Departments of Pathology.
Urology.
Am J Surg Pathol. 2023 Dec 1;47(12):1335-1348. doi: 10.1097/PAS.0000000000002101. Epub 2023 Aug 1.
The concept of oncocytoid renal cell carcinoma in patients who have survived neuroblastoma as a distinct biologic entity has been controversial since its original description in 1999. This is in part because similar oncocytoid renal cell carcinomas have been described in association with other pediatric cancers, and also because other renal cell carcinoma subtypes (such as MiT family translocation renal cell carcinoma) have been described in children who have survived neuroblastoma. We identified an index case of a child who survived medulloblastoma and developed multifocal bilateral oncocytoid renal cell carcinomas with morphology and immunophenotype compatible with eosinophilic solid and cystic renal cell carcinoma (ESC RCC) and demonstrated that both neoplasms harbored distinctive mutations in the TSC1/TSC2 genes. Remarkably, the child's remaining bilateral multifocal renal neoplasms completely responded to MTOR inhibitor therapy without need for further surgery. To confirm our hypothesis that oncocytoid renal cell carcinomas after childhood cancer represent ESC RCC, we obtained formalin-fixed paraffin-embedded tissue blocks from 2 previously published cases of oncocytoid renal cell carcinoma after neuroblastoma, confirmed that the morphology and immunophenotype was consistent with ESC RCC, and demonstrated that both cases harbored somatic TSC gene mutations. Both expressed markers previously associated with neoplasms harboring TSC gene mutations, glycoprotein nonmetastatic B, and cathepsin K. Of note, one of these patients had 2 ESC RCC which harbored distinctive TSC2 mutations, while the background kidney of the other patient had multiple small cysts lined by similar oncocytoid cells which showed loss of TSC2 protein. We then reviewed 3 of 4 cases from the original 1999 report of oncocytoid renal cell carcinomas after neuroblastoma, found that all 3 demonstrated morphology (including basophilic cytoplasmic stippling) that is characteristic of ESC RCC, showed that all 3 overexpressed glycoprotein nonmetastatic B, and showed that both cases with adequate material demonstrated loss of TSC2 protein and expressed cytokeratin 20 and cathepsin K by immunohistochemistry. In summary, "oncocytoid renal cell carcinomas after neuroblastoma" represent ESC RCC which are often multifocal in patients who have survived childhood cancer, likely representing an incompletely characterized tumor predisposition syndrome. MTOR-targeted therapy represents an effective therapeutic option for such patients to preserve functional nephrons.
自 1999 年首次描述以来,患有神经母细胞瘤幸存下来的患者中具有独特生物学实体的肾嗜酸细胞瘤的概念一直存在争议。这在一定程度上是因为在其他儿科癌症中也描述了类似的嗜酸细胞瘤,并且因为在患有神经母细胞瘤的儿童中也描述了其他肾细胞癌亚型(如 MiT 家族易位肾细胞癌)。我们鉴定了一名患有髓母细胞瘤幸存下来的儿童病例,该儿童患有多发双侧嗜酸细胞瘤性肾细胞癌,其形态和免疫表型与嗜酸性实性和囊性肾细胞癌(ESC RCC)相符,并证明两种肿瘤均存在 TSC1/TSC2 基因的独特突变。值得注意的是,该儿童其余双侧多发性肾肿瘤完全对 MTOR 抑制剂治疗有反应,无需进一步手术。为了证实我们的假设,即儿童癌症后的嗜酸细胞瘤性肾细胞癌代表 ESC RCC,我们从 2 例先前发表的神经母细胞瘤后嗜酸细胞瘤性肾细胞癌病例中获得了福尔马林固定石蜡包埋组织块,证实了形态和免疫表型与 ESC RCC 一致,并证明了这两种情况均存在体细胞 TSC 基因突变。两者均表达了先前与携带 TSC 基因突变的肿瘤相关的标志物,即糖蛋白非转移性 B 和组织蛋白酶 K。值得注意的是,其中一名患者有 2 个 ESC RCC,其携带独特的 TSC2 突变,而另一名患者的背景肾脏有多个由类似嗜酸细胞组成的小囊肿,这些细胞失去了 TSC2 蛋白。然后,我们回顾了原始 1999 年神经母细胞瘤后嗜酸细胞瘤性肾细胞癌报告中的 4 例中的 3 例,发现所有 3 例均表现出 ESC RCC 的特征性形态(包括嗜碱性细胞质点状),均显示过度表达糖蛋白非转移性 B,并且在有足够材料的 2 例中均显示 TSC2 蛋白缺失,并通过免疫组化显示表达细胞角蛋白 20 和组织蛋白酶 K。总之,“神经母细胞瘤后嗜酸细胞瘤性肾细胞癌”代表 ESC RCC,它们在患有儿童癌症幸存下来的患者中通常是多灶性的,可能代表一种尚未完全描述的肿瘤易感性综合征。针对 MTOR 的靶向治疗是此类患者保留功能性肾单位的有效治疗选择。
