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Discordance in HER2 gene amplification in circulating and disseminated tumor cells in patients with operable breast cancer

机译:可手术乳腺癌患者循环和弥散性肿瘤细胞HER2基因扩增的不一致

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AbstractHuman epidermal growth factor receptor 2 (HER2) gene amplification in circulating tumor cells (CTCs) and disseminated tumor cells (DTCs) might be useful for modifying Herceptin therapy in breast cancer. In the process of investigating the utility of a microfluidic platform for detecting HER2 gene amplification in these cells, we observed novel results on discordance of HER2 status. Peripheral blood (8.5 mL) and bone marrow (BM) (7.5–10 mL) were collected prospectively from patients with clinical stages I–IV breast cancer. Mononuclear cells were recovered, stained with cytokeratin (CK), CD45, and DAPI, and processed through microfluidic channels for fluorescence in situ hybridization (FISH). A ratio of HER2:CEP17 2 in any CK+/CD45 or CK−/CD45 cell was regarded as positive for HER2 gene amplification. Peripheral blood from 95 patients and BM from 78 patients were studied. We found CK+/CD45−/DAPI+ CTCs in 27.3% of patients. We evaluated HER2 gene amplification by FISH in 88 blood and 78 BM specimens and found HER2+ CTCs in 1 of 9 (11.1%) and HER2+ DTCs (27.2%) in 3 of 11 patients with HER2+ primary tumor. Among patients with a HER2− primary tumor, 5 of 79 had HER2+ CTCs (6.3%) and 14 of 67 had HER2+ DTCs (20.8%). The overall rate of discordance in HER2 status was 15% between primary tumor and CTCs and 28.2% between primary tumor and DTCs. HER2 was amplified in CTCs and DTCs in a portion of both HER2+ and HER2− primary tumors. HER2 discordance was more frequent for DTCs. The clinical implications of evaluating HER2 status in CTCs and DTCs in breast cancer needs to be established in prospective clinical trials. The cell enrichment and extraction microfluidic technology provides a sensitive platform for evaluation of HER2 gene amplification in CTCs and DTCs.
机译:摘要循环肿瘤细胞(CTC)和弥散性肿瘤细胞(DTC)中的人类表皮生长因子受体2(HER2)基因扩增可能对修改乳腺癌的Herceptin治疗有用。在研究用于检测这些细胞中HER2基因扩增的微流体平台的实用性的过程中,我们观察到关于HER2状态不一致的新结果。前瞻性从I–IV期临床乳腺癌患者中收集外周血(8.5 mL)和骨髓(BM)(7.5–10 mL)。回收单核细胞,用细胞角蛋白(CK),CD45和DAPI染色,并通过微流体通道进行荧光原位杂交(FISH)。在任何CK + / CD45或CK- / CD45细胞中,HER2:CEP17的比例> 2被认为是HER2基因扩增阳性的。研究了95例患者的外周血和78例患者的BM。我们在27.3%的患者中发现了CK + / CD45- / DAPI + CTC。我们通过FISH对88份血液和78份BM标本中的HER2基因扩增进行了评估,发现11例HER2 +原发性肿瘤患者中的3例中9例中有1例(11.1%)HER2 + CTCs和27.2%发现了HER2 + DTCs(27.2%)。在患有HER2-原发性肿瘤的患者中,有79例中有5例具有HER2 + CTC(6.3%),而67例中有14例具有HER2 + DTC(20.8%)。 HER2状态的总体不一致率在原发肿瘤和CTC之间为15%,在原发肿瘤和DTC之间为28.2%。 HER2在部分HER2 +和HER2-原始肿瘤中的CTC和DTC中扩增。 DTC的HER2不一致更为常见。需要在前瞻性临床试验中确定评估乳腺癌CTC和DTC中HER2状态的临床意义。细胞富集和提取微流体技术为评估CTC和DTC中HER2基因扩增提供了一个敏感的平台。

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