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免疫组织化学面板鉴定浸润性微乳头状癌的原发部位。

Immunohistochemical panel to identify the primary site of invasive micropapillary carcinoma.

机构信息

Department of Pathology, The Johns Hopkins Medical Institutions, Baltimore, MD 21231, USA.

出版信息

Am J Surg Pathol. 2009 Jul;33(7):1037-41. doi: 10.1097/PAS.0b013e3181962dcd.

Abstract

Invasive micropapillary carcinoma (IMC) is generally an aggressive morphologic variant that has been described in the bladder, lung, breast, salivary gland, gastrointestinal tract, and ovary. Given the morphologic similarities between IMCs arising from different organ systems and the high propensity of this histologic subtype for lymphatic metastasis, it may be necessary to use immunohistochemical (IHC) markers to determine the primary site of an IMC. Few studies have compared the IHC profiles of IMCs originating from different sites. We tested a panel of 11 IHC markers for their ability to distinguish urothelial, lung, breast, and ovarian IMC using a tissue microarray constructed with primary tumor tissue from 47 patients with IMC (13 bladder, 6 lung, 16 breast, and 12 ovarian). For each tumor, correct classification as IMC was verified by reverse polarity MUC1 expression. We found that immunostaining for uroplakin, CK20, TTF-1, estrogen receptor (ER), WT-1 and/or PAX8, and mammaglobin was the best panel for determining the most likely primary site of IMC. The best markers to identify urothelial IMC were uroplakin and CK20, whereas p63, high molecular weight cytokeratin, and thrombomodulin were less sensitive and specific. Lung IMC was uniformly TTF-1 positive. Breast IMC was ER positive, mammaglobin positive, and PAX8/WT-1 negative, while ovarian IMC was ER positive, mammaglobin negative, and PAX8/WT-1 positive. In the metastatic setting, or when IMC occurs without an associated in situ or conventional carcinoma component, staining for uroplakin, CK20, TTF-1, ER and WT-1, and/or PAX8, and mammaglobin is the best panel for accurately classifying the likely primary site of IMC.

摘要

浸润性微乳头状癌(IMC)通常是一种侵袭性形态学变异型,已在膀胱、肺、乳腺、唾液腺、胃肠道和卵巢中描述过。鉴于不同器官系统起源的 IMC 之间存在形态学相似性,以及这种组织学亚型具有高淋巴转移倾向,因此可能需要使用免疫组织化学(IHC)标志物来确定 IMC 的原发部位。很少有研究比较过源自不同部位的 IMC 的 IHC 特征。我们使用由 47 例 IMC 患者的原发肿瘤组织构建的组织微阵列,测试了一组 11 种 IHC 标志物来区分尿路上皮、肺、乳腺和卵巢 IMC 的能力(13 例膀胱、6 例肺、16 例乳腺和 12 例卵巢)。对于每个肿瘤,通过反转极性 MUC1 表达来验证正确分类为 IMC。我们发现,uroplakin、CK20、TTF-1、雌激素受体(ER)、WT-1 和/或 PAX8 和 mammaglobin 的免疫染色是确定 IMC 最可能原发部位的最佳组合。识别尿路上皮 IMC 的最佳标志物是 uroplakin 和 CK20,而 p63、高分子量细胞角蛋白和血栓调节蛋白的敏感性和特异性较低。肺 IMC 均为 TTF-1 阳性。乳腺 IMC 为 ER 阳性、mammaglobin 阳性、PAX8/WT-1 阴性,而卵巢 IMC 为 ER 阳性、mammaglobin 阴性、PAX8/WT-1 阳性。在转移性环境中,或者当 IMC 发生而没有相关的原位或常规癌成分时,uroplakin、CK20、TTF-1、ER 和 WT-1、和/或 PAX8 和 mammaglobin 的染色是准确分类 IMC 最可能原发部位的最佳组合。

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