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Aurora A is a prognostic marker for breast cancer arising in BRCA2 mutation carriers

机译:Aurora A是BRCA2突变携带者中乳腺癌的预后标志物

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AbstractOverexpression of the Aurora A kinase has been shown to have prognostic value in breast cancer. Previously, we showed a significant association between AURKA gene amplification and BRCA2 mutation in breast cancer. The aim of this study was to assess the prognostic impact of Aurora A overexpression on breast cancer arising in BRCA2 mutation carriers. Aurora A expression was evaluated by immunohistochemistry on breast tumour tissue microarrays from 107 BRCA2 999del5 mutation carriers and 284 of sporadic origin. Prognostic value of Aurora A nuclear staining was estimated in relation to clinical markers and adjuvant treatment, using multivariate Cox's proportional hazards ratio regression model. BRCA2 wild-type allele loss was measured by TaqMan in BRCA2 mutated tumour samples. All statistical tests were two sided. Multivariate analysis of breast cancer-specific survival, including proliferative markers and treatment, indicated independent prognostic value of Aurora A nuclear staining for BRCA2 mutation carriers (hazards ratio = 7.06; 95% confidence interval = 1.23–40.6; p = 0.028). Poor breast cancer-specific survival of BRCA2 mutation carriers was found to be significantly associated with combined Aurora A nuclear expression and BRCA2 wild type allele loss in tumours (p  0.001). Multivariate analysis indicated independent prognostic value of both positive Aurora A nuclear staining (hazards ratio = 10.09; 95% confidence interval = 1.19–85.4, p = 0.034) and BRCA2 wild type allele loss (hazards ratio = 9.63; 95% confidence interval = 1.81–51.0, p = 0.008) for BRCA2 mutation carriers. Aurora A nuclear expression was found to be a significant prognostic marker for BRCA2 mutation carriers, independent of clinical parameters and adjuvant treatment. Our conclusion is that treatment benefits for BRCA2 mutation carriers and sporadic breast cancer patients with Aurora A positive tumours may be enhanced by giving attention to Aurora A targeted treatment.
机译:摘要极光A激酶的过表达已显示对乳腺癌具有预后价值。以前,我们显示了乳腺癌中AURKA基因扩增与BRCA2突变之间的显着关联。这项研究的目的是评估Aurora A过表达对BRCA2突变携带者中乳腺癌的预后影响。通过免疫组织化学在来自107个BRCA2 999del5突变携带者和284个散发性起源的乳腺肿瘤组织微阵列上评估Aurora A的表达。使用多变量Cox比例风险比回归模型,评估了Aurora A核染色与临床标志物和辅助治疗有关的预后价值。通过TaqMan在BRCA2突变的肿瘤样品中测量了BRCA2野生型等位基因的丢失。所有统计检验都是两面的。乳腺癌特异性存活的多变量分析,包括增殖标志物和治疗,表明Aurora A核染色对BRCA2突变携带者具有独立的预后价值(危险比= 7.06; 95%置信区间= 1.23-40.6; p = 0.028)。发现BRCA2突变携带者的乳腺癌特异性生存不良与肿瘤中合并的Aurora A核表达和BRCA2野生型等位基因缺失显着相关(p <0.001)。多变量分析显示阳性Aurora A核染色(危险比= 10.09; 95%置信区间= 1.19-85.4,p = 0.034)和BRCA2野生型等位基因缺失(危险比= 9.63; 95%置信区间= 1.81)的独立预后价值–51.0,p = 0.008)用于BRCA2突变携带者。发现Aurora A核表达是BRCA2突变携带者的重要预后标志物,与临床参数和辅助治疗无关。我们的结论是,通过关注Aurora A靶向治疗可以增强BRCA2突变携带者和散发性Aurora A阳性乳腺癌患者的治疗益处。

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