类固醇受体共激活因子和共抑制因子在人子宫内膜增生和癌中的表达及其与类固醇受体和Ki-67表达的相关性

Expression of steroid receptor coactivators and corepressors in human endometrial hyperplasia and carcinoma with relevance to steroid receptors and Ki-67 expression.

作者信息

Uchikawa Junko, Shiozawa Tanri, Shih Hsien-Chang, Miyamoto Tsutomu, Feng Yu-Zhen, Kashima Hiroyasu, Oka Kenji, Konishi Ikuo

机构信息

Department of Obstetrics and Gynecology, Shinshu University School of Medicine, Asahi, Matsumoto, Japan.

出版信息

Cancer. 2003 Nov 15;98(10):2207-13. doi: 10.1002/cncr.11760.

DOI:10.1002/cncr.11760

PMID:14601091

Abstract

BACKGROUND

To examine the steroid hormone dependent growth mechanism of human endometrial hyperplasia and carcinoma, expression levels of steroid receptor cofactors, such as coactivators (steroid receptor coactivator 1 [SRC-1] and p300/cyclic AMP-response element-binding protein (p300/CBP]) and corepressors (nuclear receptor corepressor [NCoR] and silencing mediator for retinoid and thyroid-hormone receptors [SMRT]), were investigated.

METHODS

The expression levels of cofactors were examined immunohistochemically using 20 samples of normal endometria, 36 samples of hyperplastic endometria, and 58 of malignant endometria and were compared with the expression levels of estrogen receptor (ER), progesterone receptor (PR), and a proliferation marker, Ki-67.

RESULTS

In samples of normal endometria, the expression of coactivators was observed diffusely in glandular cells in the proliferative phase, with a mean positivity index (PI) of 81.8 for SRC-1 and 91.3 for p300/CBP, whereas expression levels decreased in endometrial hyperplasia (PI: SRC-1, 58.9; p300/CBP, 83.8) and endometrial carcinoma (PI: SRC-1, 45.0; p300/CBP, 55.4). In endometrial hyperplasia, there was a significant correlation between the expression of ER and SRC-1 or p300/CBP. In contrast, there were no significant statistical or topologic correlations between the expression of coactivators and the expression of ER/PR in endometrial carcinoma. The expression of corepressors generally was limited, except for elevated expression of NCoR in endometrial hyperplasia (PI, 23.8).

CONCLUSIONS

The current study showed that expression levels of the steroid receptor coactivators SRC-1 and p300/CBP were reduced in endometrial carcinoma compared with normal and hyperplastic endometrium. In addition, topologic coexpression of both coactivators and ER/PR was lost in endometrial carcinoma. Accordingly, limited response to sex steroids in patients with endometrial carcinoma may be ascribed to the dissociation of cofactors and ER/PR.

摘要

背景

为研究人子宫内膜增生和癌的类固醇激素依赖性生长机制，对类固醇受体辅因子的表达水平进行了研究，这些辅因子包括共激活因子（类固醇受体共激活因子1 [SRC-1] 和p300/环磷酸腺苷反应元件结合蛋白 [p300/CBP]）和共抑制因子（核受体共抑制因子 [NCoR] 以及维甲酸和甲状腺激素受体沉默介质 [SMRT]）。

方法

采用免疫组织化学方法检测20例正常子宫内膜、36例增生性子宫内膜和58例恶性子宫内膜样本中辅因子的表达水平，并与雌激素受体（ER）、孕激素受体（PR）以及增殖标志物Ki-67的表达水平进行比较。

结果

在正常子宫内膜样本中，共激活因子在增殖期腺细胞中呈弥漫性表达，SRC-1的平均阳性指数（PI）为81.8，p300/CBP为91.3，而在子宫内膜增生（PI：SRC-1，58.9；p300/CBP，83.8）和子宫内膜癌（PI：SRC-1，45.0；p300/CBP，55.4）中表达水平降低。在子宫内膜增生中，ER与SRC-1或p300/CBP的表达之间存在显著相关性。相比之下，在子宫内膜癌中，共激活因子的表达与ER/PR的表达之间不存在显著的统计学或拓扑相关性。共抑制因子的表达一般有限，除了在子宫内膜增生中NCoR表达升高（PI，23.8）。