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促性腺激素释放激素(GnRH)激动剂曲普瑞林可抑制雌二醇诱导的人子宫内膜癌、卵巢癌和乳腺癌细胞中的血清反应元件(SRE)激活及c-fos表达。

Gonadotropin-releasing hormone (GnRH) agonist triptorelin inhibits estradiol-induced serum response element (SRE) activation and c-fos expression in human endometrial, ovarian and breast cancer cells.

作者信息

Gründker Carsten, Günthert Andreas R, Hellriegel Martin, Emons Günter

机构信息

Department of Gynecology and Obstetrics, Georg-August-University, D-37099 Göttingen, Germany.

出版信息

Eur J Endocrinol. 2004 Nov;151(5):619-28. doi: 10.1530/eje.0.1510619.

DOI:10.1530/eje.0.1510619
PMID:15538941
Abstract

BACKGROUND AND METHODS

The majority of human endometrial (>80%), ovarian (>80%) and breast (>50%) cancers express GnRH receptors. Their spontaneous and epidermal growth-factor-induced proliferation is dose- and time-dependently reduced by treatment with GnRH and its agonists. In this study, we demonstrate that the GnRH agonist triptorelin inhibits estradiol (E2)-induced cancer cell proliferation.

RESULTS

The proliferation of quiescent estrogen receptor alpha (ER alpha)-/ER beta-positive, but not of ER alpha-negative/ER beta-positive endometrial, ovarian and breast cancer cell lines, was significantly stimulated (P<0.001) (ANOVA) after treatment with E2 (10(-8) M). This effect was time- and dose-dependently antagonized by simultaneous treatment with triptorelin. The inhibitory effect was maximal at 10(-5) M concentration of triptorelin (P<0.001). In addition, we could show that, in ER alpha-/ER beta-positive cell lines, E2 induces activation of serum response element (SRE) and expression of the immediate early-response gene c-fos. These effects were blocked by triptorelin (P<0.001). E2-induced activation of estrogen-response element (ERE) was not affected by triptorelin.

CONCLUSIONS

The transcriptional activation of SRE by E2 is due to ER alpha activation of the mitogen-activated protein kinase (MAPK) pathway. This pathway is impeded by GnRH, resulting in a reduction of E2-induced SRE activation and, in consequence, a reduction of E2-induced c-fos expression. This causes downregulation of E2-induced cancer cell proliferation.

摘要

背景与方法

大多数人类子宫内膜癌(>80%)、卵巢癌(>80%)和乳腺癌(>50%)表达促性腺激素释放激素(GnRH)受体。GnRH及其激动剂治疗可剂量和时间依赖性地降低其自发增殖以及表皮生长因子诱导的增殖。在本研究中,我们证明GnRH激动剂曲普瑞林可抑制雌二醇(E2)诱导的癌细胞增殖。

结果

用E2(10⁻⁸ M)处理后,静止的雌激素受体α(ERα)/ERβ阳性的子宫内膜、卵巢和乳腺癌细胞系的增殖受到显著刺激(P<0.001)(方差分析),而ERα阴性/ERβ阳性的细胞系则未受刺激。同时用曲普瑞林处理可时间和剂量依赖性地拮抗这一效应。曲普瑞林浓度为10⁻⁵ M时抑制作用最大(P<0.001)。此外,我们还发现,在ERα/ERβ阳性细胞系中,E2可诱导血清反应元件(SRE)激活和即刻早期反应基因c-fos表达。这些效应被曲普瑞林阻断(P<0.001)。E2诱导的雌激素反应元件(ERE)激活不受曲普瑞林影响。

结论

E2对SRE的转录激活是由于ERα激活了丝裂原活化蛋白激酶(MAPK)途径。GnRH可阻碍该途径,导致E2诱导的SRE激活减少,进而导致E2诱导的c-fos表达减少。这导致E2诱导的癌细胞增殖下调。

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