首页> 外文期刊>The lancet oncology >Prediction of late distant recurrence in patients with oestrogen-receptor-positive breast cancer: A prospective comparison of the breast-cancer index (BCI) assay, 21-gene recurrence score, and IHC4 in the TransATAC study population
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Prediction of late distant recurrence in patients with oestrogen-receptor-positive breast cancer: A prospective comparison of the breast-cancer index (BCI) assay, 21-gene recurrence score, and IHC4 in the TransATAC study population

机译:雌激素受体阳性乳腺癌患者晚期远距离复发的预测:TransATAC研究人群中乳腺癌指数(BCI)测定,21基因复发评分和IHC4的前瞻性比较

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Background: Biomarkers to improve the risk-benefit of extended adjuvant endocrine therapy for late recurrence in patients with oestrogen-receptor-positive breast cancer would be clinically valuable. We compared the prognostic ability of the breast-cancer index (BCI) assay, 21-gene recurrence score (Oncotype DX), and an immunohistochemical prognostic model (IHC4) for both early and late recurrence in patients with oestrogen-receptor-positive, node-negative (N0) disease who took part in the Arimidex, Tamoxifen, Alone or in Combination (ATAC) clinical trial. Methods: In this prospective comparison study, we obtained archival tumour blocks from the TransATAC tissue bank from all postmenopausal patients with oestrogen-receptor-positive breast cancer from whom the 21-gene recurrence score and IHC4 values had already been derived. We did BCI analysis in matched samples with sufficient residual RNA using two BCI models-cubic (BCI-C) and linear (BCI-L)-using previously validated cutoffs. We assessed prognostic ability of BCI for distant recurrence over 10 years (the primary endpoint) and compared it with that of the 21-gene recurrence score and IHC4. We also tested the ability of the assays to predict early (0-5 years) and late (5-10 years) distant recurrence. To assess the ability of the biomarkers to predict recurrence beyond standard clinicopathological variables, we calculated the change in the likelihood-ratio χ2 (LR-δχ2) from Cox proportional hazards models. Findings: Suitable tissue was available from 665 patients with oestrogen-receptor-positive, N0 breast cancer for BCI analysis. The primary analysis showed significant differences in risk of distant recurrence over 10 years in the categorical BCI-C risk groups (p0·0001) with 6·8% (95% CI 4·4-10·0) of patients in the low-risk group, 17·3% (12·0-24·7) in the intermediate group, and 22·2% (15·3-31·5) in the high-risk group having distant recurrence. The secondary analysis showed that BCI-L was a much stronger predictor for overall (0-10 year) distant recurrence compared with BCI-C (interquartile HR 2·30 [95% CI 1·62-3·27]; LR-δχ2=22·69; p0·0001). When compared with BCI-L, the 21-gene recurrence score was less predictive (HR 1·48 [95% CI 1·22-1·78]; LR-δχ2=13·68; p=0·0002) and IHC4 was similar (HR 1·69 [95% CI 1·51-2·56]; LR-δχ2=22·83; p0·0001). All further analyses were done with the BCI-L model. In a multivariable analysis, all assays had significant prognostic ability for early distant recurrence (BCI-L HR 2·77 [95% CI 1·63-4·70], LR-δχ2=15·42, p0·0001; 21-gene recurrence score HR 1·80 [1·42-2·29], LR-δχ2=18·48, p0·0001; IHC4 HR 2·90 [2·01-4·18], LR-δχ2=29·14, p0·0001); however, only BCI-L was significant for late distant recurrence (BCI-L HR 1·95 [95% CI 1·22-3·14], LR-δχ2=7·97, p=0·0048; 21-gene recurrence score HR 1·13 [0·82-1·56], LR-δχ2=0·48, p=0·47; IHC4 HR 1·30 [0·88-1·94], LR-δχ2=1·59, p=0·20). Interpretation: BCI-L was the only significant prognostic test for risk of both early and late distant recurrence and identified two risk populations for each timeframe. It could help to identify patients at high risk for late distant recurrence who might benefit from extended endocrine or other therapy. Funding: Avon Foundation, National Institutes of Health, Breast Cancer Foundation, US Department of Defense Breast Cancer Research Program, Susan G Komen for the Cure, Breakthrough Breast Cancer through the Mary-Jean Mitchell Green Foundation, AstraZeneca, Cancer Research UK, and the National Institute for Health Research Biomedical Research Centre at the Royal Marsden (London, UK).
机译:背景:改善雌激素受体阳性乳腺癌患者晚期复发辅助内分泌治疗风险的生物标志物将具有临床价值。我们比较了乳腺癌指数(BCI)分析,21基因复发评分(Oncotype DX)和免疫组化预后模型(IHC4)对雌激素受体阳性,淋巴结转移的早期和晚期患者的预后能力参与Arimidex,他莫昔芬,单独治疗或联合治疗(ATAC)临床试验的阴性(N0)疾病。方法:在这项前瞻性比较研究中,我们从所有已经绝经后的雌激素受体阳性乳腺癌患者的TransATAC组织库中获得了档案肿瘤块,这些患者已经获得了21个基因的复发评分和IHC4值。我们使用先前验证的临界值,使用立方(BCI-C)和线性(BCI-L)这两种BCI模型,在具有足够残留RNA的匹配样品中进行了BCI分析。我们评估了10年后BCI远处复发的预后能力(主要终点),并将其与21基因复发评分和IHC4的预后能力进行了比较。我们还测试了预测早期(0-5年)和晚期(5-10年)远处复发的能力。为了评估生物标志物预测超出标准临床病理变量的复发的能力,我们从Cox比例风险模型计算了似然比χ2(LR-δχ2)的变化。结果:从665例雌激素受体阳性N0乳腺癌患者中可获得合适的组织用于BCI分析。初步分析显示,分类BCI-C风险组(p <0·0001)在10年内远距离复发的风险存在显着差异,其中BCI-C风险组的患者有6·8%(95%CI 4·4-10·0)。低危组中,远处复发的中危组为17·3%(12·0-24·7),高危组为22·2%(15·3-31·5)。次要分析显示,与BCI-C相比,BCI-L是整体(0-10年)远距离复发的更强预测指标(四分位间HR 2·30 [95%CI 1·62-3·27];LR-δχ2 = 22·69; p <0·0001)。与BCI-L相比,21基因复发评分的预测性较低(HR 1·48 [95%CI 1·22-1·78];LR-δχ2= 13·68; p = 0·0002)和IHC4相似(HR 1·69 [95%CI 1·51-2·56];LR-δχ2= 22·83; p <0·0001)。所有进一步的分析都是使用BCI-L模型进行的。在多变量分析中,所有测定均具有早期远处复发的显着预后能力(BCI-L HR 2·77 [95%CI 1·63-4·70],LR-δχ2= 15·42,p <0·0001; 21基因复发评分HR 1·80 [1·42-2·29],LR-δχ2= 18·48,p <0·0001; IHC4 HR 2·90 [2·01-4·18],LR- δχ2= 29·14,p <0·0001);然而,只有BCI-L对于远处复发具有显着意义(BCI-L HR 1·95 [95%CI 1·22-3·14],LR-δχ2= 7·97,p = 0·0048; 21个基因复发评分HR 1·13 [0·82-1·56],LR-δχ2= 0·48,p = 0·47; IHC4 HR 1·30 [0·88-1·94],LR-δχ2= 1 ·59,p = 0·20)。解释:BCI-L是唯一的早期和晚期远距离复发风险的重要预后测试,并在每个时间范围内确定了两个风险人群。它可以帮助确定晚期远距离复发的高风险患者,这些患者可能会受益于延长的内分泌或其他疗法。资金来源:雅芳基金会,美国国立卫生研究院,乳腺癌基金会,美国国防部乳腺癌研究计划,Susan G Komen治愈,通过Mary-Jean Mitchell Green基金会突破乳腺癌,阿斯利康,英国癌症研究以及皇家马斯登国家卫生研究所生物医学研究中心(英国伦敦)。

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