Literature DB >> 1140867

The mechanism of carcinogenic action of 1,2-dimethylhydrazine (SDMH) in rats.

K M Pozharisski, Y M Kapustin, A J Likhachev, J D Shaposhnikov.   

Abstract

The radioactivity level in blood, bile, urine and contents of parts of the gastro-intestinal tract in rats was studied after subcutaneous administration of 3-H-1,2-dimethylhydrazine (3-H-SDMH) which induces colonic tumours. The alkylation of DNA, RNA and protein in the intestinal mucosa, liver and kidneys was estimated 1 h to 28 days after 3-H-SDMH treatment from the 3-H-incorporation into these macromolecules. Administration of 3-H-1,2-diethylhydrazine (3-H-SDEH) which does not induce intestinal tumours was made as a control. Fifteen to 30 min after 3-H-SDMH treatment, marked radioactivity was found in blood, bile, urine and in contents of all regions of gastro-intestinal tract. After 3-H-SDMH administration no label occurred in the contents of localized segments of gastro-intestinal tract although it was present in blood, bile and urine. 3-H-SDMH methylated DNA, RNA and proteins of intestinal mucosa, liver and kidney to a high degree. One hour after 3-H-SDMH treatment the incorporation of label into protein of intestinal mucosa was higher than into liver and kidneys. 3-H-SDEH did not alkylate macromolecules in these organs but did so in thymus, spleen and brain, which are target organs for this carcinogen. After total hepatectomy, 3-H-SDMH did not methylate macromolecules of the intestinal mucosa. The following mechanism for the carcinogenic effect of SDMH is suggested. A carcinogenic metabolite of SDMH forms, in the liver, a conjugate with glucuronic acid. This glucuronide enters the gut both with bile and directly via the circulation. Microbial beta-glucuronidase releases the active metabolite which, in turn, alkylates tissue macromolecules.

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Year:  1975        PMID: 1140867     DOI: 10.1002/ijc.2910150417

Source DB:  PubMed          Journal:  Int J Cancer        ISSN: 0020-7136            Impact factor:   7.396


  7 in total

1.  Experimental colonic carcinogenesis: changes in faecal bile acids after promotion of intestinal tumours by small bowel resection in the rat.

Authors:  A P Savage; M S Sian; J L Matthews; S R Bloom; T Cooke
Journal:  Gut       Date:  1988-04       Impact factor: 23.059

Review 2.  Assessment of the mode of action underlying development of rodent small intestinal tumors following oral exposure to hexavalent chromium and relevance to humans.

Authors:  Chad M Thompson; Deborah M Proctor; Mina Suh; Laurie C Haws; Christopher R Kirman; Mark A Harris
Journal:  Crit Rev Toxicol       Date:  2013-03       Impact factor: 5.635

3.  Distribution and carcinogenic action of 1,2-dimethylhydrazine (SDMH) in rats.

Authors:  K M Pozharisski; J D Shaposhnikov; A S Petrov; A J Likhachev
Journal:  Z Krebsforsch Klin Onkol Cancer Res Clin Oncol       Date:  1976-09-24

4.  Increased paracellular permeability of tumor-adjacent areas in 1,2-dimethylhydrazine-induced colon carcinogenesis in rats.

Authors:  Viktoria V Bekusova; Evgeny L Falchuk; Larisa S Okorokova; Natalia M Kruglova; Alexander D Nozdrachev; Alexander G Markov
Journal:  Cancer Biol Med       Date:  2018-08       Impact factor: 4.248

5.  Kinetics of changes in the crypts of the jejunal mucosa of dimethylhydrazine-treated rats.

Authors:  J P Sunter; D R Appleton; N A Wright; A J Watson
Journal:  Br J Cancer       Date:  1978-05       Impact factor: 7.640

6.  Antioxidant and Anticancer Potentials of the Olive and Sesame Mixture against Dimethylhydrazine-Induced Colorectal Cancer in Wistar Rats.

Authors:  Amirhasan Valaei; Fatemeh Azadeh; Seyedeh Talayeh Mostafavi Niaki; Alireza Salehi; Maede Shakib Khoob; Seyed Hesam Odin Mirebrahimi; Sohrab Kazemi; Seyed Mohammad Hosseini
Journal:  Biomed Res Int       Date:  2022-10-10       Impact factor: 3.246

7.  Role of hepatic and intestinal p450 enzymes in the metabolic activation of the colon carcinogen azoxymethane in mice.

Authors:  Vandana Megaraj; Xinxin Ding; Cheng Fang; Nataliia Kovalchuk; Yi Zhu; Qing-Yu Zhang
Journal:  Chem Res Toxicol       Date:  2014-03-05       Impact factor: 3.739

  7 in total

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