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Different immunohistochemical and ultrastructural phenotypes of squamous differentiation in bladder cancer

机译:膀胱鳞癌分化的不同免疫组织化学和超微结构表型

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Besides worse prognosis of bladder cancer with squamous differentiation (pure squamous cell carcinoma (SCC) or mixed urothelial carcinoma (UC/SCC)), high-grade non-keratinising squamous differentiation is difficult to identify in haematoxylin–eosin stainings. This study aims to validate routine immunohistochemical markers for squamous differentiation in a larger cohort of patients. Tissue microarrays of 89 pure SCCs and mixed UC/SCCs, 66 urothelial carcinomas (UC), precursor lesions and normal urothelium were stained for cytokeratin (CK) 5/6, CK 5/14, CK 7, CK 20 and uroplakin III. Electron microscopy was performed to confirm the differentiation. Pure SCCs displayed staining throughout the epithelium for CK 5/6 (76.6% (36/47)) and CK 5/14 (95.8% (46/48)), focal staining for CK 7 (28.9% (13/45)) and no staining for CK 20 and uroplakin III (both 0% (0/48)). UCs exhibited a basal or diffuse staining for CK 5/6 (30.2% (16/53)) and CK 5/14 (57.1% (32/56)), focal positivity for CK 7 (83.6% (46/55)), CK 20 (50.9% (29/57)) and uroplakin III (21.8% (12/55)). Each marker discriminated SCC and UC significantly (p < 0.01). A third subgroup rarely showed full epithelial staining for CK 5/6 (14.3% (1/7)) and CK 5/14 (28.6% (2/7)), focal staining for CK 7 (85.7% (6/7)) and no staining for CK 20 and uroplakin III (both 0% (0/7)). Electron microscopy could prove both, SCC and UC characteristics, revealing a transient type. A staining pattern with CK 5/6- and CK 5/14-positivity plus CK 20- and uroplakin III-negativity identified squamous differentiation in bladder tumours and revealed a third type of squamous transdifferentiation.
机译:除了具有鳞状分化的膀胱癌(纯鳞状细胞癌(SCC)或混合尿路上皮癌(UC / SCC))的预后较差外,苏木精-伊红染色很难鉴定出高度的非角化鳞状分化。这项研究旨在验证常规免疫组化标记物在更大范围的患者群体中的鳞状分化。对89个纯SCC和混合UC / SCC,66个尿路上皮癌(UC),前体病变和正常尿道上皮的组织芯片进行了细胞角蛋白(CK)5/6,CK 5/14,CK 7,CK 20和uroplakin III染色。进行电子显微镜检查以确认分化。纯SCC对整个上皮显示CK 5/6(76.6%(36/47))和CK 5/14(95.8%(46/48))染色,CK 7局部染色(28.9%(13/45)) CK 20和uroplakin III(均为0%(0/48))均无染色。 UC对CK 5/6(30.2%(16/53))和CK 5/14(57.1%(32/56))表现出基础或弥漫性染色,对CK 7(83.6%(46/55))有局灶性阳性,CK 20(50.9%(29/57))和uroplakin III(21.8%(12/55))。每个标记物均能明显区分SCC和UC(p <0.01)。第三亚组很少显示CK 5/6(14.3%(1/7))和CK 5/14(28.6%(2/7))的完整上皮染色,CK 7(85.7%(6/7))的局部染色),而CK 20和uroplakin III(均为0%(0/7))无染色。电子显微镜可同时证明SCC和UC特性,揭示出一种瞬态类型。 CK 5 / 6-和CK 5/14阳性加上CK 20-和uroplakin III阴性的染色模式确定了膀胱肿瘤中的鳞状分化,并揭示了第三种鳞状转分化。

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