Apollo Hospital, Bhubaneswar, 751005, India; Prolife Diagnostics, Bhubaneswar, 751019, India.
National Institute of Science Education and Research, Bhubaneswar, 752050, India.
Hum Pathol. 2020 Oct;104:84-95. doi: 10.1016/j.humpath.2020.08.001. Epub 2020 Aug 14.
Primary Ewing sarcoma (ES) of the urinary bladder is a rare and aggressive small blue round cell malignant neoplasm associated primarily with translocation involving EWSR1 and FLI1 genes located in the 22nd and 11th chromosomes, respectively. To date, 18 cases have been published in the literature as single-case reports, based chiefly on CD99 positivity (17 patients). Molecular confirmation by fluorescence in situ hybridization was performed in 9 patients, and FLI1 immunohistochemical (IHC) analysis was not performed in any of these published cases. Herein, we present thirteen patients of more comprehensive primary round cell sarcomas of the urinary bladder with EWSR1 rearrangement. Clinicopathologic parameters including demographics; clinical presentation; histopathologic, IHC, and molecular profiles; and management and follow-up data of 13 patients with primary round cell sarcomas with EWSR1 rearrangement (Ewing family of tumor) of the urinary bladder were analyzed. The studied patients (n = 13) included 6 females and 7 males; their age ranged from 4 years to 81 years (median = 30 years). The most common clinical presentation was hematuria (n = 7), followed by hydronephrosis (n = 2, one with renal failure). The tumor size ranged from 2.9 cm to 15 cm in maximum dimension. Conventional ES architecture and histology was observed in 6 cases, and diverse histology was observed in 7 cases (adamantinomatous pattern [n = 1], alveolar pattern [n = 1], ganglioneuroblastoma-like pattern [n = 2], and small cell carcinoma-like pattern [n = 3]). All the tumors were muscle invasive (invasion into the muscularis propria). IHC analysis showed that all tumors expressed FLI1, CD99, and at least one neuroendocrine marker. Focal cytokeratin staining was positive in 2 patients, and RB1 was retained in all patients. EWSR1 rearrangement was seen in 12 of 12 tumors (in 12 patients) tested. A combined multimodal approach that included surgery with chemotherapy was instituted in all patients. Follow-up was available for 11 patients (ranging from 5 to 24 months). Six patients either died of disease (n = 3) or other causes (n = 3). Five patients were alive with metastases to the liver (n = 1), liver and lung (n = 2), liver and abdominal wall (n = 1), and kidney (n = 1). Based on our experience with the largest series to date and aggregate of the published data, ES/round cell sarcomas with EWSR1 rearrangement occurring in the bladder have bimodal age distribution with poor prognosis despite aggressive therapy. Owing to its rarity and age distribution, the differential diagnosis is wide and requires a systematic approach for ruling out key age-dependent differential diagnoses aided with molecular confirmation.
原发性膀胱尤文肉瘤(ES)是一种罕见且侵袭性的小圆蓝细胞恶性肿瘤,主要与分别位于第 22 号和第 11 号染色体上的 EWSR1 和 FLI1 基因的易位有关。迄今为止,已有 18 例文献报道为单病例报告,主要基于 CD99 阳性(17 例患者)。在这些已发表的病例中,有 9 例进行了荧光原位杂交的分子确认,而没有进行任何 FLI1 免疫组化(IHC)分析。在此,我们报告了 13 例更为全面的原发性膀胱小圆细胞肉瘤病例,这些病例均存在 EWSR1 重排。分析了 13 例原发性膀胱小圆细胞肉瘤患者的临床病理参数,包括人口统计学;临床表现;组织病理学、免疫组化和分子特征;以及管理和随访数据。研究患者(n=13)包括 6 名女性和 7 名男性;年龄 4 岁至 81 岁不等(中位数=30 岁)。最常见的临床表现为血尿(n=7),其次为肾积水(n=2,其中 1 例合并肾衰竭)。肿瘤最大径为 2.9cm 至 15cm。6 例观察到典型的尤文肉瘤结构和组织学,7 例观察到不同的组织学(造釉细胞瘤样[1 例]、肺泡状[1 例]、神经节母细胞瘤样[2 例]和小细胞癌样[3 例])。所有肿瘤均为肌层浸润性(浸润至固有肌层)。免疫组化分析显示所有肿瘤均表达 FLI1、CD99 和至少一种神经内分泌标志物。2 例患者的局灶性细胞角蛋白染色阳性,所有患者的 RB1 均保留。在 12 例(12 例患者)检测的肿瘤中均观察到 EWSR1 重排。所有患者均采用包括化疗在内的联合多模式方法进行治疗。11 例患者(5 至 24 个月)可获得随访。6 例患者因疾病(n=3)或其他原因(n=3)死亡。5 例患者存活,肝转移(n=1)、肝肺转移(n=2)、肝腹壁转移(n=1)和肾转移(n=1)。根据我们目前为止的最大系列经验和已发表数据的综合分析,尽管进行了积极的治疗,但发生在膀胱中的具有 EWSR1 重排的尤文肉瘤/小圆细胞肉瘤具有双峰年龄分布,预后不良。由于其罕见性和年龄分布,鉴别诊断范围广泛,需要采用系统的方法排除关键的年龄依赖性鉴别诊断,并通过分子确认为辅助。
