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基于异黄酮的保骨治疗对去卵巢大鼠的生殖器官及雌二醇的肝脏代谢作用较弱。

Isoflavonoid-based bone-sparing treatments exert a low activity on reproductive organs and on hepatic metabolism of estradiol in ovariectomized rats.

作者信息

Phrakonkham Pascal, Chevalier Joëlle, Desmetz Catherine, Pinnert Marie-France, Bergès Raymond, Jover Emmanuel, Davicco Marie-Jeanne, Bennetau-Pelissero Catherine, Coxam Véronique, Artur Yves, Canivenc-Lavier Marie-Chantal

机构信息

UMR 1129 FLAVIC, INRA-ENESAD-Université de Bourgogne, F-21000 Dijon, France.

出版信息

Toxicol Appl Pharmacol. 2007 Oct 15;224(2):105-15. doi: 10.1016/j.taap.2007.06.012. Epub 2007 Jun 30.

DOI:10.1016/j.taap.2007.06.012
PMID:17655901
Abstract

The use of soy isoflavones is a potential alternative to hormone replacement therapy in post-menopausal bone-loss prevention. Nevertheless, phytoestrogens can target other organs and may disrupt cell proliferation, or could modify endogenous steroid hormone metabolism. These mechanisms could be linked to an increased risk of developing cancer. We therefore studied the possible side effects of such treatments in an experimental model of menopause. Forty adult female Wistar rats were ovariectomized and fed with a genistein-, daidzein- or equol-supplemented diet at bone-sparing levels (10 mg/kg BW/day) for 3 months. The estrogenic effects were assessed by histological and molecular analyses on reproductive organs. The impact on the oxidative metabolism of estradiol and on associated cytochrome P450 (CYP) activities was evaluated in liver microsomes. The relative wet weights of both the uterus and the vagina were increased in the equol group, but no significant changes in proliferating cell nuclear antigen or hormone receptor mRNA expression were noticed. In contrast, genistein and daidzein did not induce uterotrophy but caused an overexpression of estrogen receptor alpha mRNA which could correspond to a long-lasting effect of physiological concentrations of estrogens. The hepatic metabolism of estradiol was influenced by daidzein which increased the synthesis of putative mutagenic derivatives. At the same time, genistein favored estrogen 2-hydroxylation, and equol decreased 4-hydroxyestrogen production. Surprisingly, no significant alteration in hepatic CYP activities was detected. Taken together, these results demonstrate that isoflavonoid-based bone-sparing treatments are able to cause side effects on other estrogen-sensitive target organs when given in the long-term.

摘要

大豆异黄酮的使用是绝经后预防骨质流失中激素替代疗法的一种潜在替代方法。然而,植物雌激素可作用于其他器官,可能会扰乱细胞增殖,或改变内源性甾体激素代谢。这些机制可能与患癌风险增加有关。因此,我们在绝经实验模型中研究了此类治疗可能产生的副作用。将40只成年雌性Wistar大鼠进行卵巢切除,并以骨保护水平(10毫克/千克体重/天)给予补充染料木黄酮、大豆苷元或雌马酚的饮食,持续3个月。通过对生殖器官进行组织学和分子分析来评估雌激素效应。在肝微粒体中评估对雌二醇氧化代谢及相关细胞色素P450(CYP)活性的影响。雌马酚组子宫和阴道的相对湿重均增加,但增殖细胞核抗原或激素受体mRNA表达未发现显著变化。相比之下,染料木黄酮和大豆苷元未诱导子宫肥大,但导致雌激素受体α mRNA过表达,这可能对应于生理浓度雌激素的长期效应。大豆苷元影响雌二醇的肝脏代谢,增加了潜在诱变衍生物的合成。同时,染料木黄酮有利于雌激素2-羟化,而雌马酚减少了4-羟基雌激素的产生。令人惊讶的是,未检测到肝脏CYP活性有显著改变。综上所述,这些结果表明,长期给予基于异黄酮的骨保护治疗能够对其他雌激素敏感靶器官产生副作用。

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