4.7 Article

Anti-obesity action of Salix matsudana leaves (Part 2).: Isolation of anti-obesity effectors from Polyphenol fractions of Salix matsudana

Journal

PHYTOTHERAPY RESEARCH
Volume 17, Issue 10, Pages 1195-1198

Publisher

WILEY
DOI: 10.1002/ptr.1405

Keywords

Salix matsudana; alpha-amylase activity; brush border membrane vesicles; flavonoids

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Previously, it was reported that polyphenol fractions prepared from the leaves of Salix matsudana reduced the elevation of the rat plasma triacylglycerol level at 3 and 4 h after oral administration of a lipid emulsion containing corn oil, at a dose of 570 mg/kg. Moreover, body weights at 2-9 weeks and the final parametrial adipose tissue weights were significantly lower in mice fed the high-fat diet with 5% polyphenol fractions of S. matsudana leaves than in those fed the high-fat diet alone. The polyphenol fractions of S. matsudana leaves also significantly reduced the hepatic total cholesterol content, which was elevated in mice fed the high-fat diet alone. In addition, the polyphenol fractions of S. matsudana leaves inhibited palmitic acid uptake into brush border membrane vesicles prepared from rat jejunum and alpha-amylase activity, and their fractions enhanced norepinephrine-induced lipolysis in fat cells. To clarify the active substances inhibiting the palmitic acid uptake into small intestinal brush border membrane, the alpha-amylase activity or enhancing the norepinephrine-induced lipolyis in fat cells, the isolation of the active substances from polyphenol fraction was attempted using the above three assay systems. Compounds 1, 2 and 3 were isolated from the polyphenol fractions and identified as apigenin-7-O-D-glucoside, luteolin-7-O-D-glucoside and chrysoeriol-7-O-D-glucoside, respectively. Among three flavonoids, apigenin-7-O-D-glucoside inhibited a-amylase activity, and luteolin-7-O-D-glucoside and chnysoeriol-7-O-D-glucoside inhibited palmitic acid uptake into small intestinal brush border membrane. Furthermore, three flavonoid glucosides enhanced norepinephrine-induced lipolysis in fat cells. Copyright (C) 2003 John Wiley Sons, Ltd.

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