p53及选定增殖标志物（Ki-67、MCM3、PCNA和拓扑异构酶IIα）在卵巢交界性肿瘤中的表达：与临床病理特征的相关性

Expression of p53 and selected proliferative markers (Ki-67, MCM3, PCNA, and topoisomerase IIα) in borderline ovarian tumors: Correlation with clinicopathological features.

作者信息

Ciepliński Klaudiusz, Jóźwik Maciej, Semczuk-Sikora Anna, Gogacz Marek, Lewkowicz Dorota, Ignatov Atanas, Semczuk Andrzej

机构信息

Department of Obstetrics and Gynecology, Municipal Hospital, Płock, Poland.

Department of Gynecology and Gynecologic Oncology, Medical University of Białystok, Białystok, Poland.

出版信息

Histol Histopathol. 2018 Feb;33(2):171-179. doi: 10.14670/HH-11-902. Epub 2017 May 11.

DOI:10.14670/HH-11-902

PMID:28493257

Abstract

BACKGROUND

The expression of p53 has been studied not only in primary human ovarian carcinomas, but also in borderline ovarian tumors, however, the results were discordant. Expression patterns of proteins involved in cell proliferation and apoptosis have been investigated in various human neoplasms, including female genital tract neoplasms.

OBJECTIVE

The aim of this investigation was to assess the staining pattern and immunolocalization of p53 and selected proliferative markers (Ki-67, MCM3, PCNA, and topoisomerase IIα) in borderline ovarian tumors (BOTs).

DESIGN

The study group consisted of 42 women who underwent pelvic surgery between 2006-2015. The median patients' age was 46 years. The immunoperoxidase technique was employed using antibodies against p53, Ki-67, MCM3, PCNA, and topoisomerase IIα.

RESULTS

For p53, nuclear expression was observed in BOTs, however, cytoplasmatic immunoreactivity was also detected. Altogether, 25 (60%) tumors demonstrated positive p53 immunostaining, including overexpression found in 6 (14%). There were no significant differences in p53 expression between subgroups of clinicopathological variables. Immunoexpression of Ki-67, MCM3, PCNA, and topoisomerase IIα was nuclear. Ki-67 expression was positive in 12 (29%) cases and there was a trend towards a relationship between patients' age and Ki-67 staining (P=0.08). Interestingly, a significantly higher Ki-67 expression was found in tumors of ≥10 cm in diameter compared to smaller tumors (P=0.008). MCM3 expression was detected in 38 (90%) tumors, and PCNA expression in 28 (67%), yet none of clinicopathological factors was related to them. Topoisomerase IIα expression was present in 14 (33%) cases and, interestingly, its significantly higher expression was observed in BOTs of ≥10 cm in diameter compared to smaller tumors (P=0.008). Moreover, Spearman's correlation revealed highly significant positive associations between Ki-67 and topoisomerase IIα (R=0.403, P=0.008) and Ki-67 and MCM3 (R=0.469, P=0.001).

CONCLUSIONS

We report a high positive immunostaining rate for p53, suggesting a role of TP53 alterations in the development of BOTs in humans. The new finding of higher topoisomerase IIα immunostaining positivity in BOTs of ≥10 cm may be clinically relevant and requires further studies on larger patient groups.

摘要

背景

p53的表达不仅在原发性人类卵巢癌中得到研究，在卵巢交界性肿瘤中也有研究，但结果不一致。参与细胞增殖和凋亡的蛋白质表达模式已在包括女性生殖道肿瘤在内的各种人类肿瘤中进行了研究。

目的

本研究旨在评估p53以及选定的增殖标志物（Ki-67、MCM3、PCNA和拓扑异构酶IIα）在卵巢交界性肿瘤（BOTs）中的染色模式和免疫定位。

设计

研究组由2006年至2015年间接受盆腔手术的42名女性组成。患者的中位年龄为46岁。采用免疫过氧化物酶技术，使用针对p53、Ki-67、MCM3、PCNA和拓扑异构酶IIα的抗体。

结果

对于p53，在BOTs中观察到核表达，但也检测到细胞质免疫反应性。总共有25个（60%）肿瘤显示p53免疫染色呈阳性，其中6个（14%）发现有过表达。临床病理变量亚组之间p53表达无显著差异。Ki-67、MCM3、PCNA和拓扑异构酶IIα的免疫表达为核表达。Ki-67表达在12例（29%）病例中呈阳性，患者年龄与Ki-67染色之间存在相关趋势（P=0.08）。有趣的是，与较小肿瘤相比，直径≥10 cm的肿瘤中Ki-67表达显著更高（P=0.008）。38个（90%）肿瘤检测到MCM3表达，28个（67%）检测到PCNA表达，但没有临床病理因素与它们相关。拓扑异构酶IIα表达出现在14例（33%）病例中，有趣的是，与较小肿瘤相比，直径≥10 cm的BOTs中其表达显著更高（P=0.008）。此外，Spearman相关性分析显示Ki-67与拓扑异构酶IIα之间存在高度显著的正相关（R=0.403，P=0.008）以及Ki-67与MCM3之间存在高度显著的正相关（R=0.469，P=0.001）。