BtpB, a novel Brucella TIR-containing effector protein with immune modulatory functions

Salcedo, Suzana P.; Marchesini, María Inés; Degos, Clara; Terwagne, Matthiew; Bargen, Kristine von; Lépidi, Hubert; Herrmann, Claudia; Lacerda, Thaís Lourdes Santos; Imbert, Paul R. C.; Pierre, Philippe; Alexopoulou, Lena; Letesson, Jean‐Jacques; Comerci, Diego J.; Gorvel, Jean‐Pierre

doi:10.3389/fcimb.2013.00028

Cited by 107 publications

(141 citation statements)

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“…24 Redundancy of TcpB/BtpA and BtpB function may explain the failure to identify these immunoregulatory genes by using simple transposon screens. Interaction between BtpA/BtpB and MyD88 may also explain the substantial increase in survival of Brucella in MyD88 À/À knockout mice in contrast to TLR4…”

Section: Central Role For Immunoregulatory Componentsmentioning

confidence: 99%

Pathogenesis and Immunobiology of Brucellosis

Figueiredo

Ficht

Rice‐Ficht

et al. 2015

The American Journal of Pathology

344

270

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This review of Brucellaehost interactions and immunobiology discusses recent discoveries as the basis for pathogenesis-informed rationales to prevent or treat brucellosis. Brucella spp., as animal pathogens, cause human brucellosis, a zoonosis that results in worldwide economic losses, human morbidity, and poverty. Although Brucella spp. infect humans as an incidental host, 500,000 new human infections occur annually, and no patient-friendly treatments or approved human vaccines are reported. Brucellae display strong tissue tropism for lymphoreticular and reproductive systems with an intracellular lifestyle that limits exposure to innate and adaptive immune responses, sequesters the organism from the effects of antibiotics, and drives clinical disease manifestations and pathology. Stealthy brucellae exploit strategies to establish infection, including i) evasion of intracellular destruction by restricting fusion of type IV secretion systemdependent Brucella-containing vacuoles with lysosomal compartments, ii) inhibition of apoptosis of infected mononuclear cells, and iii) prevention of dendritic cell maturation, antigen presentation, and activation of naive T cells, pathogenesis lessons that may be informative for other intracellular pathogens. Data sets of next-generation sequences of Brucella and host time-series global expression fused with proteomics and metabolomics data from in vitro and in vivo experiments now inform interactive cellular pathways and gene regulatory networks enabling full-scale systems biology analysis. The newly identified effector proteins of Brucella may represent targets for improved, safer brucellosis vaccines and therapeutics. It is noteworthy that long ago in his publication Epidemics, Hippocrates described brucellosis-type syndromes in humans living in the Mediterranean littoral. Many centuries later, British physician, David Bruce, and Greek physician, Themistokles Zammit, in 1886 would discover the causative agent, Micrococcus melitensis, of brucellosis and would identify milk products of goats as the source of infection for military troops on the island of Malta. Even after more than a century of extensive research, Brucella spp. are still serious animal pathogens that cause brucellosis, a zoonosis that results in substantial economic losses, human morbidity, and perpetuates poverty worldwide.1 These Gram-negative bacteria infect a diverse array of land and aquatic mammals,

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Section: Central Role For Immunoregulatory Componentsmentioning

confidence: 99%

Pathogenesis and Immunobiology of Brucellosis

Figueiredo

Ficht

Rice‐Ficht

et al. 2015

The American Journal of Pathology

344

270

View full text Add to dashboard Cite

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“…As bacterial TIR proteins down‐modulate NF‐κB activation (Newman et al , 2006; Cirl et al , 2008; Salcedo et al , 2008, 2013; Spear et al , 2012; Askarian et al , 2014; Zou et al , 2014), we infected the lung carcinoma epithelial cell line A549, a well‐established cellular model for Pseudomonas infection and analysed NF‐κB translocation into the nucleus after one hour of infection by confocal microscopy. We developed an automated analysis of p65/RelA fluorescence in relation to DAPI labelling using a specific ImageJ plugin from images obtained by confocal microscopy (Fig EV1A) which allowed us to clearly differentiate between TNFα‐treated and mock‐infected cells (Figs 2A and EV1B).…”

Section: Resultsmentioning

confidence: 99%

“…Bacterial targeting of TLRs has been best described for uropathogenic E. coli TcpC (Cirl et al , 2008) and Brucella BtpA, also known as TcpB (Cirl et al , 2008; Salcedo et al , 2008), even though their molecular mode of action remains elusive. Brucella relies on an additional TIR protein, BtpB to down‐modulate inflammation during infection (Salcedo et al , 2013). TcpC was shown to interfere with MyD88‐dependent and independent pathways to down‐modulate TLR signalling and contribute to kidney pathology (Cirl et al , 2008; Yadav et al , 2010).…”

Section: Discussionmentioning

confidence: 99%

“…In the case of TcpC, internalization into host cells was observed but the export mechanism was not identified (Cirl et al , 2008), whereas no data are available regarding Salmonella , Yersinia, Staphyloccocus and Enteroccoccus . In the case of Brucella , depending on the fusion tags, translocation into host cells of BtpA/TcpB or BtpB was dependent or independent of the T4SS (Salcedo et al , 2013) whereas a separate group has proposed that BtpA/TcpB is cell permeable and may enter host cells in a passive manner (Radhakrishnan & Splitter, 2010). Unfortunately, PumA fusion with CyaA resulted in its cleavage preventing us from using this system.…”

Section: Discussionmentioning

confidence: 99%

“…In contrast, few examples of direct blocking at the level of initial receptor–adaptor complexes are known. Some bacterial pathogens rely on TIR domain‐containing proteins to perturb TIR‐dependent interactions (Newman et al , 2006; Cirl et al , 2008; Salcedo et al , 2008, 2013), essential in innate immune signalling. The growing number of bacterial TIR proteins recently identified in both Gram‐negative and Gram‐positive human pathogens (Spear et al , 2012; Askarian et al , 2014; Zou et al , 2014) highlights the importance of this immune evasion strategy in disease.…”

Section: Introductionmentioning

confidence: 99%

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A Pseudomonas aeruginosa TIR effector mediates immune evasion by targeting UBAP1 and TLR adaptors

et al. 2017

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Bacterial pathogens often subvert the innate immune system to establish a successful infection. The direct inhibition of downstream components of innate immune pathways is particularly well documented but how bacteria interfere with receptor proximal events is far less well understood. Here, we describe a Toll/interleukin 1 receptor (TIR) domain‐containing protein (PumA) of the multi‐drug resistant Pseudomonas aeruginosa PA7 strain. We found that PumA is essential for virulence and inhibits NF‐κB, a property transferable to non‐PumA strain PA14, suggesting no additional factors are needed for PumA function. The TIR domain is able to interact with the Toll‐like receptor (TLR) adaptors TIRAP and MyD88, as well as the ubiquitin‐associated protein 1 (UBAP1), a component of the endosomal‐sorting complex required for transport I (ESCRT‐I). These interactions are not spatially exclusive as we show UBAP1 can associate with MyD88, enhancing its plasma membrane localization. Combined targeting of UBAP1 and TLR adaptors by PumA impedes both cytokine and TLR receptor signalling, highlighting a novel strategy for innate immune evasion.

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