Response of mouse intestinal loop to botulinum C2 toxin: enterotoxic activity induced by cooperation of nonlinked protein components

Ohishi, Iwao

doi:10.1128/iai.40.2.691-695.1983

Cited by 90 publications

(36 citation statements)

References 19 publications

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“…Unlike diphtheria toxin and P. aeruginosa exotoxin, it does not typically cause cell death. The botulinum binary toxin superficially mimics cholera toxin and related substances, because it does promote the movement of fluids across membranes (11,19,20,25), but an action of this toxin on nucleotide-binding proteins has not been reported.…”

Section: Discussionmentioning

confidence: 99%

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Molecular basis for the pathological actions of Clostridium perfringens iota toxin

Simpson¹,

Stiles²,

Zepeda³

et al. 1987

Infect Immun

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Clostridium perfringens type E iota toxin is composed of two separate and independent polypeptide chains that act synergistically in mouse lethal assays. The light chain is an enzyme that mono(ADP-ribosyl)ates certain amino acids. The enzyme displays substantial activity when homopoly-L-arginine is used as a substrate, but it shows little activity when polyasparagine, polylysine or polyglutamic acid are used. In keeping with the properties of an ADP-ribosylating enzyme, the toxin possesses the following characteristics. It produces incorporation of radioactivity into polyarginine when adenine-labeled NAD is used, but radioactivity is not incorporated when nicotinamide-labeled NAD is used. Irrespective of labeling, enzymatic activity is accompanied by the release of free nicotinamide. After incorporation of ADP-ribose groups into polyarginine, enzymatic and chemical techniques can be used to release the incorporated material. Snake venom phosphodiesterase releases mainly AMP; hydroxylamine releases AMP and ADP-ribose. The heavy chain of iota toxin has little or no enzyme activity, and it does not substantially affect the enzyme activity of the light chain. The heavy chain may be a binding component that directs the toxin to vulnerable cells. The data suggest that iota toxin is a representative of a novel class of ADP-ribosylating toxins.

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Section: Discussionmentioning

confidence: 99%

“…Iota toxin appears to share certain properties with the botulinum binary toxin, including the ability to promote the movement of fluids across membranes (5,11,19,20,24). There are also the obvious similarities that both toxins are * Corresponding author.…”

mentioning

confidence: 99%

Molecular basis for the pathological actions of Clostridium perfringens iota toxin

Simpson¹,

Stiles²,

Zepeda³

et al. 1987

Infect Immun

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“…On the other hand, C. botulinum and C. spiroforme have been reported to produce binary toxins (consisting of light and heavy chain components), each of which is similar in molecular weight and action (11,12,14,15). It has been reported that these light chain components ADP-ribosylate synthetic substrates such as homo-poly-L-arginine and actin-like proteins in platelets (12,13), and that the heavy chain component of C. botulinum C2 toxin is responsible for binding of the light chain component to the eucaryotic cells surface (4,(6)(7)(8). On the other hand, little is known about the relationship, between Ia and I, components in lethality and dermonecrosis caused by iota toxin.…”

mentioning

confidence: 99%

Lethal and Dermonecrotic Activities of Clostridium perfringens Iota Toxin: Biological Activities Induced by Cooperation of Two Nonlinked Components

Sakùrai

Kobayashi

1995

Microbiology and Immunology

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The effect of separate injections of two components of Clostridium perfringens iota toxin , designated I. and I, components, on the biological activities of the toxin was investigated . The intravenous injection of one component within 120 min after the injection of the other component killed mice . The activity of iota toxin was abolished by anti-Ia or anti-I, antiserum. On the other hand , when Ib component was intravenously administered to mice given anti-Ia antiserum within 120 min after the intravenous injection of Ia component, the lethal activity was completely neutralized , but when I. component was injected into mice that were given anti-Ib antiserum over 5 min after the injection of Ib component , the activity was not neutralized. The separate injections of I. and Ib components in skin of guinea pigs indicated dermonecrosis at the injection site of I, components, but not at the site of I . components. Furthermore, when one component was intradermally injected in guinea pigs and then the other intraperitoneally, the dermonecrotic activity of the toxin was observed at the intradermal injection site of I, component, but not at that of I. component. From the data, it appears that the lethal and dermonecrotic activities of iota toxin are initiated by the binding of Ib component to specific sites on tissues .

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“…These results indicate that even when the two components of C2T are incubated separately, component I binds to the cell surface bound with T-II and is processed together with T-II during internalization, as was observed with cells exposed simultaneously to both components. Previous studies by indirect immunofluorescence staining have shown that both UT-II and T-II, the binding component of C2T, bind to isolated epithelial cells and to brush borders of mouse intestine, while component I, the active component of the toxin, binds to cells and brush borders only in the presence of T-II (6). In these experiments, these findings were confirmed with two directly fluorescence-labeled components of C2T in tissue culture cells, and the difference in the dynamic processes of components I and II after binding to the cells was visualized.…”

Section: ) This Indicates That Component I Binds To Cells Bound With mentioning

confidence: 96%

“…These two molecules are functionally different proteins: component II is a binding subunit, and component I is an ADP-ribosyltransferase whose substrate is cytoplasmic actin (7,11). The toxin has various biological activities, lethality, enterotoxicity, and cytotoxicity, all of which are activated by trypsinization of a mixture of the two components and elicited by their cooperation (5,6). These activities of C2T are caused by ADPribosylation of cytoplasmic actin by component I (11).…”

mentioning

confidence: 99%

Visualizations of binding and internalization of two nonlinked protein components of botulinum C2 toxin in tissue culture cells

Ohishi

Yanagimoto

1992

Infect Immun

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Binding and internalization of two nonlinked components of botulinum C2 toxin were visualized in tissue culture cells with components directly labeled with fluorescence. The binding of both untrypsinized and trypsinized component II (UT-II and T-II, respectively) to common specific sites on the cell membrane was evidenced by competitive binding between fluorescence-labeled and unlabeled components. The distribution patterns of fluorescence-labeled T-II and UT-II after binding to cells at 37°C were different; T-HI clustered on the cell membrane and entered the cells in endosomes, whereas UT-H entered the cells inefficiently and not in vesicles and was distributed on the nuclear surface. The difference may be due to the multivalent property of

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Response of mouse intestinal loop to botulinum C2 toxin: enterotoxic activity induced by cooperation of nonlinked protein components

Cited by 90 publications

References 19 publications

Molecular basis for the pathological actions of Clostridium perfringens iota toxin

Molecular basis for the pathological actions of Clostridium perfringens iota toxin

Lethal and Dermonecrotic Activities of Clostridium perfringens Iota Toxin: Biological Activities Induced by Cooperation of Two Nonlinked Components

Visualizations of binding and internalization of two nonlinked protein components of botulinum C2 toxin in tissue culture cells

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