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1. C. difficile intoxicates neurons and pericytes to drive neurogenic inflammation.

Author

Manion, John, Musser, Melissa, Kuziel, Gavin, Liu, Min, Shepherd, Amy, Wang, Siyu, Lee, Pyung-Gang, Zhao, Leo, Zhang, Jie, Marreddy, Ravi, Goldsmith, Jeffrey, Yuan, Ke, Hurdle, Julian, Gerhard, Ralf, Jin, Rongsheng, Rakoff-Nahoum, Seth, Rao, Meenakshi, and Dong, Min

Subjects
Animals, Mice, Bacterial Toxins, Calcitonin Gene-Related Peptide, Clostridioides difficile, Clostridium Infections, Neurogenic Inflammation, Pericytes, Receptors, Neurokinin-1, Substance P, Neurons, Afferent, Inflammation Mediators, Cecum, Signal Transduction
Abstract

Clostridioides difficile infection (CDI) is a major cause of healthcare-associated gastrointestinal infections1,2. The exaggerated colonic inflammation caused by C. difficile toxins such as toxin B (TcdB) damages tissues and promotes C. difficile colonization3-6, but how TcdB causes inflammation is unclear. Here we report that TcdB induces neurogenic inflammation by targeting gut-innervating afferent neurons and pericytes through receptors, including the Frizzled receptors (FZD1, FZD2 and FZD7) in neurons and chondroitin sulfate proteoglycan 4 (CSPG4) in pericytes. TcdB stimulates the secretion of the neuropeptides substance P (SP) and calcitonin gene-related peptide (CGRP) from neurons and pro-inflammatory cytokines from pericytes. Targeted delivery of the TcdB enzymatic domain, through fusion with a detoxified diphtheria toxin, into peptidergic sensory neurons that express exogeneous diphtheria toxin receptor (an approach we term toxogenetics) is sufficient to induce neurogenic inflammation and recapitulates major colonic histopathology associated with CDI. Conversely, mice lacking SP, CGRP or the SP receptor (neurokinin 1 receptor) show reduced pathology in both models of caecal TcdB injection and CDI. Blocking SP or CGRP signalling reduces tissue damage and C. difficile burden in mice infected with a standard C. difficile strain or with hypervirulent strains expressing the TcdB2 variant. Thus, targeting neurogenic inflammation provides a host-oriented therapeutic approach for treating CDI.

Published
2023

3. Identification of TFPI as a receptor reveals recombination-driven receptor switching in Clostridioides difficile toxin B variants

Author

Tian, Songhai, Xiong, Xiaozhe, Zeng, Ji, Wang, Siyu, Tremblay, Benjamin Jean-Marie, Chen, Peng, Chen, Baohua, Liu, Min, Chen, Pengsheng, Sheng, Kuanwei, Zeve, Daniel, Qi, Wanshu, Breault, David T, Rodríguez, César, Gerhard, Ralf, Jin, Rongsheng, Doxey, Andrew C, and Dong, Min

Subjects
Biological Sciences, Biomedical and Clinical Sciences, Clinical Sciences, Biodefense, Vaccine Related, Digestive Diseases, Infectious Diseases, Emerging Infectious Diseases, Prevention, Aetiology, 2.1 Biological and endogenous factors, Infection, Animals, Cattle, Dogs, Mice, Bacterial Proteins, Bacterial Toxins, Clostridioides difficile, Recombination, Genetic, Humans
Abstract

Toxin B (TcdB) is a major exotoxin responsible for diseases associated with Clostridioides difficile infection. Its sequence variations among clinical isolates may contribute to the difficulty in developing effective therapeutics. Here, we investigate receptor-binding specificity of major TcdB subtypes (TcdB1 to TcdB12). We find that representative members of subtypes 2, 4, 7, 10, 11, and 12 do not recognize the established host receptor, frizzled proteins (FZDs). Using a genome-wide CRISPR-Cas9-mediated screen, we identify tissue factor pathway inhibitor (TFPI) as a host receptor for TcdB4. TFPI is recognized by a region in TcdB4 that is homologous to the FZD-binding site in TcdB1. Analysis of 206 TcdB variant sequences reveals a set of six residues within this receptor-binding site that defines a TFPI binding-associated haplotype (designated B4/B7) that is present in all TcdB4 members, a subset of TcdB7, and one member of TcdB2. Intragenic micro-recombination (IR) events have occurred around this receptor-binding region in TcdB7 and TcdB2 members, resulting in either TFPI- or FZD-binding capabilities. Introduction of B4/B7-haplotype residues into TcdB1 enables dual recognition of TFPI and FZDs. Finally, TcdB10 also recognizes TFPI, although it does not belong to the B4/B7 haplotype, and shows species selectivity: it recognizes TFPI of chicken and to a lesser degree mouse, but not human, dog, or cattle versions. These findings identify TFPI as a TcdB receptor and reveal IR-driven changes on receptor-specificity among TcdB variants.

Published
2022

4. Structural basis for CSPG4 as a receptor for TcdB and a therapeutic target in Clostridioides difficile infection.

Author

Chen, Peng, Zeng, Ji, Liu, Zheng, Thaker, Hatim, Wang, Siyu, Tian, Songhai, Zhang, Jie, Tao, Liang, Gutierrez, Craig B, Xing, Li, Gerhard, Ralf, Huang, Lan, Dong, Min, and Jin, Rongsheng

Subjects
Animals, Mice, Inbred C57BL, Mice, Knockout, Mice, Enterocolitis, Pseudomembranous, Multiprotein Complexes, Proteoglycans, Bacterial Proteins, Bacterial Toxins, Antibodies, Monoclonal, Antigens, Cryoelectron Microscopy, Binding Sites, Protein Conformation, Protein Binding, Broadly Neutralizing Antibodies, Clostridioides difficile, Infectious Diseases, Emerging Infectious Diseases, Digestive Diseases, 2.1 Biological and endogenous factors, 5.1 Pharmaceuticals, Infection
Abstract

C. difficile is a major cause of antibiotic-associated gastrointestinal infections. Two C. difficile exotoxins (TcdA and TcdB) are major virulence factors associated with these infections, and chondroitin sulfate proteoglycan 4 (CSPG4) is a potential receptor for TcdB, but its pathophysiological relevance and the molecular details that govern recognition remain unknown. Here, we determine the cryo-EM structure of a TcdB-CSPG4 complex, revealing a unique binding site spatially composed of multiple discontinuous regions across TcdB. Mutations that selectively disrupt CSPG4 binding reduce TcdB toxicity in mice, while CSPG4-knockout mice show reduced damage to colonic tissues during C. difficile infections. We further show that bezlotoxumab, the only FDA approved anti-TcdB antibody, blocks CSPG4 binding via an allosteric mechanism, but it displays low neutralizing potency on many TcdB variants from epidemic hypervirulent strains due to sequence variations in its epitopes. In contrast, a CSPG4-mimicking decoy neutralizes major TcdB variants, suggesting a strategy to develop broad-spectrum therapeutics against TcdB.

Published
2021

5. Cytosolic sodium accumulation is a cellular danger signal triggering endocytic dysfunction and NLRP3 inflammasome activation

Author

Mangan, Matthew S.J., primary, Akbal, Anil, additional, Rivara, Sophie, additional, Horvath, Gabor L., additional, Walch, Philipp, additional, Hegermann, Jan, additional, Kaiser, Romina, additional, Duthie, Fraser, additional, Selkrig, Joel, additional, Gerhard, Ralf, additional, Wachten, Dagmar, additional, and Latz, Eicke, additional

Published
2024
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8. Receptors and Binding Structures for Clostridium difficile Toxins A and B

Author

Gerhard, Ralf, Compans, Richard W, Series editor, Honjo, Tasuku, Series editor, Malissen, Bernard, Series editor, Aktories, Klaus, Series editor, Rappuoli, Rino, Series editor, Galan, Jorge E., Series editor, Ahmed, Rafi, Series editor, Palme, Klaus, Series editor, Casadevall, Arturo, Series editor, Garcia-Sastre, Adolfo, Series editor, and Barth, Holger, editor

Published
2017
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12. Transcriptional licensing is required for Pyrin inflammasome activation in human macrophages and bypassed by mutations causing familial Mediterranean fever

Author

Mangan, Matthew S. J., primary, Gorki, Friederike, additional, Krause, Karoline, additional, Heinz, Alexander, additional, Pankow, Anne, additional, Ebert, Thomas, additional, Jahn, Dieter, additional, Hiller, Karsten, additional, Hornung, Veit, additional, Maurer, Marcus, additional, Schmidt, Florian I., additional, Gerhard, Ralf, additional, and Latz, Eicke, additional

Published
2022
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20. Clostridium difficile Toxin B activates the NLRP3 inflammasome in human macrophages, demonstrating a novel regulatory mechanism for the Pyrin inflammasome

Author

Mangan, Matthew S.J., primary, Gorki, Friederike, additional, Krause, Karoline, additional, Heinz, Alexander, additional, Ebert, Thomas, additional, Jahn, Dieter, additional, Hiller, Karsten, additional, Hornung, Veit, additional, Mauer, Marcus, additional, Schmidt, Florian I., additional, Gerhard, Ralf, additional, and Latz, Eicke, additional

Published
2021
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23. C.difficileintoxicates neurons and pericytes to drive neurogenic inflammation

Author

Manion, John, Musser, Melissa A., Kuziel, Gavin A., Liu, Min, Shepherd, Amy, Wang, Siyu, Lee, Pyung-Gang, Zhao, Leo, Zhang, Jie, Marreddy, Ravi K. R., Goldsmith, Jeffrey D., Yuan, Ke, Hurdle, Julian G., Gerhard, Ralf, Jin, Rongsheng, Rakoff-Nahoum, Seth, Rao, Meenakshi, and Dong, Min

Abstract

Clostridioides difficileinfection (CDI) is a major cause of healthcare-associated gastrointestinal infections1,2. The exaggerated colonic inflammation caused by C.difficiletoxins such as toxin B (TcdB) damages tissues and promotes C.difficilecolonization3–6, but how TcdB causes inflammation is unclear. Here we report that TcdB induces neurogenic inflammation by targeting gut-innervating afferent neurons and pericytes through receptors, including the Frizzled receptors (FZD1, FZD2 and FZD7) in neurons and chondroitin sulfate proteoglycan 4 (CSPG4) in pericytes. TcdB stimulates the secretion of the neuropeptides substance P (SP) and calcitonin gene-related peptide (CGRP) from neurons and pro-inflammatory cytokines from pericytes. Targeted delivery of the TcdB enzymatic domain, through fusion with a detoxified diphtheria toxin, into peptidergic sensory neurons that express exogeneous diphtheria toxin receptor (an approach we term toxogenetics) is sufficient to induce neurogenic inflammation and recapitulates major colonic histopathology associated with CDI. Conversely, mice lacking SP, CGRP or the SP receptor (neurokinin 1 receptor) show reduced pathology in both models of caecal TcdB injection and CDI. Blocking SP or CGRP signalling reduces tissue damage and C.difficileburden in mice infected with a standard C.difficilestrain or with hypervirulent strains expressing the TcdB2 variant. Thus, targeting neurogenic inflammation provides a host-oriented therapeutic approach for treating CDI.

Published
2023
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25. Upregulation of the immediate early gene product RhoB by exoenzyme C3 from Clostridium limosum and Toxin B from Clostridium difficile

Author

Huelsenbeck, ohannes, Dreger, Stefanie C., Gerhard, Ralf, Fritz, Gerhard, Just, Ingo, and Genth, Harald

Subjects
Clostridium difficile -- Chemical properties, Clostridium difficile -- Structure, Cytoskeleton -- Chemical properties, Cytoskeleton -- Structure, Thioredoxin -- Chemical properties, Thioredoxin -- Structure, Biological sciences, Chemistry
Abstract

A study conducted provides evidence that the upregulation of RhoB is based on the inactivation of either Rho(A,B,C) or (H-,K-,N-)Ras but neither on the reorganization of the actin cytoskeleton nor the inactivation of Rac1.

Published
2007

31. Impairment of lysosomal function by Clostridioides difficile TcdB.

Author

Klepka, Carmen, Sandmann, Moritz, Tatge, Helma, Mangan, Matthew, Arens, Annabel, Henkel, Daniel, and Gerhard, Ralf

Subjects
LYSOSOMES, CLOSTRIDIOIDES difficile, RHO GTPases, CALCIUM antagonists, DETECTION limit, GALECTINS
Abstract

TcdB is a potent cytotoxin produced by pathogenic Clostridioides difficile that inhibits Rho GTPases by mono-glucosylation. TcdB enters cells via receptor-mediated endocytosis. The pathogenic glucosyltransferase domain (GTD) egresses endosomes by pH-mediated conformational changes, and is subsequently released in an autoproteolytic manner. We here investigated the uptake, localization and degradation of TcdB. TcdB colocalized with lysosomal marker protein LAMP1, verifying the endosomallysosomal route of the toxin. In pulse assays endocytosed TcdB declined to a limit of detection within 2 hr, whereas the released GTD accumulated for up to 8 hr. We observed that autoproteolytic deficient TcdB NXN C698S was degraded significantly faster than wildtype TcdB, suggesting interference of TcdB with lysosomal degradation process. In fact, TcdB reduced lysosomal degradation of endosome cargo as tested with DQ-Green BSA. Lysosomal dysfunction was accompanied by perinuclear accumulation of LAMP1 and a weaker detection in immunoblots. Galectin-8 or galectin-3 was not recruited to lysosomes speaking against lysosome membrane damage. Changes in the autophagosomal marker LC3B suggested additional indirect effect of lysosomal dysfunction on the autophagic flux. In contrast to necrotic signaling induced in by TcdB, lysosomal dysfunction was not abolished by calcium channel blocker nifedipin, indicating separate cytopathogenic effects induced by TcdB during endo-lysosomal trafficking. [ABSTRACT FROM AUTHOR]

Published
2022
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37. Evidence for an adaptation of a phage-derived holin/endolysin system to toxin transport in Clostridioides difficile

Author

Mehner-Breitfeld, Denise, Rathmann, Claudia, Riedel, Thomas, Just, Ingo, Gerhard, Ralf, Overmann, Jörg, and Brüser, Thomas

Subjects
Holins, Dewey Decimal Classification::500 | Naturwissenschaften::570 | Biowissenschaften, Biologie, Protein transport, Clostridioides difficile, ddc:570, Endolysins, Toxins
Abstract

The pathogenicity locus (PaLoc) of Clostridioides difficile usually comprises five genes (tcdR, tcdB, tcdE, tcdA, tcdC). While the proteins TcdA and TcdB represent the main toxins of this pathogen, TcdR and TcdC are involved in the regulation of their production. TcdE is a holin family protein, members of which are usually involved in the transport of cell wall-degrading enzymes (endolysins) for phage-induced lysis. In the past, TcdE has been shown to contribute to the release of TcdA and TcdB, but it is unclear whether it mediates a specific transport or rather a lysis of cells. TcdE of C. difficile strains analyzed so far can be produced in three isoforms that are initiated from distinct N-terminal ATG codons. When produced in Escherichia coli, we found that the longest TcdE isoform had a moderate effect on cell growth, whereas the shortest isoform strongly induced lysis. The effect of the longest isoform was inhibitory for cell lysis, implying a regulatory function of the N-terminal 24 residues. We analyzed the PaLoc sequence of 44 C. difficile isolates and found that four of these apparently encode only the short TcdE isoforms, and the most closely related holins from C. difficile phages only possess one of these initiation codons, indicating that an N-terminal extension of TcdE evolved in C. difficile. All PaLoc sequences comprised also a conserved gene encoding a short fragment of an endolysin remnant of a phage holin/endolysin pair. We could produce this peptide, which we named TcdL, and demonstrated by bacterial two-hybrid analysis a self-interaction and an interaction with TcdB that might serve to mediate TcdE-dependent transport.

Published
2018

38. Impact of clostridial glucosylating toxins on the proteome of colonic cells determined by isotope-coded protein labeling and LC-MALDI

Author

Just Ingo, Gerhard Ralf, Jochim Nelli, and Pich Andreas

Subjects
C. difficile-associated diarrhea, colonic cells, ICPL™, relative quantification, Toxin A, Cytology, QH573-671
Abstract

Abstract Background The anaerobe Clostridium difficile produces two major virulence factors toxin A and B that inactivate Rho proteins by glucosylation of a pivotal threonine residue. Purified toxins induce reorganization of the cytoskeleton and cell death in colonic cells. Whether all toxin effects on target cells depend on catalytic glucosyltransferase activity is unclear at present. Thus, we conducted a proteome approach to compare the protein profile of target cells treated either with wild type toxin A (rTcdA wt) or with a catalytically inactive mutant toxin A (mutant rTcdA). Relative protein quantification was feasible using isotope-coded protein labeling techniques (ICPL) and mass spectrometry (LC-MALDI). Results Altogether we found a significant differential expression of thirty proteins after treatment with rTcdA wt or mutant rTcdA. Mutant rTcdA caused up-regulation of seven proteins and sixteen proteins were responsive to rTcdA wt after 5 h. Long-term effect of rTcdA wt on protein expression was the down-regulation of eleven proteins. Up- or down-regulation of several proteins was verified by western blot analysis confirming the MS results. Conclusion Our results indicate incubation time-dependent effects of the clostridial glucosylating toxin A on colonic cells. The rTcdA wt impact more cellular functions than actin cytoskeleton reorganization and apoptosis. Furthermore, these data give insight into glucosyltransferase independent effects of clostridial glucosylating toxins on target cells after short incubation time. Additionally, our data reveal pro-inflammatory and proliferative effects of mutant rTcdA after short-term incubation.

Published
2011
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48. Killing of rat basophilic leukemia cells by lethal toxin from Clostridium sordellii: critical role of phosphatidylinositide 3'-OH kinase/Akt signaling

Author

Dreger, Stefanie C., Schulz, Florian, Huelsenbeck, Johannes, Gerhard, Ralf, Hofmann, Fred, Just, Ingo, and Genth, Harald

Subjects
Basophils -- Physiological aspects, Clostridium -- Physiological aspects, Clostridium -- Genetic aspects, Leukemia -- Research, Phosphotransferases -- Chemical properties, Rats -- Physiological aspects, Rattus -- Physiological aspects, Biological sciences, Chemistry
Abstract

Several studies are conducted to explain the factors that affect the cytotoxic effects of Clostridium sordellii lethal toxin (TcsL), which is usually used for the killing of rat basophilic leukemia cells. The cytotoxic effects of TcsL are shown to be highly influenced by Ras glucosylation and subsequent inhibition of phosphatidylinositide 3'-OH kinase (PI3K)/Akt signaling.

Published
2009

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