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雌激素受体β(ERβ)在人前列腺组织、癌前病变以及原发性、转移性和复发性前列腺腺癌中的差异表达。

Differential expression of the estrogen receptor beta (ERbeta) in human prostate tissue, premalignant changes, and in primary, metastatic, and recurrent prostatic adenocarcinoma.

作者信息

Fixemer Thomas, Remberger Klaus, Bonkhoff Helmut

机构信息

Institute of Pathology, University of the Saarland, Homburg-Saar, Germany.

出版信息

Prostate. 2003 Feb 1;54(2):79-87. doi: 10.1002/pros.10171.

Abstract

BACKGROUND

Estrogen signaling mediated by the estrogen receptor beta (ERbeta) has potential implications in normal and abnormal prostate growth. Few studies have addressed this issue in human prostate tissue leaving conflicting results on the immunolocalization of the ERbeta in benign and neoplastic lesions.

METHODS

Using a new monoclonal antibody, the current study reports on the differential expression of the ERbeta in tissue sections from 132 patients with prostate cancer.

RESULTS

The prostatic epithelium expressed the ERbeta extensively in secretory luminal cell types and at lower levels in basal cells. Atrophic changes of the peripheral zone (PZ) were more immunoreactive than hyperplastic lesions of the transition zone (TZ). When compared with glandular tissue of the PZ, high-grade prostatic intraepithelial neoplasia (HGPIN) revealed decreased levels of the ERbeta in 30 of 47 cases and was unreactive in six lesions. In informative cases with suitable internal controls, all primary tumors (n = 60), lymph node (n = 7), and bone metastases (n = 5) expressed the ERbeta at variable degree. No correlation was found between the ERbeta status, the primary Gleason grade (P = 0.254), and the pathological stage (P = 0.157). Recurrent adenocarcinoma revealed markedly decreased levels in 15 of 40 cases and was ERbeta negative in five recurrent lesions.

CONCLUSIONS

The secretory epithelium is a major target of ERbeta-mediated estrogen signaling in the human prostate. Its downregulation in HGPIN is consistent with chemopreventive effects that the ERbeta may exert on the prostatic epithelium. The continuous expression of the receptor protein at significant levels in untreated primary and metastatic adenocarcinoma indicates that these tumors can use estrogens through an ERbeta-mediated pathway. The partial loss of the ERbeta in recurrent tumors after androgen-deprivation may reflect the androgen-dependence of ERbeta gene expression in human prostate cancer.

摘要

背景

由雌激素受体β(ERβ)介导的雌激素信号传导在前列腺的正常和异常生长中具有潜在影响。很少有研究在人类前列腺组织中探讨这一问题,关于ERβ在良性和肿瘤性病变中的免疫定位存在相互矛盾的结果。

方法

本研究使用一种新的单克隆抗体,报告了132例前列腺癌患者组织切片中ERβ的差异表达情况。

结果

前列腺上皮在分泌性腔面细胞类型中广泛表达ERβ,在基底细胞中表达水平较低。外周区(PZ)的萎缩性改变比移行区(TZ)的增生性病变免疫反应性更强。与PZ的腺组织相比,47例中有30例高级别前列腺上皮内瘤变(HGPIN)的ERβ水平降低,6个病变无反应。在有合适内部对照的信息充分的病例中,所有原发性肿瘤(n = 60)、淋巴结(n = 7)和骨转移瘤(n = 5)均不同程度表达ERβ。未发现ERβ状态与原发性Gleason分级(P = 0.254)及病理分期(P = 0.157)之间存在相关性。复发性腺癌在40例中有15例水平明显降低,5例复发性病变ERβ呈阴性。

结论

分泌上皮是人类前列腺中ERβ介导的雌激素信号传导的主要靶点。其在HGPIN中的下调与ERβ可能对前列腺上皮发挥的化学预防作用一致。在未经治疗的原发性和转移性腺癌中,受体蛋白持续高水平表达表明这些肿瘤可通过ERβ介导的途径利用雌激素。雄激素剥夺后复发性肿瘤中ERβ部分缺失可能反映了人类前列腺癌中ERβ基因表达的雄激素依赖性。

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