Fumarate Hydratase-Deficient Renal Cell Carcinoma With Predominant Tubulocystic Features Mimics Tubulocystic Renal Cell Carcinoma.

Xiaoqun Yang, Yang Liu, Huafeng Wang, Yunze Xu, Huizhi Zhang, Ming Zhao, Xiaoqing Luo, Hongtao Jin, Ji Xiong, Lili Tao, Jiankun Xu, Luting Zhou, Xiangyun Li, Haimin Xu, Lei Dong, Chaofu Wang
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Abstract

Context.—: Fumarate hydratase (FH)-deficient renal cell carcinoma (RCC) rarely exhibits a predominant tubulocystic architecture with few other components. RCC with pure tubules and cysts lined by eosinophilic tumor cells with prominent nucleoli would raise the diagnosis of tubulocystic RCC. It is important to differentiate the 2 entities because they lead to different outcomes.

Objective.—: To address this concern, a multicenter study was implemented to explore useful clinicopathologic features in differentiation between tubulocystic FH-deficient RCC and tubulocystic RCC.

Design.—: Clinical factors included age, sex, tumor size, and outcome. Morphologic factors included cell morphology, presence or absence of a nontubulocystic component, and stromal findings. Immunohistochemistry, fluorescence in situ hybridization, and next-generation sequencing were performed to explore the protein expression and molecular profiles of the 2 entities.

Results.—: We evaluated 6 patients with tubulocystic RCC and 10 patients with tubulocystic FH-deficient RCC. Tubulocystic RCC exhibited a small size (<4.0 cm, pT1a), low Ki-67 index (<5%), retained FH, and negative 2SC expression. Tubulocystic FH-deficient RCC had a relatively large size and a high Ki-67 index. Perinucleolar haloes, loss of FH, and 2SC positivity were always observed. Pure tubulocystic architecture was not observed in FH-deficient RCC, because focal nontubulocystic components can always be seen.

Conclusions.—: We emphasized multiple sectioning to identify a nontubulocystic architecture to exclude tubulocystic RCC. Moreover, tumor size, FH/2SC staining, and the Ki-67 index can differentiate tubulocystic FH-deficient RCC from tubulocystic RCC. The diagnosis of tubulocystic RCC was not recommended in renal mass biopsy because of the limited tissues sampled.

富马酸氢化酶缺陷型肾细胞癌以管囊肿为主要特征,与管囊肿型肾细胞癌相似。
背景:富马酸氢化酶(FH)缺陷型肾细胞癌(RCC)很少表现出以小管囊肿为主、其他成分很少的结构。肾小管和囊肿内有嗜酸性肿瘤细胞,核小体突出的RCC可诊断为肾小管囊性RCC。区分这两种实体非常重要,因为它们会导致不同的结果:为了解决这一问题,我们开展了一项多中心研究,以探索鉴别管状囊肿型FH缺乏症RCC和管状囊肿型RCC的有用临床病理特征:临床因素包括年龄、性别、肿瘤大小和预后。形态学因素包括细胞形态、是否存在非管状囊肿成分以及基质发现。通过免疫组化、荧光原位杂交和新一代测序,研究了这两种实体的蛋白质表达和分子特征:我们评估了6例管状囊肿型RCC患者和10例管状囊肿型FH缺陷型RCC患者。管状囊肿型 RCC 体积较小(结论):我们强调通过多次切片检查来确定非管状囊肿结构,以排除管状囊肿型 RCC。此外,肿瘤大小、FH/2SC染色和Ki-67指数可以区分管状囊肿型FH缺陷RCC和管状囊肿型RCC。由于取样组织有限,不建议在肾脏肿块活检中诊断出肾小管囊肿型 RCC。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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