拓扑异构酶IIα基因扩增预示HER-2/neu扩增型乳腺癌患者对量身定制的、剂量递增的蒽环类辅助化疗有良好的治疗反应:斯堪的纳维亚乳腺癌研究组9401试验
Topoisomerase IIalpha gene amplification predicts favorable treatment response to tailored and dose-escalated anthracycline-based adjuvant chemotherapy in HER-2/neu-amplified breast cancer: Scandinavian Breast Group Trial 9401.
作者信息
Tanner Minna, Isola Jorma, Wiklund Tom, Erikstein Björn, Kellokumpu-Lehtinen Pirkko, Malmström Per, Wilking Nils, Nilsson Jonas, Bergh Jonas
机构信息
Laboratory of Cancer Biology, Institute of Medical Technology, and Department of Oncology, Tampere University and Tampere University Hospital, Tampere, Finland.
出版信息
J Clin Oncol. 2006 Jun 1;24(16):2428-36. doi: 10.1200/JCO.2005.02.9264. Epub 2006 May 8.
PURPOSE
Amplification of the HER-2/neu and topoisomerase IIalpha (TOP2A) genes has been linked to the effects of anthracyclines. Their role in predicting the outcome of anthracycline-based adjuvant chemotherapy for breast cancer patients has remained controversial.
PATIENTS AND METHODS
The present substudy of the Scandinavian Breast Group trial 9401, in which an epirubicin-based regimen (nine courses of tailored and dose-escalated fluorouracil, epirubicin, and cyclophosphamide [FEC]) was compared with three or four courses of standard FEC followed by bone marrow-supported high-dose chemotherapy (cyclophosphamide, thiotepa, and carboplatin), included high-risk breast cancer patients (with eight or more positive axillary lymph nodes or at least five nodes with additional poor prognostic indicators). Amplification of HER-2/neu was determined retrospectively in paraffin-embedded tumor tissue sections by chromogenic in situ hybridization. TOP2A was tested only in HER-2/neu-amplified tumors.
RESULTS
HER-2/neu amplification alone, which was present in 32.7% of the tumors, was a strong prognostic factor for short relapse-free (P = .0034) and overall survival (P = .0008) but showed no direct association with treatment assignment. TOP2A coamplification, which was present in 37% of HER-2/neu-amplified tumors, was associated with better relapse-free survival in patients treated with tailored and dose-escalated FEC (hazard ratio [HR] = 0.45; P = .049). A statistical multivariate Cox's regression analysis confirmed the predictive significance of TOP2A coamplification (HR = 0.30; P = .020) in HER-2/neu-amplified tumors. There was no such association in patients with HER-2/neu-amplified tumors without TOP2A gene amplification.
CONCLUSION
Coamplification of HER-2/neu and TOP2A may define a subgroup of high-risk breast cancer patients who benefit from individually tailored and dose-escalated adjuvant anthracyclines.
目的
HER-2/neu和拓扑异构酶IIα(TOP2A)基因的扩增与蒽环类药物的疗效相关。它们在预测乳腺癌患者蒽环类辅助化疗结局中的作用仍存在争议。
患者与方法
斯堪的纳维亚乳腺癌组试验9401的本亚组研究中,将基于表柔比星的方案(九个疗程的个体化且剂量递增的氟尿嘧啶、表柔比星和环磷酰胺[FEC])与三或四个疗程的标准FEC随后进行骨髓支持的高剂量化疗(环磷酰胺、噻替派和卡铂)进行比较,纳入了高危乳腺癌患者(腋窝淋巴结阳性八个或更多或至少五个淋巴结伴有其他不良预后指标)。通过显色原位杂交对石蜡包埋的肿瘤组织切片进行回顾性HER-2/neu扩增检测。仅在HER-2/neu扩增的肿瘤中检测TOP2A。
结果
单独的HER-2/neu扩增存在于32.7%的肿瘤中,是无复发生存期短(P = 0.0034)和总生存期短(P = 0.0008)的强预后因素,但与治疗分配无直接关联。TOP2A共扩增存在于37%的HER-2/neu扩增肿瘤中,与接受个体化且剂量递增FEC治疗的患者更好的无复发生存期相关(风险比[HR] = 0.45;P = 0.049)。多变量Cox回归分析证实TOP2A共扩增在HER-2/neu扩增肿瘤中的预测意义(HR = 0.30;P = 0.020)。在无TOP2A基因扩增的HER-2/neu扩增肿瘤患者中无此关联。
结论
HER-2/neu和TOP2A的共扩增可能定义了一组高危乳腺癌患者亚组,他们从个体化且剂量递增的辅助蒽环类药物中获益。
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