Binding of intraluminal toxin in cholera: trial of GM1 ganglioside charcoal

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dc.contributor.authorStoll, Barbara J.-
dc.contributor.authorHolmgren, Jan-
dc.contributor.authorBardhan, P.K.-
dc.contributor.authorHuq, Imdadul-
dc.contributor.authorGreenough, William B. III-
dc.contributor.authorFredman, Pam-
dc.contributor.authorSvennerholm, Lars-
dc.date.accessioned2008-01-13T03:29:54Z-
dc.date.available2008-01-13T03:29:54Z-
dc.date.issued1980-10-
dc.identifier.citationLancet 1980 Oct 25;2(8200):888-91-
dc.identifier.urihttp://hdl.handle.net/123456789/589-
dc.description.abstractA study was undertaken to investigate whether toxin produced in the gut lumen contributes significantly to clinical illness and whether binding such toxin by GM1 ganglioside adsorbed onto charcoal could alter the clinical course of disease. 46 patients with severe cholera receiving standard intravenous therapy were randomly assigned to one of three groups: GM1 ganglioside-charcoal (16), charcoal alone (16), or water (14). The results demonstrated that patients were given sufficient GM1 ganglioside-charcoal to bind all luminal toxin produced by Vibrio cholerae in their intestines. Patients treated with GM1 ganglioside tended to have a greater reduction in purging than patients treated with either charcoal alone or water. This difference was statistically significant soon after beginning medication (8-15 h) and the reduction in fluid-loss was especially pronounced in patients with very severe initial purging who had been ill only for a short time before admission. These results suggest that toxin produced in the gut lumen increases fluid-loss early in cholera, but that later in the course of disease, toxin which is inaccessible to luminal binding agents in the major stimulus of purgingen
dc.format.extent316117 bytes-
dc.format.mimetypeapplication/pdf-
dc.language.isoenen
dc.subjectCholeraen
dc.subjectCholera toxinen
dc.subjectG(M1) gangliosideen
dc.subjectVibrio choleraeen
dc.subjectVibrio cholerae-therapyen
dc.subjectBangladeshen
dc.titleBinding of intraluminal toxin in cholera: trial of GM1 ganglioside charcoalen
dc.typeArticleen
Appears in Collections:A. Original papers

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