Your search keyword '"Ralf Gerhard"' showing total 156 results

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

Author

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

Subjects

Science

Abstract

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

2. A Colonic Organoid Model Challenged with the Large Toxins of Clostridioides difficile TcdA and TcdB Exhibit Deregulated Tight Junction Proteins

Author

Martina Schneemann, Lucas Heils, Verena Moos, Franziska Weiß, Susanne M. Krug, January Weiner, Dieter Beule, Ralf Gerhard, Jörg-Dieter Schulzke, and Roland Bücker

Subjects

intestinal epithelial human colonic organoid monolayer, claudin, leak flux diarrhea, leaky gut, super-resolution STED microscopy, tricellulin, Medicine

Abstract

Background: Clostridioides difficile toxins TcdA and TcdB are responsible for diarrhea and colitis. Lack of functional studies in organoid models of the gut prompted us to elucidate the toxin’s effects on epithelial barrier function and the molecular mechanisms for diarrhea and inflammation. Methods: Human adult colon organoids were cultured on membrane inserts. Tight junction (TJ) proteins and actin cytoskeleton were analyzed for expression via Western blotting and via confocal laser-scanning microscopy for subcellular localization. Results: Polarized intestinal organoid monolayers were established from stem cell-containing colon organoids to apply toxins from the apical side and to perform functional measurements in the organoid model. The toxins caused a reduction in transepithelial electrical resistance in human colonic organoid monolayers with sublethal concentrations. Concomitantly, we detected increased paracellular permeability fluorescein and FITC-dextran-4000. Human colonic organoid monolayers exposed to the toxins exhibited redistribution of barrier-forming TJ proteins claudin-1, -4 and tricellulin, whereas channel-forming claudin-2 expression was increased. Perijunctional F-actin cytoskeleton organization was affected. Conclusions: Adult stem cell-derived human colonic organoid monolayers were applicable as a colon infection model for electrophysiological measurements. The TJ changes noted can explain the epithelial barrier dysfunction and diarrhea in patients, as well as increased entry of luminal antigens triggering inflammation.

Published

2023

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

Author

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

Subjects

Biology (General), QH301-705.5

Abstract

Pyrin is a cytosolic immune sensor that nucleates an inflammasome in response to inhibition of RhoA by bacterial virulence factors, triggering the release of inflammatory cytokines, including IL-1β. Gain-of-function mutations in the MEFV gene encoding Pyrin cause autoinflammatory disorders, such as familial Mediterranean fever (FMF) and Pyrin-associated autoinflammation with neutrophilic dermatosis (PAAND). To precisely define the role of Pyrin in pathogen detection in human immune cells, we compared initiation and regulation of the Pyrin inflammasome response in monocyte-derived macrophages (hMDM). Unlike human monocytes and murine macrophages, we determined that hMDM failed to activate Pyrin in response to known Pyrin activators Clostridioides difficile (C. difficile) toxins A or B (TcdA or TcdB), as well as the bile acid analogue BAA-473. The Pyrin inflammasome response was enabled in hMDM by prolonged priming with either LPS or type I or II interferons and required an increase in Pyrin expression. Notably, FMF mutations lifted the requirement for prolonged priming for Pyrin activation in hMDM, enabling Pyrin activation in the absence of additional inflammatory signals. Unexpectedly, in the absence of a Pyrin response, we found that TcdB activated the NLRP3 inflammasome in hMDM. These data demonstrate that regulation of Pyrin activation in hMDM diverges from monocytes and highlights its dysregulation in FMF.

Published

2022

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

Author

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

Subjects

Science

Abstract

Chondroitin sulfate proteoglycan 4 (CSPG4) is a potential receptor for C. difficile toxin B (TcdB) during C. difficile infections (CDIs). Here, the cryo-EM structure of a TcdB–CSPG4 complex and CDI mouse models offer insights into CSPG4 role in CDIs and suggest a therapeutic strategy targeting TcdB.

Published

2021

5. CDT of Clostridioides difficile Induces MLC-Dependent Intestinal Barrier Dysfunction in HT-29/B6 Epithelial Cell Monolayers

Author

Lucas Heils, Martina Schneemann, Ralf Gerhard, Jörg-Dieter Schulzke, and Roland Bücker

Subjects

binary toxin, tight junction, barrier function, claudin, tricellulin, occludin, Medicine

Abstract

Background: Clostridioides difficile binary toxin (CDT) defines the hypervirulence of strains in nosocomial antibiotic-induced colitis with the highest mortality. The objective of our study was to investigate the impact of CDT on the intestinal epithelial barrier and to enlighten the underlying molecular mechanisms. Methods: Functional measurements of epithelial barrier function by macromolecular permeability and electrophysiology were performed in human intestinal HT-29/B6 cell monolayers. Molecular analysis of the spatial distribution of tight junction protein and cytoskeleton was performed by super-resolution STED microscopy. Results: Sublethal concentrations of CDT-induced barrier dysfunction with decreased TER and increased permeability for 332 Da fluorescein and 4 kDa FITC-dextran. The molecular correlate to the functional barrier defect by CDT was found to be a tight junction protein subcellular redistribution with tricellulin, occludin, and claudin-4 off the tight junction domain. This redistribution was shown to be MLCK-dependent. Conclusions: CDT compromised epithelial barrier function in a human intestinal colonic cell model, even in sublethal concentrations, pointing to barrier dysfunction in the intestine and leak flux induction as a diarrheal mechanism. However, this cannot be attributed to the appearance of apoptosis and necrosis, but rather to an opening of the paracellular leak pathway as the result of epithelial tight junction alterations.

Published

2023

6. Clostridioides difficile Toxin CDT Induces Cytotoxic Responses in Human Mucosal-Associated Invariant T (MAIT) Cells

Author

Isabel Marquardt, Josefine Jakob, Jessica Scheibel, Julia Danielle Hofmann, Frank Klawonn, Meina Neumann-Schaal, Ralf Gerhard, Dunja Bruder, and Lothar Jänsch

Subjects

MAIT cells, C. difficile, TcdA, TcdB, CDT, CDAC, Microbiology, QR1-502

Abstract

Clostridioides difficile is the major cause of antibiotic-associated colitis (CDAC) with increasing prevalence in morbidity and mortality. Severity of CDAC has been attributed to hypervirulent C. difficile strains, which in addition to toxin A and B (TcdA, TcdB) produce the binary toxin C. difficile transferase (CDT). However, the link between these toxins and host immune responses as potential drivers of immunopathology are still incompletely understood. Here, we provide first experimental evidence that C. difficile toxins efficiently activate human mucosal-associated invariant T (MAIT) cells. Among the tested toxins, CDT and more specifically, the substrate binding and pore-forming subunit CDTb provoked significant MAIT cell activation resulting in selective MAIT cell degranulation of the lytic granule components perforin and granzyme B. CDT-induced MAIT cell responses required accessory immune cells, and we suggest monocytes as a potential CDT target cell population. Within the peripheral blood mononuclear cell fraction, we found increased IL-18 levels following CDT stimulation and MAIT cell response was indeed partly dependent on this cytokine. Surprisingly, CDT-induced MAIT cell activation was found to be partially MR1-dependent, although bacterial-derived metabolite antigens were absent. However, the role of antigen presentation in this process was not analyzed here and needs to be validated in future studies. Thus, MR1-dependent induction of MAIT cell cytotoxicity might be instrumental for hypervirulent C. difficile to overcome cellular barriers and may contribute to pathophysiology of CDAC.

Published

2021

7. The Binary Toxin of Clostridioides difficile Alters the Proteome and Phosphoproteome of HEp-2 Cells

Author

Florian Stieglitz, Ralf Gerhard, and Andreas Pich

Subjects

binary toxin, Clostridioides difficile, proteome, phosphoproteome, signaling, Microbiology, QR1-502

Abstract

Clostridioides difficile is a major cause of nosocomial infection worldwide causing antibiotic-associated diarrhea and some cases are leading to pseudomembranous colitis. The main virulence factors are toxin A and toxin B. Hypervirulent strains of C. difficile are linked to higher mortality rates and most of these strains produce additionally the C. difficile binary toxin (CDT) that possesses two subunits, CDTa and CDTb. The latter is responsible for binding and transfer of CDTa into the cytoplasm of target cells; CDTa is an ADP ribosyltransferase catalyzing the modification of actin fibers that disturbs the actin vs microtubule balance and induces microtubule-based protrusions of the cell membrane increasing the adherence of C. difficile. The underlying mechanisms remain elusive. Thus, we performed a screening experiment using MS-based proteomics and phosphoproteomics techniques. Epithelial Hep-2 cells were treated with CDTa and CDTb in a multiplexed study for 4 and 8 h. Phosphopeptide enrichment was performed using affinity chromatography with TiO2 and Fe-NTA; for quantification, a TMT-based approach and DDA measurements were used. More than 4,300 proteins and 5,600 phosphosites were identified and quantified at all time points. Although only moderate changes were observed on proteome level, the phosphorylation level of nearly 1,100 phosphosites responded to toxin treatment. The data suggested that CSNK2A1 might act as an effector kinase after treatment with CDT. Additionally, we confirmed ADP-ribosylation on Arg-177 of actin and the kinetic of this modification for the first time.

Published

2021

8. Receptor Binding Domains of TcdB from Clostridioides difficile for Chondroitin Sulfate Proteoglycan-4 and Frizzled Proteins Are Functionally Independent and Additive

Author

Daniel Henkel, Helma Tatge, Dennis Schöttelndreier, Liang Tao, Min Dong, and Ralf Gerhard

Subjects

Clostridioides difficile, glucosyltransferase, receptor binding, Medicine

Abstract

Toxin B (TcdB) produced by Clostridioides difficile is a main pathogenicity factor that affects a variety of different cell types within the colonic mucosa. TcdB is known to utilize frizzled-1,2,7 and chondroitin sulfate proteoglycan-4 (CSPG4) as protein receptors. By using human cervical cancer cell line HeLa CSPG4 knockout (CSPG4−/−) cells as well as TcdB mutants which do not bind to either CSPG4 or frizzled-1,2,7, or both, we evaluated the impact of the individual receptors for cytopathic and cytotoxic effects of TcdB. We compared TcdB from the reference strain VPI10463 (TcdBVPI) and the endemic strain R20291 (TcdBR20) which does not interact with frizzled-1,2,7. TcdBVPI devoid of CSPG4 binding (TcdBVPI ΔCROP) shows identical cytopathic potency as full-length TcdB in HeLa CSPG4−/− cells, indicating that interaction with frizzled proteins is not affected in the presence of the C-terminal CROP domain. We validated CSPG4 as cellular receptor for both TcdB toxinotypes in HeLa and HEp-2 cells. By exchange of a single phenylalanine residue, 1597 with serine, we generated a mutated TcdBVPI variant (TcdBVPI F1597S) that in accordance with TcdBR20 lacks binding to frizzled-1,2,7 and showed identical potency as TcdBR20 on HeLa cells. This enabled us to estimate the respective share of CSPG4 and frizzled-1,2,7 in the cytotoxic and cytopathic effect induced by TcdB. Our data reveal that binding to frizzled-1,2,7 and to CSPG4 occurs independently and in an additive manner.

Published

2020

9. Development of Neutralizing and Non-neutralizing Antibodies Targeting Known and Novel Epitopes of TcdB of Clostridioides difficile

Author

Viola Fühner, Philip Alexander Heine, Saskia Helmsing, Sebastian Goy, Jasmin Heidepriem, Felix F. Loeffler, Stefan Dübel, Ralf Gerhard, and Michael Hust

Subjects

Toxin B (TcdB), Clostridioides difficile, antibody phage display, recombinant antibody, epitope mapping, neutralization, Microbiology, QR1-502

Abstract

Clostridioides difficile is the causative bacterium in 15–20% of all antibiotic associated diarrheas. The symptoms associated with C. difficile infection (CDI) are primarily induced by the two large exotoxins TcdA and TcdB. Both toxins enter target cells by receptor-mediated endocytosis. Although different toxin receptors have been identified, it is no valid therapeutic option to prevent receptor endocytosis. Therapeutics, such as neutralizing antibodies, directly targeting both toxins are in development. Interestingly, only the anti-TcdB antibody bezlotoxumab but not the anti-TcdA antibody actoxumab prevented recurrence of CDI in clinical trials. In this work, 31 human antibody fragments against TcdB were selected by antibody phage display from the human naive antibody gene libraries HAL9/10. These antibody fragments were further characterized by in vitro neutralization assays. The epitopes of the neutralizing and non-neutralizing antibody fragments were analyzed by domain mapping, TcdB fragment phage display, and peptide arrays, to identify neutralizing and non-neutralizing epitopes. A new neutralizing epitope within the glucosyltransferase domain of TcdB was identified, providing new insights into the relevance of different toxin regions in respect of neutralization and toxicity.

Published

2018

10. Quantitative Phosphoproteome Analysis of Clostridioides difficile Toxin B Treated Human Epithelial Cells

Author

Johannes Junemann, Ingo Just, Ralf Gerhard, and Andreas Pich

Subjects

Clostridioides difficile, phosphoproteome, shotgun proteomics, small GTPases, TcdB, Microbiology, QR1-502

Abstract

The large clostridial glucosylating toxin B (TcdB) is a major virulence factor of the nosocomial pathogen Clostridioides difficile. TcdB inhibits small GTPases by glucosylation leading to impaired downstream signaling. TcdB also possesses a glucosyltransferase independent effect described as pyknosis. To elucidate the impact of TcdB and its glucosylation-inactive mutant TcdBNXN on the kinome of human cells, SILAC labeled HEp-2 cells were treated with 2 nM TcdB for 8 h. Phosphopeptides were enriched using SCX chromatography, IMAC and TiO2 followed shotgun mass spectrometry analysis. Overall 4,197 phosphopeptides were identified; more than 1,200 phosphosites responded to treatment with TcdB or TcdBNXN. The data suggested that predominantly stress-activated MAPK-dependent signaling pathways were triggered by toxin B treatment.

Published

2018

11. Difference in Mono-O-Glucosylation of Ras Subtype GTPases Between Toxin A and Toxin B From Clostridioides difficile Strain 10463 and Lethal Toxin From Clostridium sordellii Strain 6018

Author

Harald Genth, Johannes Junemann, Chantal M. Lämmerhirt, Arlen-Celina Lücke, Ilona Schelle, Ingo Just, Ralf Gerhard, and Andreas Pich

Subjects

Rho, Ras, GTPase, large clostridial glucosylating toxins, MRM analysis, Microbiology, QR1-502

Abstract

Clostridioides difficile toxin A (TcdA) and Toxin B (TcdB) trigger inflammasome activation with caspase-1 activation in cultured cells, which in turn induce the release of IL-6, IFN-γ, and IL-8. Release of these proinflammatory responses is positively regulated by Ras-GTPases, which leads to the hypothesis that Ras glucosylation by glucosylating toxins results in (at least) reduced proinflammatory responses. Against this background, data on toxin-catalyzed Ras glucosylation are required to estimate of pro-inflammatory effect of the glucosylating toxins. In this study, a quantitative evaluation of the GTPase substrate profiles glucosylated in human colonic (Caco-2) cells treated with either TcdA, TcdB, or the related Clostridium sordellii lethal toxin (TcsL) was performed using multiple reaction monitoring (MRM) mass spectrometry. (H/K/N)Ras are presented to be glucosylated by TcsL and TcdA but by neither TcdB isoform tested. Furthermore, the glucosylation of (H/K/N)Ras was detected in TcdA-(not TcdB)-treated cells, as analyzed exploiting immunoblot analysis using the Ras glucosylation-sensitive 27H5 antibody. Furthermore, [14C]glucosylation of substrate GTPase was found to be increased in a cell-free system complemented with Caco-2 lysates. Under these conditions, (H/K/N)Ras glucosylation by TcdA was detected. In contrast, TcdB-catalyzed (H/K/N)Ras glucosylation was detected by neither MRM analysis, immunoblot analysis nor [14C]glucosylation in a cell-free system. The observation that TcdA (not TcdB) glucosylates Ras subtype GTPases correlates with the fact that TcdB (not TcdA) is primarily responsible for inflammatory responses in CDI. Finally, TcsL more efficaciously glucosylated Ras subtype GTPase as compared with TcdA, reinforcing the paradigm that TcsL is the prototype of a Ras glucosylating toxin.

Published

2018

12. The Conserved Cys-2232 in Clostridioides difficile Toxin B Modulates Receptor Binding

Author

Soo-Young Chung, Dennis Schöttelndreier, Helma Tatge, Viola Fühner, Michael Hust, Lara-Antonia Beer, and Ralf Gerhard

Subjects

Clostridioides difficile, toxins, receptor binding, autoproteolysis, neutralization, antibody phage display, Microbiology, QR1-502

Abstract

Clostridioides difficile toxins TcdA and TcdB are large clostridial glucosyltransferases which are the main pathogenicity factors in C. difficile-associated diseases. Four highly conserved cysteines are present in all large clostridial glucosyltransferases. In this study we focused on the conserved cysteine 2232 within the combined repetitive oligopeptide domain of TcdB from reference strain VPI10463 (clade I). Cysteine 2232 is not present in TcdB from hypervirulent strain R20291 (clade II), where a tyrosine is found instead. Replacement of cysteine 2232 by tyrosine in TcdBV PI10463 reduced binding to the soluble fragments of the two known TcdB receptors, frizzled-2 (FZD2) and poliovirus receptor-like protein-3/nectin-3 (PVRL3). In line with this, TcdBR20291 showed weak binding to PVRL3 in pull-down assays which was increased when tyrosine 2232 was exchanged for cysteine. Surprisingly, we did not observe binding of TcdBR20291 to FZD2, indicating that this receptor is less important for this toxinotype. Competition assay with the receptor binding fragments (aa 1101–1836) of TcdBV PI10463 and TcdBR20291, as well as antibodies newly developed by antibody phage display, revealed different characteristics of the yet poorly described delivery domain of TcdB harboring the second receptor binding region. In summary, we found that conserved Cys-2232 in TcdB indirectly contributes to toxin–receptor interaction.

Published

2018

13. Evidence for an Adaptation of a Phage-Derived Holin/Endolysin System to Toxin Transport in Clostridioides difficile

Author

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

Subjects

Clostridioides difficile, toxins, holins, endolysins, protein transport, Microbiology, QR1-502

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

14. The Combined Repetitive Oligopeptides of Clostridium difficile Toxin A Counteract Premature Cleavage of the Glucosyl-Transferase Domain by Stabilizing Protein Conformation

Author

Alexandra Olling, Corinna Hüls, Sebastian Goy, Mirco Müller, Simon Krooss, Isa Rudolf, Helma Tatge, and Ralf Gerhard

Subjects

Clostridium difficile toxin, domain interaction, autoprocessing, cytotoxicity, microscale thermophoresis, Medicine

Abstract

Toxin A (TcdA) and B (TcdB) from Clostridium difficile enter host cells by receptor-mediated endocytosis. A prerequisite for proper toxin action is the intracellular release of the glucosyltransferase domain by an inherent cysteine protease, which is allosterically activated by inositol hexaphosphate (IP6). We found that in in vitro assays, the C-terminally-truncated TcdA1–1065 was more efficient at IP6-induced cleavage compared with full-length TcdA. We hypothesized that the C-terminally-located combined repetitive oligopeptides (CROPs) interact with the N-terminal part of the toxin, thereby preventing autoproteolysis. Glutathione-S-transferase (GST) pull-down assays and microscale thermophoresis confirmed binding between the CROPs and the glucosyltransferase (TcdA1–542) or intermediate (TcdA1102–1847) domain of TcdA, respectively. This interaction between the N- and C-terminus was not found for TcdB. Functional assays revealed that TcdB was more susceptible to inactivation by extracellular IP6-induced cleavage. In vitro autoprocessing and inactivation of TcdA, however, significantly increased, either by acidification of the surrounding milieu or following exchange of its CROP domain by the homologous CROP domain of TcdB. Thus, TcdA CROPs contribute to the stabilization and protection of toxin conformation in addition to function as the main receptor binding domain.

Published

2014

15. The Binary Toxin CDT of Clostridium difficile as a Tool for Intracellular Delivery of Bacterial Glucosyltransferase Domains

Author

Lara-Antonia Beer, Helma Tatge, Carmen Schneider, Maximilian Ruschig, Michael Hust, Jessica Barton, Stefan Thiemann, Viola Fühner, Giulio Russo, and Ralf Gerhard

Subjects

binary toxins, Clostridium difficile, ADP-ribosyltransferase, glucosyltransferase, protein delivery, Medicine

Abstract

Binary toxins are produced by several pathogenic bacteria. Examples are the C2 toxin from Clostridium botulinum, the iota toxin from Clostridium perfringens, and the CDT from Clostridium difficile. All these binary toxins have ADP-ribosyltransferases (ADPRT) as their enzymatically active component that modify monomeric actin in their target cells. The binary C2 toxin was intensively described as a tool for intracellular delivery of allogenic ADPRTs. Here, we firstly describe the binary toxin CDT from C. difficile as an effective tool for heterologous intracellular delivery. Even 60 kDa glucosyltransferase domains of large clostridial glucosyltransferases can be delivered into cells. The glucosyltransferase domains of five tested large clostridial glucosyltransferases were successfully introduced into cells as chimeric fusions to the CDTa adapter domain (CDTaN). Cell uptake was demonstrated by the analysis of cell morphology, cytoskeleton staining, and intracellular substrate glucosylation. The fusion toxins were functional only when the adapter domain of CDTa was N-terminally located, according to its native orientation. Thus, like other binary toxins, the CDTaN/b system can be used for standardized delivery systems not only for bacterial ADPRTs but also for a variety of bacterial glucosyltransferase domains.

Published

2018

16. Reactive Oxygen Species as Additional Determinants for Cytotoxicity of Clostridium difficile Toxins A and B

Author

Claudia Frädrich, Lara-Antonia Beer, and Ralf Gerhard

Subjects

Clostridium difficile infection, reactive oxygen species, cytotoxicity, NADPH oxidase, neutrophils, Rho GTPases, toxin, Medicine

Abstract

Clostridium difficile infections can induce mild to severe diarrhoea and the often associated characteristic pseudomembranous colitis. Two protein toxins, the large glucosyltransferases TcdA and TcdB, are the main pathogenicity factors that can induce all clinical symptoms in animal models. The classical molecular mode of action of these homologous toxins is the inhibition of Rho GTPases by mono-glucosylation. Rho-inhibition leads to breakdown of the actin cytoskeleton, induces stress-activated and pro-inflammatory signaling and eventually results in apoptosis of the affected cells. An increasing number of reports, however, have documented further qualities of TcdA and TcdB, including the production of reactive oxygen species (ROS) by target cells. This review summarizes observations dealing with the production of ROS induced by TcdA and TcdB, dissects pathways that contribute to this phenomenon and speculates about ROS in mediating pathogenesis. In conclusion, ROS have to be considered as a discrete, glucosyltransferase-independent quality of at least TcdB, triggered by different mechanisms.

Published

2016

17. Serine-71 phosphorylation of Rac1 modulates downstream signaling.

Author

Janett Schwarz, Julia Proff, Anika Hävemeier, Markus Ladwein, Klemens Rottner, Britta Barlag, Andreas Pich, Helma Tatge, Ingo Just, and Ralf Gerhard

Subjects

Medicine, Science

Abstract

The Rho GTPases Rac1 and Cdc42 regulate a variety of cellular functions by signaling to different signal pathways. It is believed that the presence of a specific effector at the location of GTPase activation determines the route of downstream signaling. We previously reported about EGF-induced Ser-71 phosphorylation of Rac1/Cdc42. By using the phosphomimetic S71E-mutants of Rac1 and Cdc42 we investigated the impact of Ser-71 phosphorylation on binding to selected effector proteins. Binding of the constitutively active (Q61L) variants of Rac1 and Cdc42 to their specific interaction partners Sra-1 and N-WASP, respectively, as well as to their common effector protein PAK was abrogated when Ser-71 was exchanged to glutamate as phosphomimetic substitution. Interaction with their common effector proteins IQGAP1/2/3 or MRCK alpha was, however, hardly affected. This ambivalent behaviour was obvious in functional assays. In contrast to Rac1 Q61L, phosphomimetic Rac1 Q61L/S71E was not able to induce increased membrane ruffling. Instead, Rac1 Q61L/S71E allowed filopodia formation, which is in accordance with abrogation of the dominant Sra-1/Wave signalling pathway. In addition, in contrast to Rac1 transfected cells Rac1 S71E failed to activate PAK1/2. On the other hand, Rac1 Q61L/S71E was as effective in activation of NF-kappaB as Rac1 Q61L, illustrating positive signal transduction of phosphorylated Rac1. Together, these data suggest that phosphorylation of Rac1 and Cdc42 at serine-71 represents a reversible mechanism to shift specificity of GTPase/effector coupling, and to preferentially address selected downstream pathways.

Published

2012

18. The repetitive oligopeptide sequences modulate cytopathic potency but are not crucial for cellular uptake of Clostridium difficile toxin A.

Author

Alexandra Olling, Sebastian Goy, Florian Hoffmann, Helma Tatge, Ingo Just, and Ralf Gerhard

Subjects

Medicine, Science

Abstract

The pathogenicity of Clostridium difficile is primarily linked to secretion of the intracellular acting toxins A (TcdA) and B (TcdB) which monoglucosylate and thereby inactivate Rho GTPases of host cells. Although the molecular mode of action of TcdA and TcdB is well understood, far less is known about toxin binding and uptake. It is acknowledged that the C-terminally combined repetitive oligopeptides (CROPs) of the toxins function as receptor binding domain. The current study evaluates the role of the CROP domain with respect to functionality of TcdA and TcdB. Therefore, we generated truncated TcdA devoid of the CROPs (TcdA(1-1874)) and found that this mutant was still cytopathic. However, TcdA(1-1874) possesses about 5 to 10-fold less potency towards 3T3 and HT29 cells compared to the full length toxin. Interestingly, CHO-C6 cells even showed almost identical susceptibility towards truncated and full length TcdA concerning Rac1 glucosylation or cell rounding, respectively. FACS and Western blot analyses elucidated these differences and revealed a correlation between CROP-binding to the cell surface and toxin potency. These findings refute the accepted opinion of solely CROP-mediated toxin internalization. Competition experiments demonstrated that presence neither of TcdA CROPs nor of full length TcdA reduced binding of truncated TcdA(1-1874) to HT29 cells. We assume that toxin uptake might additionally occur through alternative receptor structures and/or other associated endocytotic pathways. The second assumption was substantiated by TER measurements showing that basolaterally applied TcdA(1-1874) exhibits considerably higher cytotoxic potency than apically applied mutant or even full length TcdA, the latter being almost independent of the side of application. Thus, different routes for cellular uptake might enable the toxins to enter a broader repertoire of cell types leading to the observed multifarious pathogenesis of C. difficile.

Published

2011

19. Endovascular Therapy Versus Bypass Surgery as First-Line Treatment Strategies for Critical Limb Ischemia: Results of the Interim Analysis of the CRITISCH Registry

Author

Adili, Farzin, Balzer, Kai, Billing, Arend, Böckler, Dittmar, Brixner, Daniel, Debus, Sebastian E., Eckstein, Hans-Henning, Florek, Hans-Joachim, Gkremoutis, Asimakis, Grundmann, Reinhardt, Hupp, Thomas, Keck, Tobias, Gerß, Joachim, Klonek, Wojciech, Lang, Werner, May, Björn, Meyer, Alexander, Mühling, Bernhard, Oberhuber, Alexander, Reinecke, Holger, Reinhold, Christian, Ritter, Ralf-Gerhard, Schelzig, Hubert, Schlensack, Christian, Schmitz-Rixen, Thomas, Schulte, Karl-Ludwig, Spohn, Matthias, Steinbauer, Markus, Storck, Martin, Trede, Matthias, Uhl, Christian, Weis-Müller, Barbara, Wenk, Heiner, Zeller, Thomas, Zhorzel, Sven, Zimmermann, Alexander, Bisdas, Theodosios, Borowski, Matthias, Stavroulakis, Konstantinos, and Torsello, Giovanni

Published

2016

20. Kundenorientierte Produktentwicklung am Beispiel des Audi Q7

Author

Berger, Hans, Willner, Ralf-Gerhard, Einhorn, Martin, Albers, Sönke, editor, and Herrmann, Andreas, editor

Published

2007

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

Author

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

Subjects

0301 basic medicine, Bacterial toxins, Protein Conformation, General Physics and Astronomy, Inbred C57BL, Epitope, Mice, Monoclonal, 2.1 Biological and endogenous factors, Aetiology, Receptor, Enterocolitis, Pseudomembranous, Mice, Knockout, Multidisciplinary, biology, Pseudomembranous, Antibodies, Monoclonal, Infectious Diseases, 5.1 Pharmaceuticals, Proteoglycans, Development of treatments and therapeutic interventions, Antibody, Infection, Protein Binding, Knockout, Science, Bacterial Toxins, 030106 microbiology, Allosteric regulation, Virulence, Antibodies, Article, General Biochemistry, Genetics and Molecular Biology, 03 medical and health sciences, Bacterial Proteins, Animals, Antigens, Binding site, Binding Sites, Enterocolitis, Clostridioides difficile, Cryoelectron Microscopy, General Chemistry, Virology, Mice, Inbred C57BL, Emerging Infectious Diseases, 030104 developmental biology, Bezlotoxumab, CSPG4, Multiprotein Complexes, biology.protein, Digestive Diseases, Broadly Neutralizing Antibodies

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., Chondroitin sulfate proteoglycan 4 (CSPG4) is a potential receptor for C. difficile toxin B (TcdB) during C. difficile infections (CDIs). Here, the cryo-EM structure of a TcdB–CSPG4 complex and CDI mouse models offer insights into CSPG4 role in CDIs and suggest a therapeutic strategy targeting TcdB.

Published

2021

22. Association between statin therapy and amputation-free survival in patients with critical limb ischemia in the CRITISCH registry

Author

Stavroulakis, Konstantinos, Borowski, Matthias, Torsello, Giovanni, Bisdas, Theodosios, Adili, Farzin, Balzer, Kai, Billing, Arend, Böckler, Dittmar, Brixner, Daniel, Debus, Sebastian E., Eckstein, Hans-Henning, Florek, Hans-Joachim, Gkremoutis, Asimakis, Grundmann, Reinhardt, Hupp, Thomas, Keck, Tobias, Gerß, Joachim, Klonek, Wojciech, Lang, Werner, May, Björn, Meyer, Alexander, Mühling, Bernhard, Oberhuber, Alexander, Reinecke, Holger, Reinhold, Christian, Ritter, Ralf-Gerhard, Schelzig, Hubert, Schlensack, Christian, Schmitz-Rixen, Thomas, Schulte, Karl-Ludwig, Spohn, Matthias, Steinbauer, Markus, Storck, Martin, Trede, Matthias, Uhl, Christian, Weis-Müller, Barbara, Wenk, Heiner, Zeller, Thomas, Zhorzel, Sven, and Zimmermann, Alexander

Published

2017

23. Bypass Grafting vs Endovascular Therapy in Patients With Non-Dialysis-Dependent Chronic Kidney Disease and Chronic Limb-Threatening Ischemia (CRITISCH Registry)

Author

Konstantinos Stavroulakis, Asimakis Gkremoutis, Matthias Borowski, Giovanni Torsello, Dittmar Böckler, Thomas Zeller, Markus Steinbauer, Nikolaos Tsilimparis, Theodosios Bisdas, Farzin Adili, Kai Balzer, Arend Billing, Daniel Brixner, Sebastian E. Debus, Hans-Joachim Florek, Reinhardt Grundmann, Thomas Hupp, Tobias Keck, Joachim Gerß, Klonek Wojciech, Werner Lang, Björn May, Alexander Meyer, Bernhard Mühling, Alexander Oberhuber, Holger Reinecke, Christian Reinhold, Ralf-Gerhard Ritter, Hubert Schelzig, Christian Schlensack, Thomas Schmitz-Rixen, Karl-Ludwig Schulte, Matthias Spohn, Martin Storck, Matthias Trede, Christian Uhl, Barbara Weis-Müller, Heiner Wenk, Sven Zhorzel, and Alexander Zimmermann

Subjects

Male, medicine.medical_specialty, Time Factors, medicine.medical_treatment, Risk Assessment, Amputation, Surgical, Peripheral Arterial Disease, Ischemia, Risk Factors, Germany, Internal medicine, medicine, Humans, Radiology, Nuclear Medicine and imaging, Prospective Studies, Registries, Myocardial infarction, Renal Insufficiency, Chronic, Aged, Aged, 80 and over, Framingham Risk Score, Proportional hazards model, business.industry, Endovascular Procedures, Hazard ratio, Critical limb ischemia, Limb Salvage, medicine.disease, Confidence interval, Treatment Outcome, Amputation, Chronic Disease, Female, Vascular Grafting, Surgery, medicine.symptom, Cardiology and Cardiovascular Medicine, business, Kidney disease

Abstract

Purpose: To report the outcomes of bypass grafting (BG) vs endovascular therapy (EVT) in patients with non-dialysis-dependent chronic kidney disease (CKD) and chronic limb-threatening ischemia (CLTI). Materials and Methods: The CRITISCH Registry is a prospective, national, interdisciplinary, multicenter registry evaluating the current practice of all available treatment options in 1200 consecutive CLTI patients. For the purposes of this analysis, only the 337 patients with non-dialysis-dependent CKD treated by either BG (n=86; median 78 years, 48 men) or EVT (n=251; median age 80 years, 135 men) were analyzed. The primary composite outcome was amputation-free survival (AFS); secondary outcomes were overall survival (OS) and amputation-free time (AFT). All outcomes were evaluated in Cox proportional hazards models; the results are reported as the hazard ratio (HR) and 95% confidence interval (CI). Results: The Cox regression analysis revealed a significantly greater hazard of amputation or death after BG (HR 1.78, 95% CI 1.05 to 3.03, p=0.028). The models for AFT and overall survival also suggested a higher hazard for BG, but the differences were not significant (AFT: HR 1.66, 95% CI 0.78 to 3.53, p=0.188; OS: HR 1.41, 95% CI 0.80 to 2.47, p=0.348). The absence of runoff vessels (HR 1.73, 95% CI 1.15 to 2.60, p=0.008) was associated with a decreased AFS. The likelihood of amputation was higher in male patients (HR 2.21, 95% CI 1.10 to 4.45, p=0.027) and was associated with a lack of runoff vessels (HR 1.95, 95% CI 0.96 to 3.95, p=0.065) and myocardial infarction (HR 3.74, 95% CI 1.23 to 11.35, p=0.020). Death was more likely in patients without runoff vessels (HR 1.76, 95% CI 1.11 to 2.80, p=0.016) and those with a higher risk score (HR 1.73, 95% CI 1.03 to 2.91, p=0.038). Conclusion: This analysis suggested that BG was associated with poorer AFS than EVT in patients with non-dialysis-dependent CKD and CLTI. Male sex, previous myocardial infarction, and the absence of runoff vessels were additionally identified as predictors of poorer outcomes.

Published

2020

24. Impairment of lysosomal function by Clostridioides difficile TcdB

Author

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

Subjects

metabolism [Bacterial Proteins], Clostridioides difficile, Bacterial Toxins, lysosome inhibition, autophagic flux, Microbiology, metabolism [Lysosomes], Clostridioides, Bacterial Proteins, ddc:570, Clostridioides difficile Toxin B, DQ-BSA assay, Lysosomes, Molecular Biology, metabolism [Bacterial Toxins]

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 endosomal-lysosomal 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.

Published

2022

25. In-hospital outcomes in patients with critical limb ischemia and end-stage renal disease after revascularization

Author

Meyer, Alexander, Lang, Werner, Borowski, Matthias, Torsello, Giovanni, Bisdas, Theodosios, Schmitz-Rixen, Thomas, Gkremoutis, Asimakis, Steinbauer, Markus, Betz, Thomas, Eckstein, Hans-Henning, Zimmermann, Alexander, Schelzig, Hubert, Oberhuber, Alexander, Florek, Hans-Joachim, May, Björn, Storck, Martin, Weis-Müller, Barbara, Reinhold, Christian, Böckler, Dittmar, Billing, Arend, Brixner, Daniel, Hupp, Thomas, Ger, Joachim, Debus, Sebastian E., Spohn, Mathias, Reinecke, Holger, Schlensack, Christian, Donas, Konstantinos P., Stavroulakis, Konstantinos, Klonek, Wojciech, Wenk, Heiner, Trede, Matthias, Ritter, Ralf-Gerhard, Schulte, Karl-Ludwig, Keck, Tobias, Balzer, Kai, Mühling, Bernhard, Adili, Farzin, Grundmann, Reinhardt, and Zeller, Thomas

Published

2016

26. Autorenverzeichnis

Author

Akca, Aycan, primary, Bechstein, Wolf O., additional, Becker, Heinz, additional, Beham, Alexander, additional, Boucher, Marc, additional, Buia, Alexander, additional, Cupisti, Kenko, additional, Dango, Sebastian, additional, Dotzenrath, Cornelia, additional, Germer, C.-T., additional, Michael Ghadimi, B., additional, Goretzki, Peter E., additional, Grade, Marian, additional, Hanisch, E., additional, Hinterthaner, Marc, additional, Hölscher, Arnulf H., additional, Homayounfar, Kia, additional, Hopt, Ulrich T., additional, Horstmann, Olaf, additional, Jänigen, Bernd, additional, Jurowich, Christian, additional, Kauffels, Anne, additional, Kienle, Peter, additional, Kollmar, Otto, additional, Lammers, Bernhard J., additional, Langer, Claus, additional, Lorf, Thomas, additional, Luther, Bernd, additional, Markus, P., additional, Möslein, Gabriela, additional, Post, Stefan, additional, Ritter, Ralf-Gerhard, additional, Schmidt-Wilcke, Philip, additional, Schmitz-Rixen, Thomas, additional, Schneider, Claudia, additional, Schneider, Ralph, additional, Schnitzbauer, Andreas A., additional, Schwarz, Katharina, additional, Simon, Dietmar, additional, Slotta, Jan E., additional, Sprenger, Thilo, additional, Weiner, Rudolf A., additional, Bollschweiler, Elfriede, additional, Bösing, Norbert M., additional, Encke, Albrecht, additional, Gutschow, Christian, additional, Hölscher, Moritz, additional, Liersch, Thorsten, additional, Müller-Dornieden, Annegret, additional, Röher, Hans-Dietrich, additional, Schneider, Paul M., additional, Schröder, Wolfgang, additional, Schulte, Klaus-Martin, additional, Vallböhmer, Daniel, additional, and Wahl, Robert A., additional

Published

2015

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

Author

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

Subjects

RHOA, biology, Chemistry, Familial Mediterranean fever, Clostridium difficile toxin B, Inflammasome, medicine.disease, MEFV, Pyrin domain, Microbiology, Proinflammatory cytokine, Immune system, biology.protein, medicine, medicine.drug

Abstract

Pyrin is a cytosolic immune sensor that forms an inflammasome when bacterial virulence factors inhibit RhoA, triggering the release of inflammatory cytokines, including IL-1β. Gain of function mutations in the MEFV gene encoding Pyrin cause auto-inflammatory disorders, such as familial Mediterranean fever (FMF) and Pyrin associated auto-inflammation with Neutrophilic Dermatosis (PAAND). To precisely define the role of Pyrin in detecting pathogen virulence factors in relevant human immune cells, we investigated how the Pyrin inflammasome response was initiated and regulated in monocyte-derived macrophages (hMDM) compared to human monocytes. Unlike monocytes and murine macrophages, we determined that hMDM failed to activate Pyrin in response to known Pyrin activators Clostridioides difficile (C. difficile) toxins A or B (TcdA or TcdB). In contrast, TcdB activated the NLRP3 inflammasome in hMDM. Notably, we ascertained that the Pyrin inflammasome response could be re-enabled in hMDM by prolonged priming with either LPS or type I or II interferons, and required an increase in Pyrin expression. These data demonstrate an unexpected redundancy in detecting these toxins by inflammasome sensors.

Published

2021

28. Sulfated glycosaminoglycans and low-density lipoprotein receptor contribute to Clostridium difficile toxin A entry into cells

Author

David T. Breault, Lindsey R. Robinson-McCarthy, Zhuoming Liu, Jie Zhang, Songhai Tian, Shin-Ichiro Miyashita, Ralf Gerhard, Sean P. J. Whelan, Siam Oottamasathien, Liang Tao, and Min Dong

Subjects

Microbiology (medical), Colon, Bacterial Toxins, Immunology, Clostridium difficile toxin A, Plasma protein binding, medicine.disease_cause, Endocytosis, Applied Microbiology and Biotechnology, Microbiology, Article, Enterotoxins, Mice, 03 medical and health sciences, Sulfation, Genetics, medicine, Animals, Humans, Intestinal Mucosa, Receptor, Glycosaminoglycans, 030304 developmental biology, 0303 health sciences, Clostridioides difficile, 030306 microbiology, Chemistry, Cell Membrane, Cell Biology, Molecular biology, Receptors, LDL, Mutation, LDL receptor, Heparitin Sulfate, Heparan sulfate analogue, Oligopeptides, Exotoxin, HeLa Cells, Protein Binding

Abstract

Clostridium difficile toxin A (TcdA) is a major exotoxin contributing to disruption of the colonic epithelium during C. difficile infection. TcdA contains a carbohydrate-binding combined repetitive oligopeptides (CROPs) domain that mediates its attachment to cell surfaces, but recent data suggest the existence of CROPs-independent receptors. Here, we carried out genome-wide clustered regularly interspaced short palindromic repeats (CRISPR)-CRISPR-associated protein 9 (Cas9)-mediated screens using a truncated TcdA lacking the CROPs, and identified sulfated glycosaminoglycans (sGAGs) and low-density lipoprotein receptor (LDLR) as host factors contributing to binding and entry of TcdA. TcdA recognizes the sulfation group in sGAGs. Blocking sulfation and glycosaminoglycan synthesis reduces TcdA binding and entry into cells. Binding of TcdA to the colonic epithelium can be reduced by surfen, a small molecule that masks sGAGs, by GM-1111, a sulfated heparan sulfate analogue, and by sulfated cyclodextrin, a sulfated small molecule. Cells lacking LDLR also show reduced sensitivity to TcdA, although binding between LDLR and TcdA are not detected, suggesting that LDLR may facilitate endocytosis of TcdA. Finally, GM-1111 reduces TcdA-induced fluid accumulation and tissue damage in the colon in a mouse model in which TcdA is injected into the caecum. These data demonstrate in vivo and pathological relevance of TcdA-sGAGs interactions, and reveal a potential therapeutic approach of protecting colonic tissues by blocking these interactions.

Published

2019

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

Author

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

Subjects

MEFV protein, human, General Immunology and Microbiology, Inflammasomes, Clostridioides difficile, General Neuroscience, Macrophages, Bacterial Toxins, genetics [Pyrin], genetics [Familial Mediterranean Fever], Pyrin, metabolism [Familial Mediterranean Fever], General Biochemistry, Genetics and Molecular Biology, Familial Mediterranean Fever, trimethylaminocarboxyldihydroboran, Mice, metabolism [Pyrin], Mutation, metabolism [Macrophages], Humans, Animals, ddc:610, General Agricultural and Biological Sciences, metabolism [Inflammasomes]

Abstract

Pyrin is a cytosolic immune sensor that nucleates an inflammasome in response to inhibition of RhoA by bacterial virulence factors, triggering the release of inflammatory cytokines, including IL-1β. Gain-of-function mutations in the MEFV gene encoding Pyrin cause autoinflammatory disorders, such as familial Mediterranean fever (FMF) and Pyrin-associated autoinflammation with neutrophilic dermatosis (PAAND). To precisely define the role of Pyrin in pathogen detection in human immune cells, we compared initiation and regulation of the Pyrin inflammasome response in monocyte-derived macrophages (hMDM). Unlike human monocytes and murine macrophages, we determined that hMDM failed to activate Pyrin in response to known Pyrin activators Clostridioides difficile (C. difficile) toxins A or B (TcdA or TcdB), as well as the bile acid analogue BAA-473. The Pyrin inflammasome response was enabled in hMDM by prolonged priming with either LPS or type I or II interferons and required an increase in Pyrin expression. Notably, FMF mutations lifted the requirement for prolonged priming for Pyrin activation in hMDM, enabling Pyrin activation in the absence of additional inflammatory signals. Unexpectedly, in the absence of a Pyrin response, we found that TcdB activated the NLRP3 inflammasome in hMDM. These data demonstrate that regulation of Pyrin activation in hMDM diverges from monocytes and highlights its dysregulation in FMF.

Published

2021

30. TcdB of Clostridioides difficile Mediates RAS-Dependent Necrosis in Epithelial Cells

Author

Florian Stieglitz, Ralf Gerhard, Rabea Hönig, Klaudia Giehl, and Andreas Pich

Subjects

Inorganic Chemistry, Organic Chemistry, Clostridioides difficile, C. diff, TcdB, phosphoproteomics, RAS, TcdA, pyknosis, glucosyltransferase-independent effect, General Medicine, Physical and Theoretical Chemistry, Molecular Biology, Spectroscopy, Catalysis, Computer Science Applications

Abstract

A Clostridioides difficile infection (CDI) is the most common nosocomial infection worldwide. The main virulence factors of pathogenic C. difficile are TcdA and TcdB, which inhibit small Rho-GTPases. The inhibition of small Rho-GTPases leads to the so-called cytopathic effect, a reorganization of the actin cytoskeleton, an impairment of the colon epithelium barrier function and inflammation. Additionally, TcdB induces a necrotic cell death termed pyknosis in vitro independently from its glucosyltransferases, which are characterized by chromatin condensation and ROS production. To understand the underlying mechanism of this pyknotic effect, we conducted a large-scale phosphoproteomic study. We included the analysis of alterations in the phosphoproteome after treatment with TcdA, which was investigated for the first time. TcdA exhibited no glucosyltransferase-independent necrotic effect and was, thus, a good control to elucidate the underlying mechanism of the glucosyltransferase-independent effect of TcdB. We found RAS to be a central upstream regulator of the glucosyltransferase-independent effect of TcdB. The inhibition of RAS led to a 68% reduction in necrosis. Further analysis revealed apolipoprotein C-III (APOC3) as a possible crucial factor of CDI-induced inflammation in vivo.

Published

2022

31. Receptor Binding Domains of TcdB from Clostridioides difficile for Chondroitin Sulfate Proteoglycan-4 and Frizzled Proteins Are Functionally Independent and Additive

Author

Dennis Schöttelndreier, Daniel Henkel, Ralf Gerhard, Helma Tatge, Liang Tao, and Min Dong

Subjects

Virulence Factors, Health, Toxicology and Mutagenesis, receptor binding, Bacterial Toxins, lcsh:Medicine, Clostridium difficile toxin B, Toxicology, Article, Clostridioides difficile, Cell Line, HeLa, 03 medical and health sciences, chemistry.chemical_compound, Bacterial Proteins, Humans, Cytotoxic T cell, Protein Interaction Domains and Motifs, Chondroitin sulfate, Receptor, Chondroitin Sulfate Proteoglycan 4, 030304 developmental biology, Cytopathic effect, 0303 health sciences, biology, 030302 biochemistry & molecular biology, lcsh:R, Membrane Proteins, biology.organism_classification, Molecular biology, Frizzled Receptors, Amino Acid Substitution, Chondroitin Sulfate Proteoglycans, chemistry, CSPG4, Gene Knockdown Techniques, Mutagenesis, Site-Directed, glucosyltransferase, HeLa Cells, Protein Binding

Abstract

Toxin B (TcdB) produced by Clostridioides difficile is a main pathogenicity factor that affects a variety of different cell types within the colonic mucosa. TcdB is known to utilize frizzled-1,2,7 and chondroitin sulfate proteoglycan-4 (CSPG4) as protein receptors. By using human cervical cancer cell line HeLa CSPG4 knockout (CSPG4&minus, /&minus, ) cells as well as TcdB mutants which do not bind to either CSPG4 or frizzled-1,2,7, or both, we evaluated the impact of the individual receptors for cytopathic and cytotoxic effects of TcdB. We compared TcdB from the reference strain VPI10463 (TcdBVPI) and the endemic strain R20291 (TcdBR20) which does not interact with frizzled-1,2,7. TcdBVPI devoid of CSPG4 binding (TcdBVPI &Delta, CROP) shows identical cytopathic potency as full-length TcdB in HeLa CSPG4&minus, cells, indicating that interaction with frizzled proteins is not affected in the presence of the C-terminal CROP domain. We validated CSPG4 as cellular receptor for both TcdB toxinotypes in HeLa and HEp-2 cells. By exchange of a single phenylalanine residue, 1597 with serine, we generated a mutated TcdBVPI variant (TcdBVPI F1597S) that in accordance with TcdBR20 lacks binding to frizzled-1,2,7 and showed identical potency as TcdBR20 on HeLa cells. This enabled us to estimate the respective share of CSPG4 and frizzled-1,2,7 in the cytotoxic and cytopathic effect induced by TcdB. Our data reveal that binding to frizzled-1,2,7 and to CSPG4 occurs independently and in an additive manner.

Published

2020

32. Bypass Grafting vs Endovascular Therapy in Patients With Non-Dialysis-Dependent Chronic Kidney Disease and Chronic Limb-Threatening Ischemia (CRITISCH Registry)

Author

Stavroulakis, Konstantinos, primary, Gkremoutis, Asimakis, additional, Borowski, Matthias, additional, Torsello, Giovanni, additional, Böckler, Dittmar, additional, Zeller, Thomas, additional, Steinbauer, Markus, additional, Tsilimparis, Nikolaos, additional, Bisdas, Theodosios, additional, Adili, Farzin, additional, Balzer, Kai, additional, Billing, Arend, additional, Brixner, Daniel, additional, Debus, Sebastian E., additional, Florek, Hans-Joachim, additional, Grundmann, Reinhardt, additional, Hupp, Thomas, additional, Keck, Tobias, additional, Gerß, Joachim, additional, Wojciech, Klonek, additional, Lang, Werner, additional, May, Björn, additional, Meyer, Alexander, additional, Mühling, Bernhard, additional, Oberhuber, Alexander, additional, Reinecke, Holger, additional, Reinhold, Christian, additional, Ritter, Ralf-Gerhard, additional, Schelzig, Hubert, additional, Schlensack, Christian, additional, Schmitz-Rixen, Thomas, additional, Schulte, Karl-Ludwig, additional, Spohn, Matthias, additional, Storck, Martin, additional, Trede, Matthias, additional, Uhl, Christian, additional, Weis-Müller, Barbara, additional, Wenk, Heiner, additional, Zhorzel, Sven, additional, and Zimmermann, Alexander, additional

Published

2020

33. Autorinnen und Autoren

Author

Bauer, Hartwig, primary, Bechstein, Wolf O., additional, Becker, Heinz, additional, Bollschweiler, Elfriede, additional, Bösing, Norbert M., additional, Branscheid, Detlev, additional, Cupisti, Kenko, additional, Diemel, Klaus D., additional, Dotzenrath, Cornelia, additional, Drücke, Daniel, additional, Ebener, Christoph, additional, Encke, Albrecht, additional, Fieguth, Hans-Gerd, additional, Franke, Claus, additional, Ghadimi, B. Michael, additional, Goretzki, Peter E., additional, Groß-Weege, Wilhelm, additional, Grund, Karl E., additional, Gutschow, Christian, additional, Hanisch, Ernst, additional, Hesterberg, Rudolf, additional, Heller, Klaus, additional, Hölscher, Arnulf H., additional, Hölscher, Moritz, additional, Holzer, Katharina, additional, Homann, Heinz H., additional, Hopt, Ulrich T., additional, Horeyseck, Günter, additional, Horstmann, Olaf, additional, Langer, Claus, additional, Langer, Stefan, additional, Lenhardt, Marcus, additional, Leister, Ingo, additional, Liersch, Torsten, additional, Lorf, Thomas, additional, Luther, Bernd L.P., additional, Markus, Bernd H., additional, Markus, Peter M., additional, Menger, Michael D., additional, Möslein, Gabriela, additional, Müller-Dornieden, Annegret, additional, Neugebauer, Edmund A.M., additional, Ohmann, Christian, additional, Olbrisch, Rolf R., additional, Post, Stefan, additional, Raffel, Andreas, additional, Riess, Hanno, additional, Ritter, Ralf-Gerhard, additional, Röher, Hans-Dietrich, additional, Röhrborn, Ansgar, additional, Sachs, Michael, additional, Schaudt, André, additional, Schlemminger, Rolf, additional, Schmidt, W. Ulrich, additional, Schmidt-Matthiesen, Andreas, additional, Schmitz-Rixen, Thomas, additional, Schneider, Paul M., additional, Schröder, Wolfgang, additional, Schulte, Klaus-Martin, additional, Schulze, Frank P., additional, Simanski, Christian J.P., additional, Simon, Dietmar, additional, Steinau, Hans Ulrich, additional, Steinsträsser, Lars, additional, Steitz, Heinrich Otto, additional, Thon, Klaus-Peter, additional, Ulsenheimer, Klaus, additional, Vallböhmer, Daniel, additional, Wagner, Roland, additional, Wahl, Robert A., additional, Weiner, Rudolf A., additional, and Wenisch, Hubertus C., additional

Published

2006

34. Genome-Wide CRISPR Screen Identifies Semaphorin 6A and 6B as Receptors for Paeniclostridium sordellii Toxin TcsL

Author

Hong Chen, Hao Wu, Min Dong, Ji Zeng, Yang Liu, Liu Hao, Ralf Gerhard, Mei Yuk Choi, and Songhai Tian

Subjects

Male, Frizzled, Lung Neoplasms, Virulence Factors, Bacterial Toxins, Clostridium sordellii, Clostridium difficile toxin B, Semaphorins, Biology, medicine.disease_cause, Microbiology, Virulence factor, Article, 03 medical and health sciences, Gene Knockout Techniques, Mice, 0302 clinical medicine, Semaphorin, Bacterial Proteins, Virology, Cell Line, Tumor, medicine, Animals, Humans, Clustered Regularly Interspaced Short Palindromic Repeats, Receptor, 030304 developmental biology, 0303 health sciences, Binding Sites, Toxin, Endothelial Cells, biology.organism_classification, Cell biology, A549 Cells, Parasitology, Female, CRISPR-Cas Systems, 030217 neurology & neurosurgery, Exotoxin, HeLa Cells, Protein Binding

Abstract

Summary The exotoxin TcsL is a major virulence factor in Paeniclostridium (Clostridium) sordellii and responsible for the high lethality rate associated with P. sordellii infection. Here, we present a genome-wide CRISPR-Cas9-mediated screen using a human lung carcinoma cell line and identify semaphorin (SEMA) 6A and 6B as receptors for TcsL. Disrupting SEMA6A/6B expression in several distinct human cell lines and primary human endothelial cells results in reduced TcsL sensitivity, while SEMA6A/6B over-expression increases their sensitivity. TcsL recognizes the extracellular domain (ECD) of SEMA6A/6B via a region homologous to the receptor-binding site in Clostridioides difficile toxin B (TcdB), which binds the human receptor Frizzled. Exchanging the receptor-binding interfaces between TcsL and TcdB switches their receptor-binding specificity. Finally, administration of SEMA6A-ECD proteins protects human cells from TcsL toxicity and reduces TcsL-induced damage to lung tissues and the lethality rate in mice. These findings establish SEMA6A and 6B as pathophysiologically relevant receptors for TcsL.

Published

2019

35. Ruptured abdominal aortic aneurysm with aorto-caval fistula

Author

Adili, Farzin, Balzer, Jörn O., Ritter, Ralf-Gerhard, Schmandra, Thomas C., Tenholt, Matthias, Vogl, Thomas J., and Schmitz-Rixen, Thomas

Published

2004

36. Endovascular Therapy Versus Bypass Surgery as First-Line Treatment Strategies for Critical Limb Ischemia

Author

Theodosios Bisdas, Matthias Borowski, Konstantinos Stavroulakis, Giovanni Torsello, Farzin Adili, Kai Balzer, Arend Billing, Dittmar Böckler, Daniel Brixner, Sebastian E. Debus, Hans-Henning Eckstein, Hans-Joachim Florek, Asimakis Gkremoutis, Reinhardt Grundmann, Thomas Hupp, Tobias Keck, Joachim Gerß, Wojciech Klonek, Werner Lang, Björn May, Alexander Meyer, Bernhard Mühling, Alexander Oberhuber, Holger Reinecke, Christian Reinhold, Ralf-Gerhard Ritter, Hubert Schelzig, Christian Schlensack, Thomas Schmitz-Rixen, Karl-Ludwig Schulte, Matthias Spohn, Markus Steinbauer, Martin Storck, Matthias Trede, Christian Uhl, Barbara Weis-Müller, Heiner Wenk, Thomas Zeller, Sven Zhorzel, and Alexander Zimmermann

Subjects

medicine.medical_specialty, business.industry, medicine.medical_treatment, Hazard ratio, Retrospective cohort study, Critical limb ischemia, 030204 cardiovascular system & hematology, Interim analysis, Confidence interval, law.invention, Surgery, 03 medical and health sciences, 0302 clinical medicine, Randomized controlled trial, Bypass surgery, Amputation, law, medicine, 030212 general & internal medicine, medicine.symptom, Cardiology and Cardiovascular Medicine, business

Abstract

Objectives The most effective first-line treatment between endovascular therapy and bypass surgery for patients with critical limb ischemia (CLI) is still not well defined. The primary aim of the interim analysis of CRITISCH (Registry of First-Line Treatments in Patients With Critical Limb Ischemia) was to compare both treatment options in a prospective confirmatory manner. Background Only 1 randomized controlled trial between endovascular therapy and bypass surgery has been published yet. Several retrospective studies showed comparable outcomes between the 2 treatment strategies, but in the majority of them, current endovascular technologies have not been included. Methods Between January 2013 and September 2014, 1,200 CLI patients (Rutherford 4 to 6) from 27 vascular centers were enrolled. The selection of the first-line treatment was left completely to the discretion of the responsible physician. The primary composite endpoint was amputation-free survival (AFS), that is, time to major amputation and/or death from any cause. A pre-specified interim analysis aimed at showing noninferiority of the endovascular therapy versus bypass surgery as to the hazard ratio (HR) of AFS (noninferiority bound = 1.33; interim α = 0.0058). Time-to-event analyses of major amputation, death, and the composite endpoint of reintervention and/or above-ankle amputation were also conducted. Results Endovascular therapy was applied to 642 (54%) and bypass surgery to 284 (24%) patients. Median follow-up time was 12 months in both groups. One-year AFS was 75% and 72%, respectively. The noninferiority of endovascular therapy versus bypass surgery for AFS was confirmed (HR: 0.91; upper bound of 1-sided (1 − 0.0058) confidence interval [CI]: 1.29; p = 0.003). An impact of the treatment strategy on time until death (HR: 1.14; 95% CI: 0.80 to 1.63; p = 0.453), major amputation (HR: 0.86; 95% CI:0.56 to 1.30; p = 0.463), and reintervention and/or above-ankle amputation (HR: 0.89; 95% CI: 0.70 to 1.14; p = 0.348) was not observed. Conclusions The interim analysis confirmed that when physicians are free to individualize therapy to CLI patients, the endovascular-first approach achieved a noninferior AFS rate compared with bypass surgery. (Registry of First-Line Treatments in Patients With Critical Limb Ischemia [CRITISCH]; NCT01877252)

Published

2016

37. Difference in Mono-O-Glucosylation of Ras Subtype GTPases Between Toxin A and Toxin B From Clostridioides difficile Strain 10463 and Lethal Toxin From Clostridium sordellii Strain 6018

Author

Ilona Schelle, Johannes Junemann, Ralf Gerhard, Ingo Just, Arlen-Celina Lücke, Chantal M. Lämmerhirt, Andreas Pich, and Harald Genth

Subjects

0301 basic medicine, Microbiology (medical), lcsh:QR1-502, Clostridium difficile toxin A, Clostridium difficile toxin B, Clostridium sordellii, macromolecular substances, GTPase, medicine.disease_cause, Microbiology, lcsh:Microbiology, Proinflammatory cytokine, 03 medical and health sciences, Rho, medicine, large clostridial glucosylating toxins, 030102 biochemistry & molecular biology, biology, Toxin, Chemistry, fungi, Inflammasome, MRM analysis, biology.organism_classification, Molecular biology, carbohydrates (lipids), 030104 developmental biology, biology.protein, Antibody, Ras, medicine.drug

Abstract

Clostridioides difficile toxin A (TcdA) and Toxin B (TcdB) trigger inflammasome activation with caspase-1 activation in cultured cells, which in turn induce the release of IL-6, IFN-γ, and IL-8. Release of these proinflammatory responses is positively regulated by Ras-GTPases, which leads to the hypothesis that Ras glucosylation by glucosylating toxins results in (at least) reduced proinflammatory responses. Against this background, data on toxin-catalyzed Ras glucosylation are required to estimate of pro-inflammatory effect of the glucosylating toxins. In this study, a quantitative evaluation of the GTPase substrate profiles glucosylated in human colonic (Caco-2) cells treated with either TcdA, TcdB, or the related Clostridium sordellii lethal toxin (TcsL) was performed using multiple reaction monitoring (MRM) mass spectrometry. (H/K/N)Ras are presented to be glucosylated by TcsL and TcdA but by neither TcdB isoform tested. Furthermore, the glucosylation of (H/K/N)Ras was detected in TcdA-(not TcdB)-treated cells, as analyzed exploiting immunoblot analysis using the Ras glucosylation-sensitive 27H5 antibody. Furthermore, [14C]glucosylation of substrate GTPase was found to be increased in a cell-free system complemented with Caco-2 lysates. Under these conditions, (H/K/N)Ras glucosylation by TcdA was detected. In contrast, TcdB-catalyzed (H/K/N)Ras glucosylation was detected by neither MRM analysis, immunoblot analysis nor [14C]glucosylation in a cell-free system. The observation that TcdA (not TcdB) glucosylates Ras subtype GTPases correlates with the fact that TcdB (not TcdA) is primarily responsible for inflammatory responses in CDI. Finally, TcsL more efficaciously glucosylated Ras subtype GTPase as compared with TcdA, reinforcing the paradigm that TcsL is the prototype of a Ras glucosylating toxin.

Published

2018

38. Quantitative Phosphoproteome Analysis of Clostridioides difficile Toxin B Treated Human Epithelial Cells

Author

Andreas Pich, Johannes Junemann, Ingo Just, and Ralf Gerhard

Subjects

0301 basic medicine, Microbiology (medical), Mutant, lcsh:QR1-502, Clostridium difficile toxin B, GTPase, Microbiology, small GTPases, Virulence factor, lcsh:Microbiology, TcdB, 03 medical and health sciences, Stable isotope labeling by amino acids in cell culture, Kinome, Shotgun proteomics, Original Research, 030102 biochemistry & molecular biology, biology, Chemistry, Clostridioides difficile, phosphoproteome, Molecular biology, 030104 developmental biology, shotgun proteomics, biology.protein, Glucosyltransferase

Abstract

The large clostridial glucosylating toxin B (TcdB) is a major virulence factor of the nosocomial pathogen Clostridioides difficile. TcdB inhibits small GTPases by glucosylation leading to impaired downstream signaling. TcdB also possesses a glucosyltransferase independent effect described as pyknosis. To elucidate the impact of TcdB and its glucosylation-inactive mutant TcdBNXN on the kinome of human cells, SILAC labeled HEp-2 cells were treated with 2 nM TcdB for 8 h. Phosphopeptides were enriched using SCX chromatography, IMAC and TiO2 followed shotgun mass spectrometry analysis. Overall 4,197 phosphopeptides were identified; more than 1,200 phosphosites responded to treatment with TcdB or TcdBNXN. The data suggested that predominantly stress-activated MAPK-dependent signaling pathways were triggered by toxin B treatment.

Published

2018

39. The Conserved Cys-2232 in Clostridioides difficile Toxin B Modulates Receptor Binding

Author

Helma Tatge, Lara-Antonia Beer, Viola Fühner, Ralf Gerhard, Michael Hust, Soo-Young Chung, and Dennis Schöttelndreier

Subjects

0301 basic medicine, Microbiology (medical), antibody phage display, Oligopeptide, Phage display, biology, Clostridioides difficile, Chemistry, receptor binding, toxins, lcsh:QR1-502, Clostridium difficile toxin B, neutralization, Microbiology, Molecular biology, lcsh:Microbiology, autoproteolysis, 03 medical and health sciences, 030104 developmental biology, Glucosyltransferases, biology.protein, Antibody, Tyrosine, Receptor, Cysteine

Abstract

Clostridioides difficile toxins TcdA and TcdB are large clostridial glucosyltransferases which are the main pathogenicity factors in C. difficile-associated diseases. Four highly conserved cysteines are present in all large clostridial glucosyltransferases. In this study we focused on the conserved cysteine 2232 within the combined repetitive oligopeptide domain of TcdB from reference strain VPI10463 (clade I). Cysteine 2232 is not present in TcdB from hypervirulent strain R20291 (clade II), where a tyrosine is found instead. Replacement of cysteine 2232 by tyrosine in TcdBV PI10463 reduced binding to the soluble fragments of the two known TcdB receptors, frizzled-2 (FZD2) and poliovirus receptor-like protein-3/nectin-3 (PVRL3). In line with this, TcdBR20291 showed weak binding to PVRL3 in pull-down assays which was increased when tyrosine 2232 was exchanged for cysteine. Surprisingly, we did not observe binding of TcdBR20291 to FZD2, indicating that this receptor is less important for this toxinotype. Competition assay with the receptor binding fragments (aa 1101–1836) of TcdBV PI10463 and TcdBR20291, as well as antibodies newly developed by antibody phage display, revealed different characteristics of the yet poorly described delivery domain of TcdB harboring the second receptor binding region. In summary, we found that conserved Cys-2232 in TcdB indirectly contributes to toxin–receptor interaction.

Published

2018

40. One-Year Results of First-Line Treatment Strategies in Patients With Critical Limb Ischemia (CRITISCH Registry)

Author

Konstantinos Stavroulakis, Matthias Borowski, Giovanni Torsello, Theodosios Bisdas, Farzin Adili, Kai Balzer, Arend Billing, Dittmar Böckler, Daniel Brixner, E. Sebastian Debus, Hans-Henning Eckstein, Hans-Joachim Florek, Asimakis Gkremoutis, Reinhardt Grundmann, Thomas Hupp, Tobias Keck, Joachim Gerß, Klonek Wojciech, Werner Lang, Björn May, Alexander Meyer, Bernhard Mühling, Alexander Oberhuber, Holger Reinecke, Christian Reinhold, Ralf-Gerhard Ritter, Hubert Schelzig, Christian Schlensack, Thomas Schmitz-Rixen, Karl-Ludwig Schulte, Matthias Spohn, Markus Steinbauer, Martin Storck, Matthias Trede, Christian Uhl, Barbara Weis-Müller, Heiner Wenk, Thomas Zeller, Sven Zhorzel, and Alexander Zimmermann

Subjects

Male, medicine.medical_specialty, Time Factors, Bypass grafting, medicine.medical_treatment, Critical Illness, Clinical Decision-Making, 030204 cardiovascular system & hematology, Conservative Treatment, Amputation, Surgical, 03 medical and health sciences, Peripheral Arterial Disease, 0302 clinical medicine, Ischemia, Risk Factors, Angioplasty, Germany, medicine, Humans, Radiology, Nuclear Medicine and imaging, In patient, 030212 general & internal medicine, Prospective Studies, Registries, Aged, Aged, 80 and over, business.industry, Patient Selection, Endovascular Procedures, Stent, Critical limb ischemia, Middle Aged, Limb Salvage, Progression-Free Survival, Surgery, Conservative treatment, First line treatment, Amputation, Female, Vascular Grafting, medicine.symptom, Cardiology and Cardiovascular Medicine, business

Abstract

Purpose: To examine the outcomes of all first-line strategies for the treatment of critical limb ischemia (CLI), identify factors that influenced the treatment choice, and determine the risk of amputation or death after each treatment. Methods: CRITISCH ( ClinicalTrials.gov identifier NCT01877252) is a multicenter, national, prospective registry evaluating all available treatment strategies applied in 1200 consecutive CLI patients in 27 vascular centers in Germany. The recruitment started in January 2013 and was completed in September 2014. Treatment options were endovascular revascularization (642, 53.5%), bypass surgery (284, 23.7%), femoral artery patchplasty (126, 10.5%) with or without concomitant peripheral intervention, conservative treatment (118, 9.8%), and primary major amputation (30, 2.5%). The primary endpoint of this study was amputation-free survival (AFS). The Society of Vascular Surgery’s suggested objective performance goal (OPG) for AFS (71%) was used as the effectiveness criterion. Multivariable regression methods were employed to identify variables that influenced the treatment selection and AFS after each treatment; results are presented as the hazard ratio (HR) and 95% confidence interval (CI). Results: The 12-month AFS estimates following endovascular therapy, bypass grafting, femoral patchplasty, and conservative treatment were 75%, 72%, 73%, and 72%, respectively. Factors influencing treatment choice were age, chronic kidney disease (CKD), diabetes, smoking, prior vascular procedures in the index leg, TransAtlantic Inter-Society Consensus II C/D lesions, and absence of runoff vessels. Cox regression analysis identified CKD (HR 2.07, 95% CI 1.26 to 3.41, p=0.004), the use of a prosthetic bypass conduit (HR 1.97, 95% CI 1.23 to 3.14, p=0.004), and previous vascular intervention in the index limb (HR 1.52, 95% CI 0.94 to 2.43, p=0.085) as independent risk factors for diminished AFS after bypass surgery. CKD (HR 1.47, 95% CI 1.09 to 1.99, p=0.012) and Rutherford category 6 (HR 1.81, 95% CI 1.30 to 2.52, p

Published

2018

41. Early cell death induced by Clostridium difficile TcdB: Uptake and Rac1-glucosylation kinetics are decisive for cell fate

Author

Klemens Rottner, Helma Tatge, Alexandra Olling, Ralf Gerhard, Sebastian Goy, Nicole Reich, Alexi K. Alekov, Lara-Antonia Beer, Michel Tenspolde, and Helmholtz-Zentrum für Infektionsforschung GmbH, Inhoffenstr. 7, 38124 Braunschweig, Germany.

Subjects

0301 basic medicine, rac1 GTP-Binding Protein, Programmed cell death, Glycosylation, Sodium-Hydrogen Exchangers, Endosome, Immunology, Bacterial Toxins, Clostridium difficile toxin A, Clostridium difficile toxin B, Apoptosis, Biology, Microbiology, Cell Line, 03 medical and health sciences, Bacterial Proteins, Virology, Humans, Cytotoxicity, reactive oxygen species, Clostridioides difficile, toxins, cellular uptake, Transfection, clostridium difficile, Molecular biology, Cytosol, Proton-Translocating ATPases, 030104 developmental biology, cell death, HEK293 Cells, Reactive Oxygen Species, Intracellular

Abstract

Toxin A and Toxin B (TcdA/TcdB) are large glucosyltransferases produced by Clostridium difficile. TcdB but not TcdA induces reactive oxygen species-mediated early cell death (ECD) when applied at high concentrations. We found that nonglucosylated Rac1 is essential for induction of ECD since inhibition of Rac1 impedes this effect. ECD only occurs when TcdB is rapidly endocytosed. This was shown by generation of chimeras using the trunk of TcdB from a hypervirulent strain. TcdB from hypervirulent strain has been described to translocate from endosomes at higher pH values and thus, meaning faster than reference type TcdB. Accordingly, intracellular delivery of the glucosyltransferase domain of reference TcdB by the trunk of TcdB from hypervirulent strain increased ECD. Furthermore, proton transporters such as sodium/proton exchanger (NHE) or the ClC-5 anion/proton exchanger, both of which contribute to endosomal acidification, also affected cytotoxic potency of TcdB: Specific inhibition of NHE reduced cytotoxicity, whereas transfection of cells with the endosomal anion/proton exchanger ClC-5 increased cytotoxicity of TcdB. Our data suggest that both the uptake rate of TcdB into the cytosol and the status of nonglucosylated Rac1 are key determinants that are decisive for whether ECD or delayed apoptosis is triggered.

Published

2018

42. Clostridium difficile toxin B inhibits the secretory response of human mast cell line-1 (HMC-1) cells stimulated with high free-Ca2+ and GTPγS

Author

Ralf Gerhard, Dorothea Lorenz, Hans Bigalke, Andrea Balletta, Florian Wegner, and Andreas Rummel

Subjects

Clostridium difficile toxin A, Clostridium difficile toxin B, Pseudomembranous colitis, Biology, Toxicology, Actin cytoskeleton, Mast cell, Molecular biology, Exocytosis, Microbiology, medicine.anatomical_structure, medicine, Secretion, Intracellular

Abstract

Clostridium difficile toxins A and B (TcdA and TcdB) belong to the class of large clostridial cytotoxins and inactivate by glucosylation some low molecular mass GTPases of the Rho-family (predominantly Rho, Rac and Cdc42), known as regulators of the actin cytoskeleton. TcdA and B also represent the main virulence factors of the anaerobic gram-positive bacterium that is the causal agent of pseudomembranous colitis. In our study, TcdB was chosen instead of TcdA for the well-known higher cytotoxic potency. Inactivation of Rho-family GTPases by this toxin in our experimental conditions induced morphological changes and reduction of electron-dense mast cell-specific granules in human mast cell line-1 (HMC-1) cells, but not cell death or permeabilisation of plasma-membranes. Previously reported patch-clamp dialysis experiments revealed that high intracellular free-Ca(2+) and GTPγS concentrations are capable of inducing exocytosis as indicated by significant membrane capacitance (Cm) increases in HMC-1 cells. In this study, we investigated the direct effects of TcdB upon HMC-1 cell "stimulated" Cm increase, as well as on "constitutive" secretion of hexosaminidase and interleukin-16 (IL-16). Compared to untreated control cells, HMC-1 cells incubated with TcdB for 3-24h exhibited a significant reduction of the mean absolute and relative Cm increase in response to free-Ca(2+) and GTPγS suggesting an inhibition of secretory processes by TcdB. In conclusion, the HMC-1 cell line represents a suitable model for the study of direct effects of C. difficile toxins on human mast cell secretory activity.

Published

2015

43. Outcomes of dialysis patients with critical limb ischemia after revascularization compared with patients with normal renal function

Author

Matthias Trede, Reinhardt Grundmann, Thomas Hupp, Hans-Joachim Florek, Alexander Zimmermann, Tobias Keck, K. Balzer, Ralf-Gerhard Ritter, Christian Reinhold, Cornelia Fiessler, Asimakis Gkremoutis, Karl-Ludwig Schulte, Werner Lang, Joachim Gerß, Klonek Wojciech, Holger Reinecke, Heiner Wenk, Björn May, Konstantinos P. Donas, Giovanni Torsello, Christian Uhl, Daniel Brixner, Thomas Schmitz-Rixen, Bernhard Mühling, Christian Schlensack, Farzin Adili, Markus Steinbauer, Mathias Spohn, Theodosios Bisdas, Hubert Schelzig, Martin Storck, Konstantinos Stavroulakis, B.T. Weis-Müller, Thomas Zeller, Hans-Henning Eckstein, Alexander Oberhuber, Alexander Meyer, Sebastian Debus, Dittmar Böckler, and Arend Billing

Subjects

Male, medicine.medical_specialty, medicine.medical_treatment, Endarterectomy, 030204 cardiovascular system & hematology, urologic and male genital diseases, Revascularization, 03 medical and health sciences, 0302 clinical medicine, Ischemia, Renal Dialysis, Risk Factors, Germany, medicine, Humans, 030212 general & internal medicine, Registries, Survival rate, Aged, Retrospective Studies, business.industry, Proportional hazards model, Vascular disease, Endovascular Procedures, Retrospective cohort study, Critical limb ischemia, Middle Aged, medicine.disease, Limb Salvage, female genital diseases and pregnancy complications, Surgery, Survival Rate, Treatment Outcome, Bypass surgery, Lower Extremity, Kidney Failure, Chronic, Female, medicine.symptom, Cardiology and Cardiovascular Medicine, business, Vascular Surgical Procedures

Abstract

An analysis was conducted of intermediate outcomes and possible influencing factors in patients with end-stage renal disease (ESRD) and critical limb ischemia after lower limb revascularization compared with patients with regular renal function (non-ESRD).Data collection was performed by inquiry of the German multicenter registry of First-Line Treatments in Patients with Critical Limb Ischemia (CRITISCH); 102 ESRD patients and 674 non-ESRD patients were included. Four different therapy modalities were analysed: bypass surgery, endovascular therapy (EVT), femoral artery endarterectomy, and no vascular intervention (conservative treatment or primary major amputation). Predefined end points were amputation-free survival (AFS), death, major amputation, and reintervention. Cox regression models were built to analyze independent risk factors for outcome parameters.ESRD patients showed inferior results at 2 years in the rate of AFS (ESRD, 35.4%; non-ESRD, 67.2%; P .001). Similarly, death rate (ESRD, 55.0%; non-ESRD, 20.7%; P .001) and major amputation rate (ESRD, 24.5%; non-ESRD, 15.8%; P = .029) were significantly elevated for ESRD patients. The choice of therapeutic approach in ESRD did not influence the incidence of the investigated end points (death or major amputation: EVT, 56.9% vs bypass, 76.9% [P = .225]; death: EVT, 46.2% vs bypass, 61.5% [P = .372]; amputation: EVT, 15.4% vs bypass, 15.4% [P = 1.000]; reintervention: EVT, 32.3% vs bypass, 15.4% [P = .324]). Cox regression analysis indicated that dialysis patients carry a twofold increased hazard of death or major amputation (hazard ratio, 2.27; 95% confidence interval, 1.67-3.10; P .001), and open surgical treatment (all patients combined) was associated with reduced risk of death compared with EVT (hazard ratio, 0.58; 95% confidence interval, 0.37-0.91; P = .017). Comorbidities were not found to have a noticeable impact on AFS, survival, reintervention, or major amputation.Two-year AFS, overall survival, and freedom from major amputation were decreased in ESRD patients compared with non-ESRD patients with critical limb ischemia. Cardiovascular comorbidities were without significant impact on outcome parameters, whereas choice of treatment modality within the ESRD group did not influence AFS. Decision-making in ESRD as to choice of therapeutic approach in dialysis patients should notably account for the individual's lesion characteristics and vascular disease; surgical revascularization and EVT may be used as complementary options.

Published

2017

44. Association between statin therapy and amputation-free survival in patients with critical limb ischemia in the CRITISCH registry

Author

Reinhardt Grundmann, Martin Storck, Hans-Joachim Florek, Asimakis Gkremoutis, Konstantinos Stavroulakis, Christian Schlensack, B.T. Weis-Müller, Werner Lang, Matthias Borowski, Joachim Gerß, Giovanni Torsello, Christian Uhl, Daniel Brixner, Sebastian Debus, Matthias Trede, Wojciech Klonek, Markus Steinbauer, Arend Billing, Alexander Meyer, Dittmar Böckler, Alexander Zimmermann, Tobias Keck, K. Balzer, Karl-Ludwig Schulte, Christian Reinhold, Holger Reinecke, Theodosios Bisdas, Thomas Zeller, Bernhard Mühling, Hans-Henning Eckstein, Farzin Adili, Matthias Spohn, Alexander Oberhuber, Heiner Wenk, Sven Zhorzel, Thomas Schmitz-Rixen, Ralf-Gerhard Ritter, Björn May, Hubert Schelzig, and Thomas Hupp

Subjects

Male, Time Factors, medicine.medical_treatment, Comorbidity, Kaplan-Meier Estimate, 030204 cardiovascular system & hematology, 0302 clinical medicine, Ischemia, Risk Factors, Germany, Odds Ratio, Secondary Prevention, 030212 general & internal medicine, Registries, Aged, 80 and over, Endovascular Procedures, Age Factors, Middle Aged, Limb Salvage, Treatment Outcome, Platelet aggregation inhibitor, Female, medicine.symptom, Cardiology and Cardiovascular Medicine, medicine.medical_specialty, Statin, medicine.drug_class, Critical Illness, Revascularization, Risk Assessment, Amputation, Surgical, Disease-Free Survival, 03 medical and health sciences, Peripheral Arterial Disease, Internal medicine, medicine, Humans, Aged, Dyslipidemias, Proportional Hazards Models, business.industry, Proportional hazards model, Critical limb ischemia, Odds ratio, Protective Factors, medicine.disease, Surgery, Logistic Models, Amputation, Multivariate Analysis, Vascular Grafting, Hydroxymethylglutaryl-CoA Reductase Inhibitors, business, Platelet Aggregation Inhibitors

Abstract

Secondary prevention in patients with critical limb ischemia (CLI) is crucial for the reduction of cardiovascular morbidity and mortality. Nonetheless, current recommendations are extrapolated from other high-risk populations because of the lack of CLI-dedicated trials. The aim of this explorative study was to evaluate the association of statin therapy with the outcomes of CLI patients.The First-Line Treatments in Patients With Critical Limb Ischemia (CRITISCH) registry is a prospective multicenter registry analyzing the effectiveness of all available treatment strategies in 1200 CLI patients. For the purposes of this analysis, patients were divided into two groups based on statin administration. Treatment crossovers and nonadherent patients were excluded from analysis. The primary composite end point of this study was the amputation-free survival (AFS). Major adverse cardiovascular and cerebral events (MACCEs), time to death, and time to major amputation were also analyzed.Statin therapy was applied in 445 individuals (37%), 371 (31%) patients received no statins, and 384 subjects were excluded from analysis (treatment crossovers). Patients receiving statins were more likely to be younger (P .001) and to have a history of coronary heart disease (P .001) or previous intervention at index limb (P .001). Patients receiving statin therapy had a lower hazard regarding AFS (hazard ratio [HR], 0.45; 95% confidence interval [CI], 0.34-0.63; P .001) and death (HR, 0.40; 95% CI, 0.24-0.66; P .001) as well as lower odds of MACCE (odds ratio, 0.41; 95% CI, 0.23-0.69; P = .001). However, statin therapy was not associated with reduced amputation rates (HR, 1.02; 95% CI, 0.67-1.56; P = .922). Statin effect on AFS was consistent among diabetics (HR, 0.47; 95% CI, 0.31-0.70; P .001), patients with chronic kidney disease (HR, 0.53; 95% CI, 0.32-0.87; P = .012), and patients older than 75 years (HR, 0.40; 95% CI, 0.26-0.60; P .001). Statin administration was also associated with an improved AFS in patients with antiplatelet medication (HR, 0.64; 95% CI, 0.41-0.99; P = .049) and without antiplatelet medication (HR, 0.26; 95% CI, 0.12-0.57; P = .001) and after both endovascular therapy (HR, 0.51; 95% CI, 0.34-0.76; P = .001) and bypass revascularization (HR, 0.38; 95% CI, 0.21-0.68; P = .001).Statin therapy in CLI patients is associated with an increased AFS and lower rates of mortality and MACCEs without improving, however, the salvage rates of the affected limb.

Published

2017

45. Pyknotic cell death induced byClostridium difficile TcdB: chromatin condensation and nuclear blister are induced independently of the glucosyltransferase activity

Author

Alexandra Olling, Sangar Srivaratharajan, Harald Genth, Ralf Gerhard, Helma Tatge, Katharina Wohlan, and Sebastian Goy

Subjects

Programmed cell death, NADPH oxidase, biology, Immunology, Cell, Bafilomycin, Microbiology, Molecular biology, chemistry.chemical_compound, medicine.anatomical_structure, chemistry, Biochemistry, Apoptosis, Virology, biology.protein, medicine, Glucosyltransferase, Pyknosis, Intracellular

Abstract

Summary TcdA and TcdB are the main pathogenicity factors of Clostridium difficile-associated diseases. Both toxins inhibit Rho GTPases, and consequently, apoptosis is induced in the affected cells. We found that TcdB at higher concentrations exhibits cytotoxic effects that are independent on Rho glucosylation. TcdB and the glucosyltransferase-deficient mutant TcdB D286/288N induced pyknotic cell death which was associated with chromatin condensation and reduced H3 phosphorylation. Affected cells showed ballooning of the nuclear envelope and loss of the integrity of the plasma membrane. Furthermore, pyknotic cells were positively stained with dihydroethidium indicating production of reactive oxygen species. In line with this, pyknosis was reduced by apocynin, an inhibitor of the NADPH oxidase. Bafilomycin A1 prevented cytotoxic effects showing that the newly observed pyknosis depends on intracellular action of TcdB rather than on a receptor-mediated effect. Blister formation and chromatin condensation was specifically induced by the glucosyltransferase domain of TcdB from strain VPI10473 since neither TcdBF from cdi1470 nor the chimera of TcdB harbouring the glucosyltransferase domain of TcdBF was able to induce these effects. In summary, TcdB induces two different and independent phenotypes: (i) cell rounding due to glucosylation of Rho GTPases and (ii) shrinkage of cells and nuclear blister induced by the high concentrations of TcdB independent of Rho glucosylation.

Published

2014

46. The Combined Repetitive Oligopeptides of Clostridium difficile Toxin A Counteract Premature Cleavage of the Glucosyl-Transferase Domain by Stabilizing Protein Conformation

Author

Sebastian Goy, Corinna Hüls, Alexandra Olling, Isa Rudolf, Ralf Gerhard, Simon Krooss, Helma Tatge, and Mirco Müller

Subjects

Cell Survival, Health, Toxicology and Mutagenesis, Bacterial Toxins, Clostridium difficile toxin A, lcsh:Medicine, Toxicology, Cleavage (embryo), medicine.disease_cause, Article, Clostridium difficile toxin, Enterotoxins, Mice, Protein structure, Bacterial Proteins, domain interaction, autoprocessing, cytotoxicity, microscale thermophoresis, medicine, Animals, Oligopeptide, biology, Microscale thermophoresis, Toxin, lcsh:R, 3T3 Cells, Cysteine protease, Protein Structure, Tertiary, Biochemistry, Glucosyltransferases, biology.protein, Glucosyltransferase, Oligopeptides

Abstract

Toxin A (TcdA) and B (TcdB) from Clostridium difficile enter host cells by receptor-mediated endocytosis. A prerequisite for proper toxin action is the intracellular release of the glucosyltransferase domain by an inherent cysteine protease, which is allosterically activated by inositol hexaphosphate (IP6). We found that in in vitro assays, the C-terminally-truncated TcdA1–1065 was more efficient at IP6-induced cleavage compared with full-length TcdA. We hypothesized that the C-terminally-located combined repetitive oligopeptides (CROPs) interact with the N-terminal part of the toxin, thereby preventing autoproteolysis. Glutathione-S-transferase (GST) pull-down assays and microscale thermophoresis confirmed binding between the CROPs and the glucosyltransferase (TcdA1–542) or intermediate (TcdA1102–1847) domain of TcdA, respectively. This interaction between the N- and C-terminus was not found for TcdB. Functional assays revealed that TcdB was more susceptible to inactivation by extracellular IP6-induced cleavage. In vitro autoprocessing and inactivation of TcdA, however, significantly increased, either by acidification of the surrounding milieu or following exchange of its CROP domain by the homologous CROP domain of TcdB. Thus, TcdA CROPs contribute to the stabilization and protection of toxin conformation in addition to function as the main receptor binding domain.

Published

2014

47. Outcomes of dialysis patients with critical limb ischemia after revascularization compared with patients with normal renal function

Author

Meyer, Alexander, primary, Fiessler, Cornelia, additional, Stavroulakis, Konstantinos, additional, Torsello, Giovanni, additional, Bisdas, Theodosios, additional, Lang, Werner, additional, Adili, Farzin, additional, Balzer, Kai, additional, Billing, Arend, additional, Böckler, Dittmar, additional, Brixner, Daniel, additional, Debus, Sebastian E., additional, Donas, Konstantinos P., additional, Eckstein, Hans-Henning, additional, Florek, Hans-Joachim, additional, Gkremoutis, Asimakis, additional, Grundmann, Reinhardt, additional, Hupp, Thomas, additional, Keck, Tobias, additional, Gerß, Joachim, additional, Wojciech, Klonek, additional, May, Björn, additional, Mühling, Bernhard, additional, Oberhuber, Alexander, additional, Reinecke, Holger, additional, Reinhold, Christian, additional, Ritter, Ralf-Gerhard, additional, Schelzig, Hubert, additional, Schlensack, Christian, additional, Schmitz-Rixen, Thomas, additional, Schulte, Karl-Ludwig, additional, Spohn, Mathias, additional, Steinbauer, Markus, additional, Storck, Martin, additional, Trede, Matthias, additional, Uhl, Christian, additional, Weis-Müller, Barbara, additional, Wenk, Heiner, additional, Zeller, Thomas, additional, and Zimmermann, Alexander, additional

Published

2018

48. One-Year Results of First-Line Treatment Strategies in Patients With Critical Limb Ischemia (CRITISCH Registry)

Author

Stavroulakis, Konstantinos, primary, Borowski, Matthias, additional, Torsello, Giovanni, additional, Bisdas, Theodosios, additional, Adili, Farzin, additional, Balzer, Kai, additional, Billing, Arend, additional, Böckler, Dittmar, additional, Brixner, Daniel, additional, Debus, E. Sebastian, additional, Eckstein, Hans-Henning, additional, Florek, Hans-Joachim, additional, Gkremoutis, Asimakis, additional, Grundmann, Reinhardt, additional, Hupp, Thomas, additional, Keck, Tobias, additional, Gerß, Joachim, additional, Wojciech, Klonek, additional, Lang, Werner, additional, May, Björn, additional, Meyer, Alexander, additional, Mühling, Bernhard, additional, Oberhuber, Alexander, additional, Reinecke, Holger, additional, Reinhold, Christian, additional, Ritter, Ralf-Gerhard, additional, Schelzig, Hubert, additional, Schlensack, Christian, additional, Schmitz-Rixen, Thomas, additional, Schulte, Karl-Ludwig, additional, Spohn, Matthias, additional, Steinbauer, Markus, additional, Storck, Martin, additional, Trede, Matthias, additional, Uhl, Christian, additional, Weis-Müller, Barbara, additional, Wenk, Heiner, additional, Zeller, Thomas, additional, Zhorzel, Sven, additional, and Zimmermann, Alexander, additional

Published

2018

49. Human mast cell line-1 (HMC-1) cells exhibit a membrane capacitance increase when dialysed with high free-Ca2+ and GTPγS containing intracellular solution

Author

Dorothea Lorenz, Florian Wegner, Hans Bigalke, Andrea Balletta, Ralf Gerhard, and Andreas Rummel

Subjects

Cell type, GTP', Interleukin-1beta, Cell, Biology, Electric Capacitance, Cell Degranulation, Cell Line, Renal Dialysis, medicine, Humans, Mast Cells, Calcimycin, Pharmacology, Cell Membrane, Interleukin-8, Degranulation, Bridged Bicyclo Compounds, Heterocyclic, Mast cell, Cell biology, medicine.anatomical_structure, Guanosine 5'-O-(3-Thiotriphosphate), Cell culture, Tetradecanoylphorbol Acetate, Thiazolidines, Calcium, Secretagogue, Intracellular

Abstract

An increase in cytosolic free calcium concentration [Ca2+]i initiates the exocytotic activity in various types of secretory cells. The guanosine 5′-O-[3-thio]triphosphate (GTPγS), a non-hydrolysable analogue of GTP (guanosine 5′-triphosphate), is an effective secretagogue for different cell types of different species, like mast cells, neutrophils or eosinophils. Consequently, the internal administration of GTPγS causes degranulation of mouse and rat mast cells. Regarding rat mast cells, it is proved that Ca2+ can cooperate with GTP or GTPγS in accelerating and increasing amplitude of the secretory response. All the previous studies with respect to capacitance recordings and mast cells were performed using mouse or rat mast cells, usually derived from peritoneum or the rat basophilic leukaemia cell line RBL. In this study, we applied the capacitance measurement technique to the human mast cell line-1 (HMC-1) cells, an immature cell line established from a patient with mast cell leukaemia. Patch-clamp dialysis experiments revealed that high intracellular free Ca2+ and GTPγS concentrations are both required for considerable capacitance increases in HMC-1 cells. During degranulation of HMC-1 cells, the total membrane capacitance (Cm) increase appeared continuously and, in some cases, as a discrete capacitance change, developing in a stepwise manner. Then, we tested the effect of latrunculin B upon HMC-1 cell capacitance increase as well as of some classic mast cell stimulators like PMA, A23187 and IL-1β in hexosaminidase release. Finally, we could conclude that the HMC-1 cell line represents a suitable model for the study of human mast cell degranulation.

Published

2013

50. Substrate Specificity of Clostridial Glucosylating Toxins and Their Function on Colonocytes Analyzed by Proteomics Techniques

Author

Ralf Gerhard, Andreas Pich, Johannes Zeiser, and Ingo Just

Subjects

Proteomics, rho GTP-Binding Proteins, Glycosylation, RHOA, Bacterial Toxins, Clostridium difficile toxin A, Virulence, Clostridium difficile toxin B, Biology, Biochemistry, Substrate Specificity, Enterotoxins, Bacterial Proteins, Tandem Mass Spectrometry, Stable isotope labeling by amino acids in cell culture, Humans, Clostridioides difficile, Proteins, rap1 GTP-Binding Proteins, General Chemistry, Molecular biology, rap GTP-Binding Proteins, rhoC GTP-Binding Protein, Host-Pathogen Interactions, Proteome, biology.protein, Caco-2 Cells, RhoG, rhoA GTP-Binding Protein

Abstract

Clostridium difficile is the major cause of intestinal infections in hospitals. The major virulence factors are toxin A (TcdA) and toxin B (TcdB), which belong to the group of clostridial glucosylating toxins (CGT) that inactivate small GTPases. After a 24 h incubation period with TcdA or a glucosyltransferase-deficient mutant TcdA (gdTcdA), quantitative changes in the proteome of colonic cells (Caco-2) were analyzed using high-resolution LC-MS/MS and the SILAC technique. The changes in abundance of more than 5100 proteins were quantified. Nearly 800 toxin-responsive proteins were identified that were involved in cell cycle, cell structure, and adhesion as well as metabolic processes. Several proteins localized to mitochondria or involved in lipid metabolism were consistently of higher abundance after TcdA treatment. All changes of protein abundance depended on the glucosyltransferase activity of TcdA. Glucosylation of the known targets of TcdA such as RhoA, RhoC, RhoG was detected by LC-MS/MS. In addition, an almost complete glucosylation of Rap1(A/B), Rap2(A/B/C) and a partial glucosylation of Ral(A/B) and (H/K/N)Ras were detected. The glucosylation pattern of TcdA was compared to that of other CGT like TcdB, the variant TcdB from C. difficile strain VPI 1470 (TcdBF), and lethal toxin from C. sordellii (TcsL).

Published

2013