Hertrampf T, Schmidt S, Laudenbach-Leschowsky U, Seibel J, Diel P
Department of Molecular and Cellular Sports Medicine, Deutsche Sporthochschule Köln, DSHS, Carl Diem Weg 6, Cologne, 50927 Köln, Germany.
Mol Cell Endocrinol. 2005 Nov 24;243(1-2):51-7. doi: 10.1016/j.mce.2005.08.007. Epub 2005 Nov 4.
Cyclooxygenase 2 (Cox-2), an enzyme involved in prostaglandin production, is a key player in the development of pathologic changes, such as colorectal cancer, arteriosclerosis and thrombosis. In this study, we investigated the effects of estrogens, selective estrogen receptor modulators (SERMs), pure antiestrogens and phytoestrogens on the tissue-specific expression of Cox-2 in the uterus and the v. cava of ovariectomized female rats. Cox-2 expression could be detected in the uterine epithelium and in the endothelium of the v. cava. Cox-2 expression was time-dependently stimulated after administration of 17beta estradiol (E2) in the uterus. In the v. cava, E2 treatment resulted in a stimulated expression of the progesterone receptor (PR), a gene known to be regulated by E2, whereas Cox-2 was simultaneously down-regulated. Administration of the pure antiestrogen faslodex (Fas) had no effect on Cox-2 expression. In contrast, administration of tamoxifen (Tam) resulted in a decrease of Cox-2 expression in the v. cava but does not stimulate Cox-2 expression in the uterus. Interestingly, the same expression pattern of Cox-2 could be detected after dose-dependent administration of genistein (Gen). Here, down-regulation of Cox-2 could already be detected after administration of merely 0.5 mg/(kgBW) Gen, a dose where no effects on uterine weight were observed. In summary, our results demonstrate a reverse tissue-specific regulation of Cox-2 expression by estrogens in the v. cava and uterus indicating the existence of complex molecular mechanisms which have to be characterized in future studies. Remarkably, Tam and the phytoestrogen Gen, both share the ability to decrease the expression of Cox-2 in the v. cava without effecting its uterine expression. These observations may be of great importance with respect to potential beneficial or adverse effects of estrogens, SERMs and phytoestrogens on the cardiovascular tissue.
环氧化酶2(Cox-2)是一种参与前列腺素生成的酶,在诸如结直肠癌、动脉硬化和血栓形成等病理变化的发展过程中起着关键作用。在本研究中,我们调查了雌激素、选择性雌激素受体调节剂(SERM)、纯抗雌激素和植物雌激素对去卵巢雌性大鼠子宫和腔静脉中Cox-2组织特异性表达的影响。在子宫上皮和腔静脉内皮中可检测到Cox-2表达。在子宫中给予17β-雌二醇(E2)后,Cox-2表达呈时间依赖性增加。在腔静脉中,E2处理导致孕酮受体(PR)表达增加,PR是一种已知受E2调节的基因,而Cox-2同时被下调。给予纯抗雌激素氟维司群(Fas)对Cox-2表达无影响。相反,给予他莫昔芬(Tam)导致腔静脉中Cox-2表达降低,但不刺激子宫中Cox-2表达。有趣的是,在给予不同剂量的染料木黄酮(Gen)后,也观察到了相同的Cox-2表达模式。在此,仅给予0.5mg/(kg体重)Gen后即可检测到Cox-2下调,该剂量对子宫重量无影响。总之,我们的结果表明雌激素对腔静脉和子宫中Cox-2表达具有相反的组织特异性调节作用,这表明存在复杂的分子机制,有待在未来的研究中进一步阐明。值得注意的是,Tam和植物雌激素Gen均具有降低腔静脉中Cox-2表达而不影响其子宫表达的能力。这些观察结果对于雌激素、SERM和植物雌激素对心血管组织的潜在有益或不利影响可能具有重要意义。
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