Binding of Clostridium botulinum Type C and D Neurotoxins to Ganglioside and Phospholipid

Tsukamoto, Kentaro; Kohda, Tomoko; Mukamoto, Masafumi; Takeuchi, Kumiko; Ihara, Hideshi; Saito, Masaki; Kozaki, Shunji

doi:10.1074/jbc.m507596200

Cited by 121 publications

(124 citation statements)

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“…Montecucco and colleagues (24) proposed that BoNTs bind neurons through coreceptor interactions. Recent studies have implicated gangliosides as the coreceptor for the BoNTs, except for BoNT/D, which appears to utilize another class of small molecules as the coreceptor (35). To address the molecular basis for the neutralizing capacity of HCR immunization, a solid-phase assay was developed.…”

Section: Resultsmentioning

confidence: 99%

Subunit Vaccine against the Seven Serotypes of Botulism

et al. 2008

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Section: Resultsmentioning

confidence: 99%

Subunit Vaccine against the Seven Serotypes of Botulism

et al. 2008

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“…injection into SD rats (female, 8 weeks old, approximately 200 g; Japan SLC, Inc., Shizuoka, Japan), and ddY and C57BL/6J mice (male, 4 weeks old, approximately 20 g; Japan SLC, Inc.) to obtain the mean 50% lethal dose (LD 50 ) by the Reed and Muench calculation (29). The toxicity of BoNT/DC to GM3 synthasedeficient (knockout) mice (42) was assayed by the intravenous injection method (21). The Ethics Committee of the Graduate School of Life and Environmental Sciences, Osaka Prefecture University, approved all animal tests.…”

Section: Methodsmentioning

confidence: 99%

“…Cerebellar granule neurons from 8-day-old C57BL/6J mice and SD rats were prepared according to a previously reported method (42). The cells were plated on polyethylenimine-coated 4-well culture dishes (Nalge Nunc, Rochester, NY) at a density of 2.6 ϫ 10 5 cells/cm 2 in HK-MEM (minimal essential medium containing 25 mM K ϩ , 10 mM glucose, 30 nM Na 2 SeO 4 , 80 g/ml gentamicin, pH 7.4) with 5% horse serum and 5% fetal calf serum and maintained overnight at 37°C in 5% CO 2 .…”

Section: Methodsmentioning

confidence: 99%

“…August 2012 Volume 80 Number 8 iai.asm.org 2887 periments were performed as described previously (42). The Glu content was determined using a high-performance liquid chromatography (HPLC)-electron capture detector (HTEC-500; Eicom, Kyoto, Japan), which consists of a GU-GEL matrix separation column, a Glu oxidaseimmobilized column, and a platinum electrode for electrochemical detection.…”

Section: Toxicity Of Botulinum D/c Mosaic Toxin In Rodentsmentioning

confidence: 99%

“…Synaptic vesicle glycoprotein SV2C and synaptotagmin I or II are considered to be the protein receptors for BoNT/A and B, respectively (8,23). Meanwhile, for BoNT/C, gangliosides GD1b and GT1b have been identified as binding components (42). Although BoNT/D lacks the SXWY ganglioside-binding motif that is present in other BoNT serotypes, it has recently been reported that the toxin binds to b-series gangliosides (14).…”

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Unique Biological Activity of Botulinum D/C Mosaic Neurotoxin in Murine Species

et al. 2012

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cClostridium botulinum types C and D cause animal botulism by the production of serotype-specific or mosaic botulinum neurotoxin (BoNT). The D/C mosaic BoNT (BoNT/DC), which is produced by the isolate from bovine botulism in Japan, exhibits the highest toxicity to mice among all BoNTs. In contrast, rats appeared to be very resistant to BoNT/DC in type C and D BoNTs and their mosaic BoNTs. We attempted to characterize the enzymatic and receptor-binding activities of BoNT/DC by comparison with those of type C and D BoNTs (BoNT/C and BoNT/D). BoNT/DC and D showed similar toxic effects on cerebellar granule cells (CGCs) derived from the mouse, but the former showed less toxicity to rat CGCs. In recombinant murine-derived vesicleassociated membrane protein (VAMP), the enzymatic activities of both BoNTs to rat isoform 1 VAMP (VAMP1) were lower than those to the other VAMP homologues. We then examined the physiological significance of gangliosides as the binding components for types C and D, and mosaic BoNTs. BoNT/DC and C were found to cleave an intracellular substrate of PC12 cells upon the exogenous addition of GM1a and GT1b gangliosides, respectively, suggesting that each BoNT recognizes a different ganglioside moiety. The effect of BoNT/DC on glutamate release from CGCs was prevented by cholera toxin B-subunit (CTB) but not by a site-directed mutant of CTB that did not bind to GM1a. Bovine adrenal chromaffin cells appeared to be more sensitive to BoNT/DC than to BoNT/C and D. These results suggest that a unique mechanism of receptor binding of BoNT/DC may differentially regulate its biological activities in animals.

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Botulism

Lonati

Rossetto

Fenicia

et al. 2009

General, Applied and Systems Toxicology

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Botulism is a paralytic illness caused by botulinum neurotoxins (BoNTs) produced by three clostridium species ( Clostridium botulinum, Clostridium butyricum and Clostridium baratii ). Seven immunological BoNTs, (A–G) have been recognized. Human botulism has been mainly caused by type‐A, B, E and rarely by F neurotoxins. BoNT is a simple dichain polypeptide that consists of a 100 kDa ‘heavy’ chain joined by a single disulfide bond to a 50 kDa ‘light’ chain. The toxin's light chain is a Zn 2+ ‐containing endopeptidase that blocks acetylcholine‐containing vesicles from fusing with the terminal membrane of the peripheral cholinergic terminals, resulting in flaccid muscle paralysis and alteration of autonomic functions. Three common and naturally occurring botulism types have been identified: foodborne, wound and intestinal botulism (including infant and adult forms). Two other forms are man‐made: inhalation botulism could result from aerosolization of BoNTs from laboratory accidents or deliberate dissemination, whereas iatrogenic botulism is related to incorrect usage of injected BoNTs for cosmetic or therapeutic purposes. The clinical syndrome is characterized by symmetrical cranial nerve palsies followed by a descending, symmetrical, flaccid paralysis that may progress to respiratory compromise and death. The diagnosis is essentially clinical and can be confirmed by the detection of BoNTs in human or in food samples; in the infant and intestinal forms, BoNTs‐producing Clostridia can be isolated from stools. Current management is based on supportive treatment (including respiratory support in severe cases) and antitoxin administration that, if early practised, may prevent or limit the extent of the paralysis, but will not reverse it.

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Binding of Clostridium botulinum Type C and D Neurotoxins to Ganglioside and Phospholipid

Cited by 121 publications

References 50 publications

Subunit Vaccine against the Seven Serotypes of Botulism

Subunit Vaccine against the Seven Serotypes of Botulism

Unique Biological Activity of Botulinum D/C Mosaic Neurotoxin in Murine Species

Botulism

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