Components of bacteria have been shown to induce innate antiviral immunity via Toll-like receptors (TLRs). We have recently shown that FimH, the adhesin portion of type 1 fimbria, can induce the innate immune system via TLR4. Here we report that FimH induces potent in vitro and in vivo innate antimicrobial responses. FimH induced an innate antiviral state in murine macrophage and primary MEFs which was correlated with IFN-β production. Moreover, FimH induced the innate antiviral responses in cells from wild type, but not from MyD88-/-, Trif-/-, IFN2α/βR-/- or IRF3-/- mice. Vaginal delivery of FimH, but not LPS, completely protected wild type, but not MyD88-/-, IFN-α/βR-/-, IRF3-/- or TLR4-/- mice from subsequent genital HSV-2 challenge. The FimH-induced innate antiviral immunity correlated with the production of IFN-β, but not IFN-α or IFN-γ. To examine whether FimH plays a role in innate immune induction in the context of a natural infection, the innate immune responses to wild type uropathogenic E. coli (UPEC) and a FimH null mutant were examined in the urinary tract of C57Bl/6 (B6) mice and TLR4-deficient mice. While UPEC expressing FimH induced a robust polymorphonuclear response in B6, but not TLR4-/- mice, mutant bacteria lacking FimH did not. In addition, the presence of TLR4 was essential for innate control of and protection against UPEC. Our results demonstrate that FimH is a potent inducer of innate antimicrobial responses and signals differently, from that of LPS, via TLR4 at mucosal surfaces. Our studies suggest that FimH can potentially be used as an innate microbicide against mucosal pathogens. [ABSTRACT FROM AUTHOR]

Published

2008

5. Bacterial Genetic Determinants of Non-O157 STEC Outbreaks and Hemolytic-Uremic Syndrome after Infection.

Author

Wickham, Mark E., Lupp, Claudia, Mascarenhas, Mariola, Vázquez, Alejandra, Coombes, Brian K., Brown, Nat F., Coburn, Bryan A., Deng, Wanyin, Puente^1,4, José L., Karmali, Mohamed A., and Finlay, B. Brett

Subjects

HEMOLYTIC anemia, VEROCYTOTOXINS, ESCHERICHIA coli, PATHOGENIC microorganisms, MICROBIAL virulence

Abstract

Although O157:H7 Shiga toxin-producing Escherichia coli (STEC) are the predominant cause of hemolyticuremic syndrome (HUS) in the world, non-O157:H7 serotypes are a medically important cause of HUS that are underdetected by current diagnostic approaches. Because Shiga toxin is necessary but not sufficient to cause HUS, identifying the virulence determinants that predict severe disease after non-O157 STEC infection is of paramount importance. Disease caused by O157:H7 STEC has been associated with a 26-gene pathogenicity island known as O island (OI) 122. To assess the public-health significance of this pathogenicity island, we examined the association between OI122 genes and outbreaks and HUS after non-O157 STEC infection. We found that a subset of OI122 genes is independently associated with outbreaks and HUS after infection with non-O157 STEC. The presence of multiple virulence genes in non-O157 serotypes strengthened this association, which suggests that the additive effects of a variable repertoire of virulence genes contribute to disease severity. In vivo, Citrobacter rodentium mutants lacking outbreak- and HUS-associated genes were deficient for virulence in mice; in particular, nleB mutant bacteria were unable to cause mortality in mice. The present study shows that virulence genes associated epidemiologically with outbreaks and HUS after non-O157 STEC infection are pivotal to the initiation, progression, and outcome of in vivo disease. [ABSTRACT FROM AUTHOR]

Published

2006

6. Crossing the Line: Selection and Evolution of Virulence Traits.

Author

Brown, Nat F., Wickham, Mark E., Coombes, Brian K., and Finlay, B. Brett

Subjects

HOST-parasite relationships, PATHOGENIC microorganisms, MICROBIAL virulence -- Molecular aspects, MOLECULAR biology, PARASITISM

Abstract

The evolution of pathogens presents a paradox. Pathogenic species are often absolutely dependent on their host species for their propagation through evolutionary time, yet the pathogenic lifestyle requires that the host be damaged during this dependence. It is clear that pathogenic strategies are successful in evolutionary terms because a diverse array of pathogens exists in nature. Pathogens also evolve using a broad range of molecular mechanisms to acquire and modulate existing virulence traits in order to achieve this success. Detailing the benefit of enhanced selection derived through virulence and understanding the mechanisms through which virulence evolves are important to understanding the natural world and both have implications for human health. [ABSTRACT FROM AUTHOR]

Published

2006

7. Genetic and Molecular Analysis of GogB, a Phage-encoded Type III-secreted Substrate in Salmonella enterica Serovar Typhimurium with Autonomous Expression from its Associated Phage

Author

Coombes, Brian K., Wickham, Mark E., Brown, Nat. F., Lemire, Sebastien, Bossi, Lionello, Hsiao, William W.L., Brinkman, Fiona S.L., and Finlay, B. Brett

Subjects

*SALMONELLA, *PATHOGENIC microorganisms, *PROTEINS, *GLANDS

Abstract

Salmonella enterica serovar Typhimurium is lysogenized by several temperate bacteriophages that encode lysogenic conversion genes, which can act as virulence factors during infection and contribute to the genetic diversity and pathogenic potential of the lysogen. We have investigated the temperate bacteriophage called Gifsy-1 in S.enterica serovar Typhimurium and show here that the product of the gogB gene encoded within this phage shares similarity with proteins from other Gram-negative pathogens. The amino-terminal portion of GogB shares similarity with leucine-rich repeat-containing virulence-associated proteins from other Gram-negative pathogens, whereas the carboxyl-terminal portion of GogB shares similarity with uncharacterized proteins in other pathogens. We show that GogB is secreted by both type III secretion systems encoded in Salmonella Pathogenicity Island-1 (SPI-1) and SPI-2 but translocation into host cells is a SPI-2-mediated process. Once translocated, GogB localizes to the cytoplasm of infected host cells. The genetic regulation of gogB in Salmonella is influenced by the transcriptional activator, SsrB, under SPI-2-inducing conditions, but the modular nature of the gogB gene allows for autonomous expression and type III secretion following horizontal gene transfer into a heterologous pathogen. These data define the first autonomously expressed lysogenic conversion gene within Gifsy-1 that acts as a modular and promiscuous type III-secreted substrate of the infection process. [Copyright &y& Elsevier]

Published

2005

8. Combinations of antibiotics and nonantibiotic drugs enhance antimicrobial efficacy.

Author

Ejim, Linda, Farha, Maya A, Falconer, Shannon B, Wildenhain, Jan, Coombes, Brian K, Tyers, Mike, Brown, Eric D, and Wright, Gerard D

Subjects

ANTIBIOTICS, PATHOGENIC microorganisms, DRUG resistance, DRUG analysis, DRUG efficacy

Abstract

Combinations of antibiotics are commonly used in medicine to broaden antimicrobial spectrum and generate synergistic effects. Alternatively, combination of nonantibiotic drugs with antibiotics offers an opportunity to sample a previously untapped expanse of bioactive chemical space. We screened a collection of drugs to identify compounds that augment the activity of the antibiotic minocycline. Unexpected synergistic drug combinations exhibited in vitro and in vivo activity against bacterial pathogens, including multidrug-resistant isolates. [ABSTRACT FROM AUTHOR]

Published

2011

9. Targeted enrichment of ancient pathogens yielding the pPCP1 plasmid of Yersinia pestis from victims of the Black Death.

Author

Schuenemann, Verena J., Bos, Kirsten, DeWitte, Sharon, Schmedes, Sarah, Jamieson, Joslyn, Mittnik, Alissa, Forrest, Stephen, Coombes, Brian K., Wood, James W., Earn, David J. D., White, William, Krause, Johannes, and Poinar, Hendrik N.

Subjects

BLACK Death pandemic, 1348-1351, YERSINIA pestis, EPIDEMIOLOGICAL research, PATHOGENIC microorganisms, MEDICAL genetics

Abstract

The article presents a study on the possible connection between the bacteria Yersinia pestis (Y. pestis) and the pandemic called Black Death. The authors state that DNA sequence data are collected to help determine epidemiological and ecological differences between the said pandemic and modern epidemic plagues. They add note that ancient pathogens such as in the Black Death is different from the modern Y. pestis.

Published

2011

10. Evasive Maneuvers by Secreted Bacterial Proteins to Avoid Innate Immune Responses

Author

Coombes, Brian K., Valdez, Yanet, and Finlay, B. Brett

Subjects

*IMMUNE response, *IMMUNOLOGY, *PATHOGENIC microorganisms, *PATHOLOGY, *IMMUNE system

Abstract

To cause disease, bacterial pathogens must first breach physical barriers, such as the mucous membrane that lines organs, and then successfully replicate and disseminate while avoiding destruction by the immune system. Many bacterial pathogens accomplish this by secreting proteins into their host environment, which act to subvert or dampen the expanding immune response. Here, we discuss how bacterial pathogens use an arsenal of secreted virulence proteins to modify the outcome of innate immune activation by altering how the immune system recognizes microbial invaders. [Copyright &y& Elsevier]

Published

2004

11. Characterization of DalS, an ATP-binding Cassette Transporter for D-Alanine, and Its Role in Pathogenesis in Salmonella enterica.

Author

Osborne, Suzanne E., Tuinema, Brian R., Mok, Mac C. Y., Pui Sai Lau, Nhat Khai Bui, Tomljenovic-Berube, Ana M., Vollmer, Waldemar, Kun Zhang, Junop, Murray, and Coombes, Brian K.

Subjects

*PATHOGENIC microorganisms, *SALMONELLA enterica, *ATP-binding cassette transporters, *PHAGOSOMES, *DNA, *INFECTION

Abstract

Expansion into new host niches requires bacterial pathogens to adapt to changes in nutrient availability and to evade an arsenal of host defenses. Horizontal acquisition of Salmonella Pathogenicity Island (SPI)-2 permitted the expansion of Salmonella enterica serovar Typhimurium into the intracellular environment of host cells by allowing it to deliver bacterial effector proteins across the phagosome membrane. This is facilitated by the SsrA-SsrB two-component regulatory system and a type III secretion system encoded within SPI-2. SPI-2 acquisition was followed by evolution of existing regulatory DNA, creating an expanded SsrB regulon involved in intracellular fitness and host infection. Here, we identified an SsrB-regulated operon comprising an ABC transporter in Salmonella. Biochemical and structural studies determined that the periplasmic solute-binding component, STM1633/DalS, transports D-alanine and that DalS is required for intracellular survival of the bacteria and for fitness in an animal host. This work exemplifies the role of nutrient exchange at the host-pathogen interface as a critical determinant of disease outcome. [ABSTRACT FROM AUTHOR]

Published

2012

12. Virulence Is Positively Selected by Transmission Success between Mammalian Hosts

Author

Wickham, Mark E., Brown, Nat F., Boyle, Erin C., Coombes, Brian K., and Finlay, B. Brett

Subjects

*PATHOGENIC microorganisms, *CYTOPLASM, *COMMUNICABLE diseases, *PATHOGENIC bacteria

Abstract

Summary: Virulence, defined as damage to the host, is a trait of pathogens that evolutionary theory suggests benefits the pathogen in the “struggle for existence”. Pathogens employ virulence mechanisms that contribute to disease. Central to the evolution of virulence of the infectious agents causing an array of bacterial disease is the evolutionary acquisition of type III secretion, a macromolecular complex that creates a syringe-like apparatus extending from the bacterial cytosol to the eukaryotic cytosol and delivers secreted bacterial virulence factors (effectors) into host cells. In this work, we quantify the contribution of virulence determinants to the evolutionary success of a pathogen. Using a natural pathogen of mice, we show that virulence factors provide a selective advantage by enhancing transmission between hosts. Virulence factors that have a major contribution to disease were absolutely required for transmission of the pathogen to naive hosts. Virulence-factor mutants with more subtle defects in pathogenesis had quantifiable roles in the time required to transmit the pathogen between mice. Virulence-factor mutants were also found to lose in competition with wild-type bacteria when iteratively transmitted from infected to uninfected mice. These results directly demonstrate that virulence is selected via the fitness advantage it provides to the host-to-host cycle of pathogenic species. [Copyright &y& Elsevier]

Published

2007

13. Citrobacter rodentium virulence in mice associates with bacterial load and the type III effector NleE

Author

Wickham, Mark E., Lupp, Claudia, Vázquez, Alejandra, Mascarenhas, Mariola, Coburn, Bryan, Coombes, Brian K., Karmali, Mohamed A., Puente, José L., Deng, Wanyin, and Brett Finlay, B.

Subjects

*ESCHERICHIA, *ESCHERICHIA coli, *MORTALITY, *PATHOGENIC microorganisms

Abstract

Abstract: Severe disease caused by Shiga toxin-producing Escherichia coli (STEC) has been associated with a pathogenicity island, O-Island 122, which encodes the type III secretion system-effector NleE. Here we show that full virulence of the related attaching and effacing mouse pathogen Citrobacter rodentium requires NleE. Relative to wild-type bacteria, nleE-mutant C. rodentium are attenuated for colonisation in mice in both single and mixed infections. Examination of the ability of nleE-mutant bacteria to induce pathologic change in vivo revealed that nleE-mutant bacteria induce significantly less pathologic change than wild-type bacteria in susceptible mice. Consistent with these results, mice infected with nleE-mutant bacteria exhibit delayed mortality. These results suggested that pathologic change during attaching and effacing pathogen infection may associate with the degree of pathogen colonisation. Using mutants of 23 type III secretion genes, including the type III effectors nleC, nleD, nleE and nleF, the association of pathologic change with the ability of these mutants to colonise mice was examined. The induction of in vivo disease correlates strongly with the degree of colonisation, suggesting that the colonisation advantage type III secretion genes afford the bacteria, contribute to, and are required for, full virulence. [Copyright &y& Elsevier]

Published

2007