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扁果红豆草中异黄酮类化合物的雌激素活性。

Estrogenic activity of isoflavonoids from Onobrychis ebenoides.

作者信息

Halabalaki Maria, Alexi Xanthippi, Aligiannis Nektarios, Lambrinidis George, Pratsinis Harris, Florentin Ida, Mitakou Sofia, Mikros Emmanuel, Skaltsounis Alexios-Leandros, Alexis Michael N

机构信息

Division of Pharmacognosy and Natural Products Chemistry, School of Pharmacy, University of Athens, Athens, Greece.

出版信息

Planta Med. 2006 May;72(6):488-93. doi: 10.1055/s-2005-916261.

DOI:10.1055/s-2005-916261
PMID:16773531
Abstract

Fractionation of the neutral extract of Onobrychis ebenoides (Leguminosae) yielded a new isoflavone, named ebenosin (1), in addition to the known ones, afrormosin (2), formononetin (3) and daidzein (4). Although the relative binding affinities of 1 - 4 for estrogen receptor alpha (ERalpha) were nearly comparable and matched those of 1-3 for ERbeta, that of 4 for the latter receptor was significantly higher than any of the other. Compounds 1 - 4 induced cell proliferation and gene expression in breast and endometrial cancer cells in an ER-dependent manner. Nonetheless, the rank order of induction potencies ( 4 > 3 >or= 2 >or= 1) matched better that of affinities for ERbeta ( 4 > 3 >or= 2 >or= 1) rather than ERalpha ( 4 >or= 3 >or= 2 >or= 1). While the antiestrogen ICI 182,780 could inhibit the induction of proliferation of ER-positive breast cancer cells by 1-4, it could not prevent 1 from exhibiting significant ER-independent cytotoxicity at 10 microM. By contrast, 1 was much less cytotoxic and only weakly estrogenic for ER-positive endometrial adenocarcinoma cells. In conclusion, our data suggest that the C-8 isoprenyl substituent of 1 renders it cytotoxic and/or estrogenic in a cell-dependent manner.

摘要

对红豆草(豆科)中性提取物进行分级分离,除了已知的异黄酮阿夫罗摩辛(2)、芒柄花黄素(3)和大豆苷元(4)外,还得到了一种新的异黄酮,命名为红豆草素(1)。虽然化合物1 - 4对雌激素受体α(ERα)的相对结合亲和力几乎相当,且与它们对雌激素受体β(ERβ)的亲和力相匹配,但化合物4对后者受体的亲和力明显高于其他任何一种。化合物1 - 4以雌激素受体依赖的方式诱导乳腺癌和子宫内膜癌细胞的增殖和基因表达。尽管如此,诱导效力的排序(4 > 3 ≥ 2 ≥ 1)与对ERβ的亲和力排序(4 > 3 ≥ 2 ≥ 1)的匹配度比对ERα的亲和力排序(4 ≥ 3 ≥ 2 ≥ 1)更好。抗雌激素ICI 182,780可以抑制1 - 4对雌激素受体阳性乳腺癌细胞增殖的诱导作用,但在10微摩尔浓度下,它无法阻止化合物1表现出显著的非雌激素受体依赖性细胞毒性。相比之下,化合物1对雌激素受体阳性子宫内膜腺癌细胞的细胞毒性要小得多,且雌激素活性也较弱。总之,我们的数据表明,化合物1的C - 8异戊烯基取代基使其在细胞依赖的方式下具有细胞毒性和/或雌激素活性。

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