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E-钙黏蛋白和β-连环蛋白在早期宫颈癌中的表达:一项147例病例的组织芯片研究

E-Cadherin and beta-Catenin expression in early stage cervical carcinoma: a tissue microarray study of 147 cases.

作者信息

Fadare Oluwole, Reddy Harini, Wang Jun, Hileeto Denise, Schwartz Peter E, Zheng Wenxin

机构信息

Department of Pathology, Yale University School of Medicine, New Haven, CT, USA.

出版信息

World J Surg Oncol. 2005 Jun 21;3:38. doi: 10.1186/1477-7819-3-38.

Abstract

BACKGROUND

The disruption of intercellular adhesions is an important component of the acquisition of invasive properties in epithelial malignancies. Alterations in the cell-cell adhesion complex, E-Cadherin/beta-Catenin, have been implicated in the oncogenesis of carcinomas arising from various anatomic sites and have been correlated with adverse clinico-pathologic parameters. In this study, the authors investigated the immunohistochemical expression of E-Cadherin and beta-Catenin in a cohort of early stage cervical cancers to determine its prognostic significance and to investigate differences between the three major histological subtypes.

PATIENTS AND METHODS

A tissue microarray of 147 cases of FIGO stage 1A and 1B cervical carcinomas [96 squamous cell carcinomas (SCC), 35 adenocarcinomas (AC), 12 adenosquamous carcinomas (ASQ), 4 miscellaneous types] was constructed from our archived surgical pathology files and stained with monoclonal antibodies to E-Cadherin and beta-Catenin. Cases were scored by multiplying the intensity of staining (1 to 3 scale) by the percentage of cells stained (0-100%) for a potential maximum score of 300. For both markers, "preserved" expression was defined as bright membranous staining with a score of 200 or above. "Impaired" expression included any of the following: negative staining, a score less than 200, or exclusively cytoplasmic or nuclear delocalization.

RESULTS

Impaired expression of beta-Catenin was found in 85.7%, 66.7%, & 58.3% of AC, SCC & ASQ respectively. Impaired expression of E-Cadherin was found in 94.3%, 86.5% & 100% of cases of AC, SCC, & ASQ respectively. The differences between the histologic subtypes were not significant. For the whole cohort, a comparison of cases showing impaired versus preserved of E-Cadherin and beta-Catenin expression showed no significant differences with respect to recurrence free survival, overall survival, patient age, histologic grade, and frequency of lymphovascular invasion or lymph node involvement. There was no correlation between the status of both markers for all three histological subtypes (overall spearman correlation co-efficient r = 0.12, p = 0.14)

CONCLUSION

Impairment of E-Cadherin and beta-Catenin expression is very frequent in early stage cervical cancers, and alterations in the E-Cadherin/beta-Catenin cell adhesion complex are therefore likely involved in the pathogenesis of cervical carcinomas even at their earliest stages. None of the three major histological subtypes of cervical carcinoma (SCC, ADCA, ADSQ) is significantly more likely than the others to show impairment in E-Cadherin and beta-Catenin expression. Overall, the expression of both markers does not significantly correlate with clinico-pathological parameters of prognostic significance.

摘要

背景

细胞间黏附的破坏是上皮性恶性肿瘤获得侵袭特性的重要组成部分。细胞-细胞黏附复合物E-钙黏蛋白/β-连环蛋白的改变与源自各种解剖部位的癌的肿瘤发生有关,并与不良临床病理参数相关。在本研究中,作者调查了一组早期宫颈癌中E-钙黏蛋白和β-连环蛋白的免疫组织化学表达,以确定其预后意义,并研究三种主要组织学亚型之间的差异。

患者与方法

从我们存档的手术病理档案中构建了一个包含147例FIGO 1A期和1B期宫颈癌的组织芯片[96例鳞状细胞癌(SCC)、35例腺癌(AC)、12例腺鳞癌(ASQ)、4例其他类型],并用抗E-钙黏蛋白和β-连环蛋白的单克隆抗体进行染色。通过将染色强度(1至3级)乘以染色细胞百分比(0-100%)来对病例进行评分,潜在最高评分为300分。对于这两种标志物,“保留”表达定义为明亮的膜染色,评分在200分及以上。“受损”表达包括以下任何一种情况:阴性染色、评分低于200分或仅为细胞质或细胞核移位。

结果

β-连环蛋白表达受损分别在85.7%的AC、66.7%的SCC和58.3%的ASQ中发现。E-钙黏蛋白表达受损分别在94.3%的AC病例、86.5%的SCC病例和100%的ASQ病例中发现。组织学亚型之间的差异不显著。对于整个队列,比较E-钙黏蛋白和β-连环蛋白表达受损与保留的病例,在无复发生存率、总生存率、患者年龄、组织学分级以及淋巴管浸润或淋巴结受累频率方面没有显著差异。所有三种组织学亚型的两种标志物状态之间均无相关性(总体斯皮尔曼相关系数r = 0.12,p = 0.14)。

结论

E-钙黏蛋白和β-连环蛋白表达受损在早期宫颈癌中非常常见,因此E-钙黏蛋白/β-连环蛋白细胞黏附复合物的改变可能即使在宫颈癌的最早阶段也参与其发病机制。宫颈癌的三种主要组织学亚型(SCC、ADCA、ADSQ)中,没有一种比其他亚型更有可能出现E-钙黏蛋白和β-连环蛋白表达受损。总体而言,这两种标志物的表达与具有预后意义的临床病理参数没有显著相关性。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/fdf5/1183253/63d20ed612ec/1477-7819-3-38-1.jpg

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