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Isoflavone metabolites and their in vitro dual functions: They can act as an estrogenic agonist or antagonist depending on the estrogen concentration

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Abstract
The major soy isoflavones are daidzin and genistin, the glycoside conjugates of daidzein (DZ) and genistein (GTN). After ingestion, they are metabolized into diverse compounds in the gut. The marked inter-individual variation has been suggested in their metabolism. The clinical effects may be modulated by the metabolic ability to produce a more potent metabolite than the precursor. Our study was, therefore, designed to analyze and compare in vitro biologic activities of their metabolites: DZ, GTN, dihydrogenistein (DGTN), dihydrodaidzein (DDZ), tetrahydrodaidzein (TDZ), O-desmethylangolensin (ODMA), and equol (EQL). Furthermore, we investigated their modulatory effects in the presence of estrogen using several in vitro systems. The intermediate metabolites, such as DGTN, DDZ, and TDZ, bind much weakly to both ERs and induce less potently in transcriptional activity, gene expression, and mammary cell proliferation than their precursors. EQL has the strongest binding affinities and estrogenic activities especially for ER beta among the daidzin metabolites and shows the ability to suppress osteoclast formation at high doses. The test isoflavonoids act like estrogen antagonists with the premenopausal dose of E-2 and thus inhibit estrogenic actions by E-2, whereas they exert estrogen agonist activity with the lower dose of estrogen close to the serum levels of postmenopausal women. Our results suggest that phytoestrogens such as isoflavones may exert their effects as estrogen antagonists in a high estrogen environment, or they may act as estrogen agonists in a low estrogen environment. (c) 2006 Elsevier Ltd. All rights reserved.
Author(s)
Hwang, Chang SunKwak, Ho SeokLim, Hwa JaeLee, Su HeeKang, Young SoonChoe, Tae BooHur, Hor-GilHan, Ki Ok
Issued Date
2006-11
Type
Article
DOI
10.1016/j.jsbmb.2006.06.020
URI
https://scholar.gist.ac.kr/handle/local/17803
Publisher
Pergamon Press Ltd.
Citation
Journal of Steroid Biochemistry and Molecular Biology, v.101, no.4-5, pp.246 - 253
ISSN
0960-0760
Appears in Collections:
Department of Environment and Energy Engineering > 1. Journal Articles
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