Identification of
            <i>Clostridium difficile</i>
            toxin B cardiotoxicity using a zebrafish embryo model of intoxication

Hamm, Elaine E.; Voth, Daniel E.; Ballard, Jimmy D.

doi:10.1073/pnas.0604725103

Cited by 71 publications

(63 citation statements)

References 54 publications

Supporting

Mentioning

Contrasting

Order By: Relevance

“…This finding drew into question the long-standing hypothesis that TcdA was actually more important in the pathogenesis of disease, but was in agreement with other recent work highlighting the importance of TcdB. 1,2,7 Our work also confirmed that systemically administered antibodies were detectable not only in the blood, as expected, but were also detectable in the intestinal lumen.…”

Section: Introductionsupporting

confidence: 76%

The roles of toxin A and toxin B inClostridium difficileinfection

2013

View full text Add to dashboard Cite

Section: Introductionsupporting

confidence: 76%

The roles of toxin A and toxin B inClostridium difficileinfection

2013

View full text Add to dashboard Cite

“…Furthermore, since toxins can induce their own transport to the basolateral/ systemic side ( Fig. 6 and reference 30), perhaps allowing them to enter the circulation and reach other organs (39,40), circulating neutralizing antibodies should prevent systemic effects, if any, of C. difficile toxins. Whether these advantages will translate to systemically administered antibodies, such as actoxumab-bezlotoxumab, versus orally delivered neutralizing antibodies remains to be confirmed.…”

Section: Discussionmentioning

confidence: 99%

Toxin-Mediated Paracellular Transport of Antitoxin Antibodies Facilitates Protection against Clostridium difficile Infection

et al. 2015

View full text Add to dashboard Cite

bThe exotoxins TcdA and TcdB are the major virulence factors of Clostridium difficile. Circulating neutralizing antitoxin antibodies are protective in C. difficile infection (CDI), as demonstrated, in part, by the protective effects of actoxumab and bezlotoxumab, which bind to and neutralize TcdA and TcdB, respectively. The question of how systemic IgG antibodies neutralize toxins in the gut lumen remains unresolved, although it has been suggested that the Fc receptor FcRn may be involved in active antibody transport across the gut epithelium. In this study, we demonstrated that genetic ablation of FcRn and excess irrelevant human IgG have no impact on actoxumab-bezlotoxumab-mediated protection in murine and hamster models of CDI, suggesting that Fc-dependent transport of antibodies across the gut wall is not required for efficacy. Tissue distribution studies in hamsters suggest, rather, that the transport of antibodies depends on toxin-induced damage to the gut lining. In an in vitro two-dimensional culture system that mimics the architecture of the intestinal mucosal epithelium, toxins on the apical side of epithelial cell monolayers are neutralized by basolateral antibodies, and antibody transport across the cell layer is dramatically increased upon addition of toxin to the apical side. Similar data were obtained with F(ab=) 2 fragments, which lack an Fc domain, consistent with FcRn-independent paracellular, rather than transcellular, transport of antibodies. Kinetic studies show that initial damage caused by apical toxin is required for efficient neutralization by basolateral antibodies. These data may represent a general mechanism of humoral response-mediated protection against enteric pathogens.

show abstract

“…However, systemic toxin is not indicative of a normal infection scenario, since the majority of clinical manifestations of CDAD are selflimiting within the intestine (51). In life-threatening cases, however, systemic complications have been documented (52)(53)(54)(55)(56), and entry of the toxin into circulation is thought to be a possible cause (57). Therefore, challenging immunized mice with intraperitoneal toxin represents a stringent method for assaying the nAb response.…”

Section: Discussionmentioning

confidence: 99%

An Optimized, Synthetic DNA Vaccine Encoding the Toxin A and Toxin B Receptor Binding Domains of Clostridium difficile Induces Protective Antibody ResponsesIn Vivo

et al. 2014

View full text Add to dashboard Cite

h Clostridium difficile-associated disease (CDAD) constitutes a large majority of nosocomial diarrhea cases in industrialized nations and is mediated by the effects of two secreted toxins, toxin A (TcdA) and toxin B (TcdB). Patients who develop strong antitoxin antibody responses can clear C. difficile infection and remain disease free. Key toxin-neutralizing epitopes have been found within the carboxy-terminal receptor binding domains (RBDs) of TcdA and TcdB, which has generated interest in developing the RBD as a viable vaccine target. While numerous platforms have been studied, very little data describes the potential of DNA vaccination against CDAD. Therefore, we created highly optimized plasmids encoding the RBDs from TcdA and TcdB in which any putative N-linked glycosylation sites were altered. Mice and nonhuman primates were immunized intramuscularly, followed by in vivo electroporation, and in these animal models, vaccination induced significant levels of both anti-RBD antibodies (blood and stool) and RBD-specific antibody-secreting cells. Further characterization revealed that sera from immunized mice and nonhuman primates could detect RBD protein from transfected cells, as well as neutralize purified toxins in an in vitro cytotoxicity assay. Mice that were immunized with plasmids or given nonhuman-primate sera were protected from a lethal challenge with purified TcdA and/or TcdB. Moreover, immunized mice were significantly protected when challenged with C. difficile spores from homologous (VPI 10463) and heterologous, epidemic (UK1) strains. These data demonstrate the robust immunogenicity and efficacy of a TcdA/B RBD-based DNA vaccine in preclinical models of acute toxin-associated and intragastric, sporeinduced colonic disease.

show abstract

Identification of Clostridium difficile toxin B cardiotoxicity using a zebrafish embryo model of intoxication

Cited by 71 publications

References 54 publications

The roles of toxin A and toxin B inClostridium difficileinfection

The roles of toxin A and toxin B inClostridium difficileinfection

Toxin-Mediated Paracellular Transport of Antitoxin Antibodies Facilitates Protection against Clostridium difficile Infection

An Optimized, Synthetic DNA Vaccine Encoding the Toxin A and Toxin B Receptor Binding Domains of Clostridium difficile Induces Protective Antibody ResponsesIn Vivo

Contact Info

Product

Resources

About