Your search keyword '"Guo, Cynthia X."' showing total 4 results

1. D-Glycero-β-D-Manno-Heptose 1-Phosphate and D-Glycerob- D-Manno-Heptose 1,7-Biphosphate Are Both Innate Immune Agonists.

Author

Adekoya, Itunuoluwa A., Guo, Cynthia X., Gray-Owen, Scott D., Cox, Andrew D., and Sauvageau, Janelle

Subjects

*IMMUNOLOGY, *EPITHELIAL cells, *CYTOKINES, *INFLAMMATION, *MASS spectrometry

Abstract

D-Glycero-β-D-manno-heptose 1,7-biphosphate (β-HBP) is a novel microbial-associated molecular pattern that triggers inflammation and thus has the potential to act as an immune modulator in many therapeutic contexts. To better understand the structure--activity relationship of this molecule, we chemically synthesized analogs of β-HBP and tested their ability to induce canonical TIFA-dependent inflammation in human embryonic kidney cells (HEK 293T) and colonic epithelial cells (HCT 116). Of the analogs tested, only D-glycero-b-D-manno-heptose 1-phosphate (β-HMP) induced TIFA-dependent NF-κB activation and cytokine production in a manner similar to β-HBP. This finding expands the spectrum of metabolites from the Gram-negative ADP--heptose biosynthesis pathway that can function as innate immune agonists and provides a more readily available agonist of the TIFA-dependent inflammatory pathway that can be easily produced by synthetic methods. [ABSTRACT FROM AUTHOR]

Published

2018

2. Bcl10 synergistically links CEACAM3 and TLR-dependent inflammatory signalling.

Author

Sintsova, Anna, Guo, Cynthia X., Sarantis, Helen, Mak, Tak W., Glogauer, Michael, and Gray‐Owen, Scott D.

Subjects

*NEUTROPHILS, *NEISSERIA gonorrhoeae, *CARCINOEMBRYONIC antigen, *CELL adhesion molecules, *NF-kappa B

Abstract

The neutrophil-specific innate immune receptor CEACAM3 functions as a decoy to capture Gram-negative pathogens, such as Neisseria gonorrhoeae, that exploit CEACAM family members to adhere to the epithelium. Bacterial binding to CEACAM3 results in their efficient engulfment and triggers activation of an nuclear factor kappa-light-chain-enhancer of activated B cells (NF-κB)-dependent inflammatory response by human neutrophils. Herein, we report that CEACAM3 cross-linking is not sufficient for induction of cytokine production and show that the inflammatory response induced by Neisseria gonorrhoeae infection is elicited by an integration of signals from CEACAM3 and toll-like receptors. Using neutrophils from a human CEACAM-expressing mouse line (CEABAC), we use a genetic approach to reveal a molecular bifurcation of the CEACAM3-mediated antimicrobial and inflammatory responses. Ex vivo experiments with CEABAC- Rac2−/−, CEABAC- Bcl10−/−, and CEABAC- Malt1−/− neutrophils indicate that these effectors are not necessary for gonococcal engulfment, yet all 3 effectors contribute to CEACAM3-mediated cytokine production. Interestingly, although Bcl10 and Malt1 are often inextricably linked, Bcl10 enabled synergy between toll-like receptor 4 and CEACAM3, whereas Malt1 did not. Together, these findings reveal an integration of the specific innate immune receptor CEACAM3 into the network of more conventional pattern recognition receptors, providing a mechanism by which the innate immune system can unleash its response to a relentless pathogen. [ABSTRACT FROM AUTHOR]

Published

2018

3. Innate Recognition of Intracellular Bacterial Growth Is Driven by the TIFA-Dependent Cytosolic Surveillance Pathway.

Author

Gaudet, Ryan G., Guo, Cynthia X., Molinaro, Raphael, Kottwitz, Haila, Rohde, John R., Dangeard, Anne-Sophie, Arrieumerlou, Cécile, Girardin, Stephen E., and Gray-Owen, Scott D.

Abstract

Summary Intestinal epithelial cells (IECs) act as sentinels for incoming pathogens. Cytosol-invasive bacteria, such as Shigella flexneri , trigger a robust pro-inflammatory nuclear factor κB (NF-κB) response from IECs that is believed to depend entirely on the peptidoglycan sensor NOD1. We found that, during Shigella infection, the TRAF-interacting forkhead-associated protein A (TIFA)-dependent cytosolic surveillance pathway, which senses the bacterial metabolite heptose-1,7-bisphosphate (HBP), functions after NOD1 to detect bacteria replicating free in the host cytosol. Whereas NOD1 mediated a transient burst of NF-κB activation during bacterial entry, TIFA sensed HBP released during bacterial replication, assembling into large signaling complexes to drive a dynamic inflammatory response that reflected the rate of intracellular bacterial proliferation. Strikingly, IECs lacking TIFA were unable to discriminate between proliferating and stagnant intracellular bacteria, despite the NOD1/2 pathways being intact. Our results define TIFA as a rheostat for intracellular bacterial replication, escalating the immune response to invasive Gram-negative bacteria that exploit the host cytosol for growth. [ABSTRACT FROM AUTHOR]

Published

2017

4. Alternate synthesis to d-glycero-β-d-manno-heptose 1,7-biphosphate.

Author

Sauvageau, Janelle, Bhasin, Milan, Guo, Cynthia X., Adekoya, Itunuoluwa A., Gray-Owen, Scott D., Oscarson, Stefan, Guazzelli, Lorenzo, and Cox, Andrew

Subjects

*GLYCERIN, *MANNOSE, *PHOSPHATES, *CHEMICAL synthesis, *LIPOPOLYSACCHARIDES, *MAMMAL diseases, *GRAM-negative bacterial diseases

Abstract

d -glycero-β- d -manno-heptose 1,7-biphosphate (HBP) is an enzymatic intermediate in the biosynthesis of the heptose component of lipopolysaccharide (LPS), and was recently revealed to be a pathogen-associated molecular pattern (PAMP) that allows detection of Gram-negative bacteria by the mammalian immune system. Cellular detection of HBP depends upon its stimulation of a cascade that leads to the phosphorylation and assembly of the TRAF-interacting with forkhead-associated domain protein A (TIFA), which activates the transcription factor NF-κB. In this note, an alternate chemical synthesis of HBP is described and its biological activity is established, providing pure material for further assessing and exploiting the biological activity of this compound. [ABSTRACT FROM AUTHOR]

Published

2017