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HER2 protein overexpression and gene amplification in upper urinary tract transitional cell carcinoma: systematic analysis applying tissue microarray technique.

机译:上尿路移行细胞癌中HER2蛋白的过表达和基因扩增:应用组织芯片技术进行系统分析。

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OBJECTIVES: To investigate HER2 (c-erbB-2) protein overexpression and HER2 gene amplification in upper urinary tract transitional cell carcinoma (TCC) with respect to its association with tumor grade and stage, as well as the prognostic significance. METHODS: A total of 53 consecutive TCC specimens were analyzed immunohistochemically (HercepTest) and with fluorescence in situ hybridization applying a tissue microarray technique. RESULTS: Overall, HER2 immunoreactivity (expression) was detected in 28 of 53 TCC specimens and tended to be stronger in high-stage (8 [36%] of 22 pT1 versus 20 [65%] of 31 pT2-T3; P = 0.06) and high-grade (11 [39%] of 28 low-grade versus 17 [68%] of 25 high-grade; P = 0.054) tumors. Weak overexpression (HercepTest score 2+) was seen in 9 cases (17%) and was associated with angioinvasion (P = 0.02) and had independent prognostic significance with respect to metastasis-free survival (risk ratio 9.6; P = 0.03). Low HER2 amplification was present in four TCC specimens (9%), with HER2/chromosome 17 ratios of 2.03, 2.77, 2.91, and 3.39, and polysomy of chromosome 17 was present in another 3 cases (7%). HER2 amplification and/or polysomy of chromosome 17 prevailed in high-stage (0 [0%] of 20 pT1 versus 7 [27%] of 26 pT2-T3; P = 0.01) and high-grade (1 [4%] of 24 low-grade versus 6 [27%] of 22 high-grade; P = 0.04) tumors, but lacked independent prognostic significance. Of nine TCC specimens with weak HER2 overexpression (HercepTest score 2+), 3 (33%) showed low HER2 amplification and two others had polysomy of chromosome 17. CONCLUSIONS: HER2 overexpression and HER2 gene amplification were infrequent in our series. Thus, only a small number of patients with upper urinary tract TCC might benefit from HER2-targeted (Herceptin) cancer therapy.
机译:目的:探讨上尿路移行细胞癌(TCC)中HER2(c-erbB-2)蛋白的过度表达和HER2基因的扩增与肿瘤分级和分期的关系,以及预后的意义。方法:对53个连续的TCC标本进行了免疫组织化学(HercepTest)分析,并采用组织芯片技术进行了荧光原位杂交。结果:总体而言,在53个TCC标本中有28个检测到HER2免疫反应(表达),并在较高阶段趋于增强(22 pT1中的8个[36%],而31 pT2-T3中的20个[65%]; P = 0.06 )和高等级(28个低等级中的11个[39%]对25个高等级中的17个[68%]; P = 0.054)肿瘤。 9例(17%)表现为弱的过表达(HercepTest得分2+),与血管浸润相关(P = 0.02),并且在无转移生存方面具有独立的预后意义(风险比9.6; P = 0.03)。在4个TCC标本中存在低HER2扩增(9%),HER2 /染色体17的比率为2.03、2.77、2.91和3.39,另外3例(7%)存在17号染色​​体多态性。第17号染色​​体的HER2扩增和/或多态性在高阶段(20 pT1的0 [0%]比26 pT2-T3的7 [27%]; P = 0.01)和高级别(1 [4%])流行。 24个低度肿瘤与22个高度肿瘤中的6个[27%]; P = 0.04)肿瘤,但缺乏独立的预后意义。在9个HER2过表达较弱的TCC标本中(HercepTest得分2+),其中3个(33%)显示出HER2扩增低,另外2个标本具有17号染色​​体多态性。因此,只有少数患有上尿路TCC的患者可以受益于靶向HER2的(赫赛汀)癌症治疗。

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