Please use this identifier to cite or link to this item: http://nopr.niscair.res.in/handle/123456789/23539
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dc.contributor.authorBiswas, Surjyo Jyoti-
dc.contributor.authorKhuda-Bukhsh, Anisur Rahman-
dc.date.accessioned2013-11-13T08:48:56Z-
dc.date.available2013-11-13T08:48:56Z-
dc.date.issued2004-07-
dc.identifier.issn0975-1009 (Online); 0019-5189 (Print)-
dc.identifier.urihttp://hdl.handle.net/123456789/23539-
dc.description698-714en_US
dc.description.abstractSeveral cytogenetical and enzymatic protocols were used to test if two microdoses of Chelidonium majus, namely Chelidonium-30 (Ch-30) and Chelidonium-200 (Ch-200), used as homeopathic drugs, showed anti-tumor activity and also favorably modulated genotoxic damages produced by an azo dye in mice at several intervals of fixation. Different sets of healthy mice were fed: (i) hepatocarcinogen, p-dimethylaminoazobenzene (p-DAB, initiator) + pl1enobarbital (PB, promoter), (ii) only p-DAB, (iii) only PB, and (iv) neither p-DAB nor PB (normal control). Mice fed with p-DAB + PB were divided into different sets that were also fed either Ch-30 (v) or Ch-200 (vi) or diluted alcohol (vii), the "vehicle" of the microdoses of Chelidonium. All mice of group (i), a few of group (ii) and group (vii) and none of groups (iii) and (iv) developed tumors in liver at the longer intervals of fixation. The frequencies of chromosome aberrations (CA), micronucleated erythrocytes (MN), mitotic index (MI) and sperm head abnormality (SHA) were much higher in groups (i) and (vii) mice than in groups (ii), (iii) and (iv) mice at all fixation intervals. However, in mice of both groups (v) and (vi), the frequencies of CA, MN, SHA were strikingly less than those of groups (i) and (vii), and moderately less than those of groups (ii) and (iii). Both Ch-30 and Ch-200 also modulated favourably some toxicity marker enzymes like acid and alkaline phosphatases, peroxidases, glutamate oxaloacetate and glutamate pyruvate transaminases in liver, kidney and spleen tissues of the carcinogen fed mice. The microdoses of Chelidonium having no visible ill effects of their own, may be strong candidates for use in delaying/ protecting liver cancer.en_US
dc.language.isoen_USen_US
dc.publisherNISCAIR-CSIR, Indiaen_US
dc.relation.ispartofseriesInt Cl7 A61Pen_US
dc.rights CC Attribution-Noncommercial-No Derivative Works 2.5 Indiaen_US
dc.sourceIJEB Vol.42(07) [July 2004]en_US
dc.subjectp-DABen_US
dc.subjectHepatocarcinogenesisen_US
dc.subjectMicrodosesen_US
dc.subjectChelidoniumen_US
dc.subjectGenotoxicityen_US
dc.subjectToxicity marker enzymesen_US
dc.titleEvaluation of protecti ve potentials of a potentized homeopathic drug, Chelidonium majus, during azo dye induced hepatocarcinogenesis in miceen_US
dc.typeArticleen_US
Appears in Collections:IJEB Vol.42(07) [July 2004]

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