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Akt、Ras和细胞周期调节因子在多囊卵巢综合征女性子宫内膜增生潜在发展中的作用。

Involvement of Akt, Ras and cell cycle regulators in the potential development of endometrial hyperplasia in women with polycystic ovarian syndrome.

作者信息

Villavicencio A, Goyeneche A, Telleria C, Bacallao K, Gabler F, Fuentes A, Vega M

机构信息

Institute of Nutrition and Food Technology, University of Chile, Chile.

Division of Basic Biomedical Sciences, Sanford School of Medicine, University of South Dakota, USA.

出版信息

Gynecol Oncol. 2009 Oct;115(1):102-107. doi: 10.1016/j.ygyno.2009.06.033. Epub 2009 Jul 23.

Abstract

OBJECTIVE

To examine whether the abundance, localization, and/or activity of cell cycle regulators CDK2, Cyclin E, p27, and survival proteins AKT and Ras in PCOS-associated endometria (with and without hyperplasia) differ from non-PCOS endometria.

METHODS

The expression of CDK2, Cyclin E, p27, AKT and Ras was measured by immunohistochemistry and/or Western blot in 9 normal endometria (NE), 12 endometria from PCOS patients without endometrial hyperplasia (PCOSE), 7 endometria from PCOS women with endometrial hyperplasia (HPCOSE), and 9 endometria from patients with endometrial hyperplasia (HE). The activity of CDK2 was assessed by an in vitro kinase assay.

RESULTS

CDK2, Cyclin E and p27 proteins were expressed mainly in the endometrial epithelial cells of the studied groups. No change in the activity of CDK2 was observed in total extracts obtained from the tissue samples. However, the nuclear expression of CDK2 in epithelial cells was slightly elevated in PCOSE and significantly increased in HPCOSE when compared to NE. Higher expression of p27 was detected in the cytoplasm of epithelial cells of PCOSE and HPCOSE when compared to NE. Also, we found an increment in Ser473-AKT phosphorylation and an over-expression of the Ras oncogene in endometria of patients with PCOS.

CONCLUSION

The PCOS condition is associated with increased Ser473-AKT phosphorylation, elevated expression of Ras, increased cytoplasmic abundance of p27, and increased nuclear abundance of CDK2 in the endometrial epithelial cells. These biological events could potentially provide a chance for endometrial cells from PCOS patients to exit the controlled cell cycle and become hyperplastic at a later stage.

摘要

目的

研究多囊卵巢综合征(PCOS)相关子宫内膜(有或无增生)中细胞周期调节因子CDK2、细胞周期蛋白E(Cyclin E)、p27以及存活蛋白AKT和Ras的丰度、定位和/或活性是否与非PCOS子宫内膜不同。

方法

采用免疫组织化学和/或蛋白质印迹法检测9例正常子宫内膜(NE)、12例无子宫内膜增生的PCOS患者的子宫内膜(PCOSE)、7例有子宫内膜增生的PCOS女性的子宫内膜(HPCOSE)以及9例子宫内膜增生患者的子宫内膜(HE)中CDK2、Cyclin E、p27、AKT和Ras的表达。通过体外激酶测定评估CDK2的活性。

结果

CDK2、Cyclin E和p27蛋白主要表达于研究组的子宫内膜上皮细胞。在从组织样本获得的总提取物中未观察到CDK2活性的变化。然而,与NE相比,PCOSE中上皮细胞CDK2的核表达略有升高,HPCOSE中则显著增加。与NE相比,PCOSE和HPCOSE上皮细胞胞质中p27的表达更高。此外,我们发现PCOS患者子宫内膜中Ser473-AKT磷酸化增加以及Ras癌基因过表达。

结论

PCOS状态与子宫内膜上皮细胞中Ser473-AKT磷酸化增加、Ras表达升高、p27胞质丰度增加以及CDK2核丰度增加有关。这些生物学事件可能为PCOS患者的子宫内膜细胞提供机会脱离受控的细胞周期,并在后期发生增生。

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