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选择性雌激素受体-α激动剂在无子宫营养作用的情况下提供广泛的心脏和血管保护,并增强内皮祖细胞的动员。

Selective estrogen receptor-alpha agonist provides widespread heart and vascular protection with enhanced endothelial progenitor cell mobilization in the absence of uterotrophic action.

机构信息

Department of Pharmacology and Anesthesiology, University of Padua, Largo Meneghetti 2, 35131 Padua, Italy.

出版信息

FASEB J. 2010 Jul;24(7):2262-72. doi: 10.1096/fj.09-139220. Epub 2010 Mar 4.

DOI:10.1096/fj.09-139220
PMID:20203089
Abstract

The beneficial effects of estrogens on the cardiovascular system are associated with adverse effects on reproductive tissues. On the basis of previous work indicating a major role for estrogen receptor (ER)-alpha in maintaining cardiovascular health, we evaluated the tissue selectivity of the ER alpha-selective agonist propyl pyrazole triol (PPT) compared with 17beta-estradiol (E2) in vivo. Four weeks postovariectomy, equimolar doses of PPT and E2 were administered to rats in subcutaneous implants for 5 d. Both treatments restored rapid vasorelaxation of aortic tissue to estrogenic agents and prevented coronary hyperresponsiveness to angiotensin II in isolated heart preparations. Accordingly, multiple endpoints of myocardial ischemia-reperfusion injury exacerbated by ovariectomy returned to baseline following treatment. These protective effects were linked to increased in vivo levels of endothelial progenitor cells (EPCs). Human EPC function was enhanced in vitro after PPT treatment. In sharp contrast to E2, PPT treatment had no effect on uterine weight and histomorphology except for vessel density, and failed to up-regulate classic estrogen target genes. Dissection of the effects on vascular reactivity and uterine morphology was also observed following increased exposure to PPT at a higher dose for longer time. These data provide the first in vivo evidence for tissue-specific ER alpha activation. By conferring cardiovascular protection dissected from unwanted uterotrophic effects, ER alpha-selective agonists may represent a potential safer alternative to natural hormones.

摘要

雌激素对心血管系统的有益作用与对生殖组织的不良作用有关。基于先前的工作表明雌激素受体 (ER)-α在维持心血管健康方面起着重要作用,我们评估了 ERα 选择性激动剂丙基吡唑三醇 (PPT)与 17β-雌二醇 (E2) 在体内的组织选择性。卵巢切除术后 4 周,将等量剂量的 PPT 和 E2 以皮下植入物的形式给予大鼠,持续 5 天。两种治疗均恢复了主动脉组织对雌激素药物的快速血管舒张作用,并防止了分离心脏制剂中血管紧张素 II 引起的冠状动脉高反应性。因此,卵巢切除术后加重的心肌缺血再灌注损伤的多个终点在治疗后恢复到基线。这些保护作用与体内内皮祖细胞 (EPC)水平的增加有关。人 EPC 功能在 PPT 处理后在体外增强。与 E2 形成鲜明对比的是,除血管密度外,PPT 处理对子宫重量和组织形态学没有影响,也不能上调经典的雌激素靶基因。在更高剂量和更长时间增加 PPT 暴露后,也观察到对血管反应性和子宫形态的影响的分离。这些数据提供了体内 ERα 激活的首个证据。通过将心血管保护与不必要的子宫营养作用分离,ERα 选择性激动剂可能代表天然激素更安全的替代物。

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