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尽管有诊断形态学依据,但许多混合型子宫内膜癌显示出意想不到的免疫组化染色模式。

Despite Diagnostic Morphology, Many Mixed Endometrial Carcinomas Show Unexpected Immunohistochemical Staining Patterns.

作者信息

Matrai Cathleen E, Pirog Edyta C, Ellenson Lora Hedrick

机构信息

Department of Pathology and Laboratory Medicine, New York Presbyterian Hospital-Weill Cornell Medicine, New York, New York.

出版信息

Int J Gynecol Pathol. 2018 Sep;37(5):405-413. doi: 10.1097/PGP.0000000000000443.

Abstract

Historically, endometrial carcinomas have been classified primarily according to their histology. However, the use of immunohistochemistry has become commonplace in their evaluation, particularly in diagnostically challenging cases. Our objective was to evaluate mixed endometrial carcinomas using a well-established panel of biomarkers to assess the consistency and utility of these stains in clinical diagnosis. Eighteen cases comprised of various combinations of classical serous (SC), endometrioid (EC), and clear cell (CC) morphologies were identified and subjected to a panel of immunohistochemical markers including p53, p16, Ki67, estrogen receptor, progesterone receptor, and Napsin A. Intensity and extent of staining were evaluated on 4-tiered and 5-tiered scales, respectively. The typical immunostaining pattern expected for the individual tumor components was seen in only 3 cases, while in 15 cases an unexpected pattern was observed with at least one immunomarker. By tumor type, the most common unexpected finding in EC/SC carcinoma cases was diffuse positivity for p16 and/or estrogen receptor/progesterone receptor in both components, while in SC/CC, diffuse positivity for p53 in both components was most frequently seen, and in SC/CC/EC, Napsin A negativity was most commonly observed. Despite displaying diagnostic morphology, components of many mixed endometrial carcinomas may not exhibit expected immunohistochemical features. This may be due to the fact that these carcinomas arise from a single clone with subsequent divergence, resulting in a tumor with both mixed histologic and genetic features. It is important to note that these tumors may not demonstrate the immunohistochemical prototype of their constituents and should be approached accordingly from a diagnostic perspective.

摘要

从历史上看,子宫内膜癌主要是根据其组织学进行分类的。然而,免疫组织化学在其评估中已变得很普遍,尤其是在诊断具有挑战性的病例中。我们的目的是使用一组成熟的生物标志物来评估混合性子宫内膜癌,以评估这些染色在临床诊断中的一致性和实用性。确定了18例由经典浆液性(SC)、子宫内膜样(EC)和透明细胞(CC)形态的各种组合组成的病例,并对其进行了一组免疫组织化学标记物检测,包括p53、p16、Ki67、雌激素受体、孕激素受体和Napsin A。分别在4级和5级尺度上评估染色强度和范围。仅在3例病例中观察到单个肿瘤成分预期的典型免疫染色模式,而在15例病例中,至少有一种免疫标记物观察到意外模式。按肿瘤类型,在EC/SC癌病例中最常见的意外发现是两个成分中p16和/或雌激素受体/孕激素受体弥漫性阳性,而在SC/CC中,最常观察到两个成分中p53弥漫性阳性,在SC/CC/EC中,最常观察到Napsin A阴性。尽管显示出诊断形态,但许多混合性子宫内膜癌的成分可能未表现出预期的免疫组织化学特征。这可能是由于这些癌起源于单个克隆,随后发生分化,导致肿瘤具有混合的组织学和遗传学特征。需要注意的是,这些肿瘤可能未表现出其成分的免疫组织化学原型,从诊断角度应相应地进行处理。

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