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Aneusomy 17 in Breast Cancer: Its Role in HER-2eu Protein Expression and Implication for Clinical Assessment of HER-2eu Status

机译:乳腺癌中的气孔17:在HER-2 / neu蛋白表达中的作用及其对HER-2 / neu状况​​临床评估的意义

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HER-2eu protein overexpression in breast cancer is mostly caused by HER-2eu gene amplification. However, it is unclear whether aneusomy 17 may also play a role. Using immunohistochemistry assay (IHC) with DAKO antibody and manual quantitation, 189 specimens were selected from archival invasive breast cancer specimens, including most IHC-positive and some IHC-negative cases (n = 158 and 31, respectively). They were then analyzed by PathVysion fluorescence in situ hybridization (FISH) assay (Vysis, Inc., Downers Grove, IL) and by an image analyzer (ACIS; ChromaVision Medical Systems, Inc., San Juan Capistrano, CA)–assisted IHC quantitation. Ninety-two cases contained disomy 17 (chromosome 17 centromere, 1.76–2.25 signals per cell) whereas 97 cases had aneusomy 17, including 82 with low polysomy (2.26–3.75 signals per cell), 10 with high polysomy (3.76 signals per cell), and 5 with hypodisomy (1.75 signals per cell). HER-2eu protein expression had the highest correlation with HER-2eu gene dosage (copy number; r = .826), followed by the HER-2eu gene to chromosome 17 ratio (r = .733). The lowest correlation was with the chromosome 17 copy number (r = .307), on which the 10 cases with high polysomy 17 had a disproportionately high impact. The FISH assay using the PathVysion criterion for HER-2eu gene amplification (HER-2eu gene to chromosome 17 ratio, 2.00) achieved higher concordance with ACIS IHC than did an alternative FISH criterion (absolute HER-2eu gene copy number, 4.00 signals per cell). Most ACIS IHC-PathVysion FISH–discordant cases contained disomy or low polysomy 17, whereas all 10 cases with high polysomy 17 had no such discordance. However, two cases with monosomy 17 had ACIS IHC-PathVysion FISH discordance, i.e., with gene amplification, but no protein overexpression. Both cases would have had no gene amplification if the alternative FISH criterion had been used. In conclusion, aneusomy 17 is common in breast cancer. Except in a certain subset of cases, aneusomy 17 probably is not a significant factor for HER-2eu protein expression or for clinical assessment of HER-2eu status.
机译:乳腺癌中的HER-2 / neu蛋白过度表达主要是由HER-2 / neu基因扩增引起的。但是,尚不清楚气孔17是否也可能起作用。使用带有DAKO抗体的免疫组织化学测定(IHC)和手动定量,从档案浸润性乳腺癌样本中选择了189个样本,包括大多数IHC阳性和一些IHC阴性的病例(分别为158和31个)。然后通过PathVysion荧光原位杂交(FISH)测定法(Vysis,Inc.,Downers Grove,IL)和图像分析仪(ACIS; ChromaVision Medical Systems,Inc.,San Juan Capistrano,CA)辅助进行IHC定量分析。 92例包含二体性17(染色体17着丝粒,每细胞1.76–2.25个信号),而97例中性神经病,其中82例具有低多体性(每细胞2.26–3.75信号),10例具有高多体性(每细胞3.76信号) ,以及5个具伪合性(每个细胞1.75个信号)。 HER-2 / neu蛋白表达与HER-2 / neu基因剂量(拷贝数; r = .826)的相关性最高,其次是HER-2 / neu基因与17号染色​​体的比率(r = .733)。最低的相关性是与17号染色​​体的拷贝数(r = .307)有关,这对10个具有17号多态性的病例产生了不成比例的高影响。使用PathVysion准则进行HER-2 / neu基因扩增的FISH分析(HER-2 / neu基因与17号染色​​体的比率为2.00)比其他FISH准则(绝对HER-2 / neu基因拷贝)与ACIS IHC的一致性更高数字,每个单元格为4.00个信号)。大多数ACIS IHC-PathVysion FISH不一致的病例包含二体性或低多态性17,而所有10例具有高多性性17的病例都没有这种不一致。但是,有两个17号单体病患者具有ACIS IHC-PathVysion FISH不一致性,即具有基因扩增,但没有蛋白过表达。如果使用替代的FISH标准,则这两种情况都不会扩增基因。总之,气肿17在乳腺癌中很常见。除某些情况外,气管切开术17可能不是影响HER-2 / neu蛋白表达或临床评估HER-2 / neu状态的重要因素。

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