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Eosinophilic Solid and Cystic Renal Cell Carcinoma (ESC RCC): Further Morphologic and Molecular Characterization of ESC RCC as a Distinct Entity.

嗜酸性实性和囊性肾细胞癌:进一步的形态学和分子遗传学特征支持其为独立的肿瘤实体

Trpkov K,Abou-Ouf H,Hes O,Lopez JI,Nesi G,Comperat E,Sibony M,Osunkoya AO,Zhou M,Gokden N,Leroy X,Berney DM,Werneck Cunha I,Musto ML,Athanazio DA,Yilmaz A,Donnelly B,Hyndman E,Gill AJ,McKenney JK,Bismar TA

Abstract

Eosinophilic solid and cystic renal cell carcinoma (ESC RCC) has been recently described as a unique and indolent renal neoplasm, found in female patients with and without tuberous sclerosis complex. Although ESC RCC has a distinct morphology and frequent CK20 reactivity, its molecular karyotype has been previously studied only in few cases. We identified 19 ESC RCC from multiple institutions; all patients were female individuals without clinical features of tuberous sclerosis complex. Molecular karyotyping was performed in 13 cases (12 with informative result). The median age was 55 years (range: 32 to 79 y). The tumors were yellow-gray with a median size of 31 mm (range: 12 to 135 mm) and showed solid and cystic gross appearance. All tumors demonstrated typical microscopic features with solid areas admixed with variably sized macrocysts and microcysts. The cells showed eosinophilic cytoplasm with granular cytoplasmic stippling and round-to-oval nuclei. CK20 was positive in 14/19 (74%) cases. Stage pT1 was found in 17/19 (89%) patients (pT1a in 12, pT1b in 5); 1 patient each had pT2a and pT3a. A total of 15/16 patients with available follow-up were alive and without evidence of disease progression, after 1 to 169 months (median: 44 mo; mean: 49.6 mo); 3 died of other causes. The most common copy number gains were 16p13.3-16q23.1 (33% to 67%), 7p21.2-7q36.2 (42% to 50%), 13q14.2 (33%), and 19p12 (33%). The most common copy number losses included Xp11.21 (42%) and 22q11.23 (33%). Loss of heterozygosity was most frequently found at 16p11.2-11.1 (75%), Xq11.1-13.1 (75%), Xq13.1-21.1 (33%), 11p11.2-11.11 (33%), 9q21.1-22.2 (33%), and 9q33.1 (33%). ESC RCC demonstrates common molecular karyotype alterations, which further support its distinct nature.

摘要

嗜酸性实性和囊性肾细胞癌(ESC RCC)是近来描述的一种发生在女性患者中罕见的惰性肾肿瘤,伴或不伴结节性硬化症。尽管ESC RCC具有独特的形态学特征,并通常表达CK20,但目前仅有极少数病例进行了分子核型研究。本文作者从多个研究机构中确定了19ESC RCC,所有患者均为女性,且不具有结节性硬化症的临床表现。对13例进行了分子核型分析(12例获得了有意义的结果)。患者年龄范围32-79岁,中位年龄55岁。肿瘤灰黄色,肉眼观呈囊实性,大小范围12-135mm,中位大小31mm。所有肿瘤均具有典型的镜下特征:实性区域与大小不等的巨囊和微囊混合组成,细胞含嗜酸性颗粒状胞质,核圆形或卵圆形。74%14/19)的病例CK20阳性。89%17/19)的患者分期为pT1期(12pT1a期,5pT1b期), pT2a期和pT3a期患者各1例。16例获得随访,15例无病存活,且无进展。随访时间1-169个月(中位随访时间44个月,平均49.6个月),3例死于其他原因。最常见的染色体拷贝数获得包括16p13.3-16q23.133%-67%)、7p21.2-7q36.242%-50%)、13q14.233%)和19q1233%)。最常见的染色体拷贝数缺失包括Xp11.21 (42%)22q11.23 (33%)。最常见的杂合性缺失包括16p11.2-11.1 (75%)Xq11.1-13.1 (75%)Xq13.1-21.1 (33%)11p11.2-11.11 (33%)9q21.1-22.2 (33%) 9q33.1 (33%)。研究结果表明ESC RCC具有共同的分子核型改变,支持其为独特的肿瘤实体。


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