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人子宫内膜腺癌中孕激素受体分布的异质性

Heterogeneity of progesterone receptor distribution in human endometrial adenocarcinoma.

作者信息

Zaino R J, Clarke C L, Mortel R, Satyaswaroop P G

机构信息

Department of Pathology, Milton S. Hershey Medical Center, Pennsylvania State University, Hershey 17033.

出版信息

Cancer Res. 1988 Apr 1;48(7):1889-95.

PMID:3280122
Abstract

The clinical response of advanced endometrial adenocarcinoma to progestin therapy does not correlate perfectly with biochemically assayed progesterone receptor status of the tumor. We have previously suggested that heterogeneity of progesterone receptor at the cellular, tumor, and tissue levels, not detectable by the biochemical assay, might contribute to this discrepancy. A monoclonal antibody, hPRa-1, generated against human progesterone receptor, was used in the present study to immunohistologically define the heterogeneity of progesterone receptor distribution in primary endometrial carcinomas. Twenty-four hysterectomy specimens removed for the treatment of endometrial adenocarcinoma were examined by biochemical assay of progesterone receptor and immunohistochemistry. In two cases, in which tumor occupied almost all of the endometrial lining, more extensive sampling was performed with removal of four noncontiguous sites. Each site was subdivided for immunohistochemistry and biochemical assay of progesterone receptor. When present, progesterone receptor localization was confined to the nuclei of target cells. Variability in the distribution and intensity of staining was consistently observed within the tumors. Of 24 tumors 15 were determined to be progesterone receptor positive by biochemical assay, while 12 of 24 tumors displayed immunolocalization for progesterone receptor. The correlation of the results by the two methods was high (20 of 24 cases, 83%), and the discrepancies in three cases appeared to reflect tissue and tumor heterogeneity. Immunolocalization has demonstrated that heterogeneity is present at the tumor, tissue, and cellular level within endometrial carcinomas, and the failure of some progesterone receptor-positive (by biochemical assay) tumors to respond to progestin therapy may reflect false positive results due to contamination of progesterone receptor-negative tumors by adjacent benign endometrium or myometrium.

摘要

晚期子宫内膜腺癌对孕激素治疗的临床反应与通过生化检测的肿瘤孕激素受体状态并非完全相关。我们之前曾提出,生化检测无法检测到的细胞、肿瘤和组织水平上孕激素受体的异质性可能导致了这种差异。在本研究中,使用一种针对人孕激素受体产生的单克隆抗体hPRa-1,通过免疫组织化学来确定原发性子宫内膜癌中孕激素受体分布的异质性。对24例因治疗子宫内膜腺癌而切除的子宫切除标本进行了孕激素受体的生化检测和免疫组织化学检查。在两例肿瘤几乎占据整个子宫内膜的病例中,进行了更广泛的取样,切除了四个不相邻的部位。每个部位再细分用于孕激素受体的免疫组织化学和生化检测。如果存在孕激素受体,其定位局限于靶细胞的细胞核。在肿瘤内部一直观察到染色分布和强度的变异性。24例肿瘤中,通过生化检测确定15例为孕激素受体阳性,而24例肿瘤中有12例显示出孕激素受体的免疫定位。两种方法结果的相关性很高(24例中有20例,83%),三例中的差异似乎反映了组织和肿瘤的异质性。免疫定位已证明子宫内膜癌在肿瘤、组织和细胞水平存在异质性,一些(通过生化检测)孕激素受体阳性的肿瘤对孕激素治疗无反应可能反映了由于相邻良性子宫内膜或肌层对孕激素受体阴性肿瘤的污染导致的假阳性结果。

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