Department of Diagnostic and Public Health, Section of Pathology, University of Verona, Italy.
Department of Pathology, Pederzoli Hospital, Peschiera del Garda, Italy.
Pathology. 2020 Apr;52(3):297-309. doi: 10.1016/j.pathol.2019.11.006. Epub 2020 Feb 24.
Recently cabozantinib, a tyrosine kinase inhibitor with activity against VEGF, MET, AXL, and downregulating cathepsin K in vitro, has been proposed for the treatment of advanced clear and non-clear renal cell carcinomas. Since it is well known that cathepsin K is expressed in the majority of MiT family translocation renal cell carcinomas, we investigated cathepsin K, MET, AXL, and VEGF in a large series of those tumours, looking for possible predictive markers. We collected the clinicopathological features of 34 genetically confirmed MiT family translocation renal cell carcinomas [26 Xp11 and 8 t(6;11) renal cell carcinomas] and studied them using an immunohistochemical panel including PAX8, cathepsin K, HMB45, Melan-A, CD68 (PG-M1), CK7, CA9, MET, AXL and by FISH for VEGFA and MET. Cathepsin K was expressed in 14 of 26, HMB45 in 8 of 25, and Melan-A in 4 of 23 Xp11 renal cell carcinomas, whereas labelling for CK7 and CA9 was minimal. In t(6;11) renal cell carcinoma, cathepsin K and melanogenesis markers were constantly positive, whereas CK7 and CA9 were negative. None of the 34 carcinomas showed CD68 (PG-M1) and AXL expression. One aggressive Xp11 renal cell carcinoma showed increased VEGFA gene copy number (4-5 copies) with concurrent gains of TFE3 and TFEB. None of the 34 carcinomas showed MET gene amplification, whereas staining for MET was found in 7 of 8 t(6;11) and in 16 of 24 Xp11 renal cell carcinomas, and in the latter cases, when the expression was >50%, correlated with aggressiveness (p=0.0049). In Xp11 renal cell carcinomas, the aggressiveness was also correlated with larger tumour size (p=0.0008) and the presence of necrosis (p=0.027) but not nucleolar grading (p=1). Interestingly, in patients with tumours exhibiting two of three parameters (necrosis, larger tumour size and MET immunolabelling >50%) an aggressive clinical behaviour was observed in 88% of cases. In conclusion, cathepsin K, CD68 (PG-M1), CK7, CA9, and PAX8 is a useful panel for the diagnosis. Larger tumour size, the presence of necrosis and MET immunohistochemical expression correlate with aggressive behaviour in Xp11 renal cell carcinomas, especially in combination. VEGF, MET, cathepsin K but not AXL may be potential predictive markers for targeted therapy in MiT family translocation renal cell carcinomas.
最近,一种针对 VEGF、MET、AXL 和下调组织蛋白酶 K 的酪氨酸激酶抑制剂卡博替尼(cabozantinib)被提议用于治疗晚期透明和非透明肾细胞癌。由于众所周知,组织蛋白酶 K 在大多数 MiT 家族易位肾细胞癌中表达,我们研究了 CATHEPSIN K、MET、AXL 和 VEGF 在一系列这些肿瘤中的表达,寻找可能的预测标志物。我们收集了 34 例经基因证实的 MiT 家族易位肾细胞癌的临床病理特征[26 例 Xp11 和 8 例 t(6;11)肾细胞癌],并使用包括 PAX8、CATHEPSIN K、HMB45、MELAN-A、CD68(PG-M1)、CK7、CA9、MET、AXL 和 FISH 检测 VEGFA 和 MET 的免疫组织化学小组进行研究。26 例 Xp11 肾细胞癌中有 14 例表达 CATHEPSIN K,25 例中有 8 例表达 HMB45,23 例中有 4 例表达 MELAN-A,而 CK7 和 CA9 的标记物很少。在 t(6;11)肾细胞癌中,CATHEPSIN K 和黑色素生成标志物始终为阳性,而 CK7 和 CA9 为阴性。34 例癌中均无 CD68(PG-M1)和 AXL 表达。1 例侵袭性 Xp11 肾细胞癌表现出 VEGFA 基因拷贝数增加(4-5 个拷贝),同时伴有 TFE3 和 TFEB 的获得。34 例癌中均未发现 MET 基因扩增,而在 8 例 t(6;11)和 24 例 Xp11 肾细胞癌中发现了 MET 染色,在后一种情况下,当表达>50%时,与侵袭性相关(p=0.0049)。在 Xp11 肾细胞癌中,侵袭性还与较大的肿瘤大小(p=0.0008)和坏死的存在(p=0.027)相关,但与核仁分级无关(p=1)。有趣的是,在具有三个参数(坏死、较大肿瘤大小和 MET 免疫标记>50%)中的两个的患者中,88%的病例观察到侵袭性临床行为。总之,CATHEPSIN K、CD68(PG-M1)、CK7、CA9 和 PAX8 是一种有用的诊断面板。较大的肿瘤大小、坏死的存在和 MET 的免疫组织化学表达与 Xp11 肾细胞癌的侵袭性行为相关,尤其是在组合时。VEGF、MET、CATHEPSIN K 但不是 AXL 可能是 MiT 家族易位肾细胞癌靶向治疗的潜在预测标志物。
