Comparative analysis of EZH2, p16 and p53 expression in uterine carcinosarcomas

E. Makk, Noémi Bohonyi, A. Oszter, Klára Éles, Tamás Tornóczky, Arnold Tóth, Endre Kálmán, Krisztina Kovács
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Abstract

Introduction: The role of p16 and p53 immunohistochemistry in the diagnosis of rare and aggressive uterine carcinosarcoma (UCS) has been well established. However, enhancer of zeste homolog 2 (EZH2), a histone methyltransferase and a member of the polycomb group family is a relatively new biomarker, with limited published data on its significance in this tumor type. The goal of this study was to examine EZH2 expression in UCS and its components, in correlation with morphological features, and p16 and p53 staining patterns.Methods: Twenty-eight UCSs were included in the study. EZH2, p16 and p53 immunoreactivity were assessed independently by two pathologists in both tumor components (epithelial and mesenchymal). EZH2 and p16 immunostains were scored semiquantitatively: based on the percentage and intensity of tumor cell staining a binary staining index (“high- or low-expressing”) was calculated. The p53 staining pattern was evaluated as wild-type or aberrant (diffuse nuclear, null, or cytoplasmic expression). Statistical tests were used to evaluate the correlation between staining patterns for all three markers and the different tumor components and histotypes.Results: High EZH2 and p16 expression and aberrant p53 patterns were present in 89.3% 78.6% and 85.7% of the epithelial component and in 78.6%, 62.5% and 82.1% of the mesenchymal component, respectively. Differences among these expression rates were not found to be significant (p > 0.05). Regarding the epithelial component, aberrant p53 pattern was found to be significantly (p = 0.0474) more frequent in the serous (100%) than in endometrioid (66.6%) histotypes. Within the mesenchymal component, p53 null expression pattern occurred significantly (p = 0.0257) more frequently in heterologous sarcoma components (71.4%) compared to the homologous histotype (18.8%).Conclusion: In conclusion, EZH2, p16 and p53 seem to play a universal role in the pathogenesis of UCS; however, a distinctive pattern of p53 expression appears to exist between the serous and endometrioid carcinoma components and also between the homologous and heterologous sarcoma components.
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子宫癌肉瘤中 EZH2、p16 和 p53 表达的比较分析
简介p16和p53免疫组化在罕见侵袭性子宫癌肉瘤(UCS)诊断中的作用已得到公认。然而,泽斯特同源增强子 2(EZH2)是一种组蛋白甲基转移酶,也是多聚酶群家族的成员,是一种相对较新的生物标记物,有关其在该肿瘤类型中的重要性的已发表数据有限。本研究的目的是检测 EZH2 在 UCS 及其组成部分中的表达,以及与形态特征、p16 和 p53 染色模式的相关性:研究纳入了 28 例 UCS。由两名病理学家独立评估两种肿瘤成分(上皮和间质)的 EZH2、p16 和 p53 免疫反应。对 EZH2 和 p16 免疫印迹进行半定量评分:根据肿瘤细胞染色的百分比和强度计算二元染色指数("高或低表达")。p53 染色模式被评估为野生型或异常型(弥漫核表达、无效表达或胞质表达)。统计检验用于评估所有三种标记物的染色模式与不同肿瘤成分和组织类型之间的相关性:结果:EZH2和p16的高表达以及p53的异常模式分别出现在89.3%、78.6%和85.7%的上皮成分以及78.6%、62.5%和82.1%的间质成分中。这些表达率之间的差异并不显著(P > 0.05)。在上皮成分中,发现浆液型(100%)p53模式异常的比例明显高于类子宫内膜型(66.6%)(p=0.0474)。在间质成分中,与同源组织型(18.8%)相比,p53无效表达模式在异源肉瘤成分(71.4%)中出现的频率明显更高(p = 0.0257):总之,EZH2、p16 和 p53 似乎在 UCS 的发病机制中发挥着普遍作用;然而,p53 的表达模式似乎在浆液性癌和子宫内膜样癌成分之间以及同源肉瘤和异源肉瘤成分之间存在差异。
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