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对与雌激素受体α和β具有不同结合亲和力的配体的血管保护作用和促子宫生长作用进行区分。

Differentiation between vasculoprotective and uterotrophic effects of ligands with different binding affinities to estrogen receptors alpha and beta.

作者信息

Mäkelä S, Savolainen H, Aavik E, Myllärniemi M, Strauss L, Taskinen E, Gustafsson J A, Häyry P

机构信息

University of Turku, Institute of Biomedicine and MediCity Research Laboratory, Kiinamyllynkatu 10, FIN-20520 Turku, Finland.

出版信息

Proc Natl Acad Sci U S A. 1999 Jun 8;96(12):7077-82. doi: 10.1073/pnas.96.12.7077.

Abstract

Estrogen-based drug therapy in cardiovascular diseases has been difficult because it has not been possible to separate the wanted vasculoprotective effect from the unwanted effects of the hormone to the reproductive system. Here, we demonstrate that, after endothelial denudation of rat carotid artery, the mRNA of the classical estrogen receptor (ERalpha) is constitutively expressed at a low level whereas the expression of the novel ERbeta mRNA increases >40-fold. Under in situ hybridization and immunohistochemistry, ERbeta mRNA and protein colocalize with the smooth muscle cells in the media and neointima. Treatment of ovariectomized female rats with the isoflavone phytoestrogen genistein, which shows 20-fold higher binding affinity to ERbeta than to ERalpha, or with 17beta-estradiol, which does not differentiate between the two receptors, provides similar dose-dependent vasculoprotective effect in rat carotid injury model. In addition in concentrations <10 microM, both ligands are equally inhibitory to the replication and migration of smooth muscle cells in vitro. However, only treatment with 17beta-estradiol, but not with genistein, is accompanied with a dose-dependent uterotrophic effect. The results suggest that preferential targeting to ERbeta will provide vasculoprotective estrogen analogs devoid of effects to the reproductive system.

摘要

基于雌激素的药物疗法在心血管疾病治疗中一直存在困难,因为无法将所需的血管保护作用与该激素对生殖系统的不良影响区分开来。在此,我们证明,大鼠颈动脉内皮剥脱后,经典雌激素受体(ERα)的mRNA以低水平组成性表达,而新型ERβ mRNA的表达增加了40多倍。在原位杂交和免疫组织化学检测下,ERβ mRNA和蛋白与中膜和新生内膜中的平滑肌细胞共定位。用异黄酮类植物雌激素染料木黄酮(其对ERβ的结合亲和力比对ERα高20倍)或17β-雌二醇(其对两种受体无区分性)处理去卵巢雌性大鼠,在大鼠颈动脉损伤模型中可提供相似的剂量依赖性血管保护作用。此外,在浓度低于10微摩尔时,两种配体对体外平滑肌细胞的增殖和迁移均具有同等抑制作用。然而,只有用17β-雌二醇处理会伴随剂量依赖性的子宫营养作用,而染料木黄酮则不会。结果表明,优先靶向ERβ将提供对生殖系统无影响的血管保护雌激素类似物。

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