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Effect of selenium and vitamin E supplements on tissue lipids, peroxides, and fatty acid distribution in experimental diabetes
Authors:C. Douillet  M. Bost  M. Accominotti  F. Borson-Chazot  M. Ciavatti
Affiliation:(1) National Institute of Health and Medical Research Unit 331, 22 av. du Doyen Lépine, 69675 Bron Cedex, France;(2) Trace Element Insitute for UNESCO, 69007 Lyon, France;(3) Department of Pharmacological Biochemistry, Edouard Herriot Hospital, 69008 Lyon, France;(4) Department of Endocrinology Antiquaille, Claude Bernard University, 69008 Lyon, France
Abstract:The protective role of selenium (Se), given as a Se-rich yeast, selenomethionine or selenomethionine+vitamin E supplement, toward changes in lipid, peroxide, and fatty acid distribution in tissues of streptozotocin-induced diabetic rats, was investigated, after 24 wk of disease. Diabetes increased liver thiobarbituric acid-reactive substances and conjugated dienes; Se supplement completely corrected these changes. In kidney, as in heart, the peroxide levels were not significantly changed by diabetes. In diabetic rat liver, a significant drop in triglycerides and phospholipids (P<0.05) was observed; this was modulated by Se+vitamin F supplementation. Se+vitamin E supplementation also inhibited the decrease in 18∶2n-6 and the increase in 22∶6n-3 observed in liver of diabetic rats, changes which reflect altered glycemic control. In kidney, heart, and aorta, diabetes produced some changes in lipid content and fatty acid distribution, especially an increase in heart triglycerides which was also corrected by the Se supplement. Se supplementation to diabetic rats also increased 18∶0 etherlinked alcohol, 20∶4 n-6, and 22∶5 n-3 in cardiac lipids. In aorta, Se + vitamin E significanlty increased 20∶5 n-3. These polyunsaturated fatty acids are precursors, in situ, of prostaglandin l2 (PGl2) and PGl3 which may protect against cardiovascular dysfunction. In kidney, converrely, Se decreased 20∶4 n-6, the precursor of thromboxane A1 implicated in diabetic glomerular injury. thus Se, and more efficiently Se + vitamin E supplementation, in experimental diabetes could play a role in controlling oxidative status and altered lipid metabolism in liver, thereby maintaining favorable fatty acid distribution in the major tissues affected by diabetic complications.
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