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Metabolism of subtoxic level of selenite by double-perfused small intestine in rats
Authors:Yeong-Chul Park  Jong-Bong Kim  Yong Heo  Dong-Cheol Park  In-Sun Lee  Hai-Won Chung  Jung-Ho Han  Woon-Gye Chung  S. C. Vendeland  Philip D. Whanger
Affiliation:(1) Natural Science Institute, Catholic University of Daegu, 330 Kumrak 1-Ri, Hayang-UP, Kyongsan-Si, 710-702 Kyongbuk, Korea;(2) Divison of Food Science, Gimcheon College, 754 Samrak-Dong, Gimcheon City, Gyung-buk, Korea;(3) TMR Center, Keimyung University, Sindang-Dong, Dalseo-Gu, 1000 Daegu, Korea;(4) Medical Research Center, School of Public Health, Seoul National University, 28 Yeonkun-Dong, Seoul, Korea;(5) Department of Pharmacology, School of Medicine, Inha University, Incheon, Korea;(6) Department of Environmental and Molecular Toxicology, Oregon State University, 97330 Corvallis, OR;(7) Present address: 10519 District Line Road, 98233 Burlington, WA
Abstract:Intestinal metabolism of the subtoxic level of selenite in rats was investigated using a double-perfusion system, which is an in situ, in vitro preparation in which the intestinal lumen and its vasculature are perfused simultaneously. The toxicity of sodium selenite was determined by inhibition of 3-O-methyl glucose (3MG) absorption and by histological examination. Levels of 1.2 mM selenite were required to significantly (p<0.05) reduce 3MG intestinal absorption (58+/-11%, mean+/-SD). Cation-exchange chromatography was used to determine the chemical forms of Se from selenite after using luminal concentrations of 1-200 microM in vascular perfusates. The chemical forms were selenite, selenodiglutathione (GS-Se-SG), mixed selenoglutathione plus cysteine (GS-Se-CYS), selenodicysteine (CYS-Se-CYS), protein-bound Se, and unidentified selenocompounds. Selenite was the predominant selenocompound found in vascular perfusate, but protein-bound Se was the predominant metabolite from selenite present in the vascular effluents. There was a corresponding increase of all metabolites with increased levels of selenite with time of absorption, but not with increased concentration of luminal selenite.
Keywords:Selenite  metabolism  intestine  perfusion  selenocompounds
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