高增殖率可预测早期乳腺癌新辅助化疗的病理完全缓解
High Proliferation Predicts Pathological Complete Response to Neoadjuvant Chemotherapy in Early Breast Cancer.
作者信息
Alba Emilio, Lluch Ana, Ribelles Nuria, Anton-Torres Antonio, Sanchez-Rovira Pedro, Albanell Joan, Calvo Lourdes, García-Asenjo Jose Antonio Lopez, Palacios Jose, Chacon Jose Ignacio, Ruiz Amparo, De la Haba-Rodriguez Juan, Segui-Palmer Miguel A, Cirauqui Beatriz, Margeli Mireia, Plazaola Arrate, Barnadas Agusti, Casas Maribel, Caballero Rosalia, Carrasco Eva, Rojo Federico
机构信息
Virgen de la Victoria University Hospital, Málaga, Spain
Valencia University Hospital, Valencia, Spain.
出版信息
Oncologist. 2016 Feb;21(2):150-5. doi: 10.1634/theoncologist.2015-0312. Epub 2016 Jan 19.
BACKGROUND
In the neoadjuvant setting, changes in the proliferation marker Ki67 are associated with primary endocrine treatment efficacy, but its value as a predictor of response to chemotherapy is still controversial.
PATIENTS AND METHODS
We analyzed 262 patients with centralized basal Ki67 immunohistochemical evaluation derived from 4 GEICAM (Spanish Breast Cancer Group) clinical trials of neoadjuvant chemotherapy for breast cancer. The objective was to identify the optimal threshold for Ki67 using the receiver-operating characteristic curve method to maximize its predictive value for chemotherapy benefit. We also evaluated the predictive role of the defined Ki67 cutoffs for molecular subtypes defined by estrogen receptor (ER) and human epidermal growth factor receptor 2 (HER2).
RESULTS
A basal Ki67 cutpoint of 50% predicted pathological complete response (pCR). Patients with Ki67 >50% achieved a pCR rate of 40% (36 of 91) versus a pCR rate of 19% in patients with Ki67 ≤ 50% (33 of 171) (p = .0004). Ki67 predictive value was especially relevant in ER-HER2- and ER-HER2+ patients (pCR rates of 42% and 64%, respectively, in patients with Ki67 >50% versus 15% and 45%, respectively, in patients with Ki67 ≤ 50%; p = .0337 and .3238, respectively). Both multivariate analyses confirmed the independent predictive value of the Ki67 cutpoint of 50%.
CONCLUSION
Basal Ki67 proliferation index >50% should be considered an independent predictive factor for pCR reached after neoadjuvant chemotherapy, suggesting that cell proliferation is a phenomenon closely related to chemosensitivity. These findings could help to identify a group of patients with a potentially favorable long-term prognosis.
IMPLICATIONS FOR PRACTICE
The use of basal Ki67 status as a predictive factor of chemotherapy benefit could facilitate the identification of a patient subpopulation with high probability of achieving pathological complete response when treated with primary chemotherapy, and thus with a potentially favorable long-term prognosis.
背景
在新辅助治疗中,增殖标志物Ki67的变化与原发性内分泌治疗疗效相关,但其作为化疗反应预测指标的价值仍存在争议。
患者与方法
我们分析了262例患者,这些患者来自西班牙乳腺癌研究组(GEICAM)的4项乳腺癌新辅助化疗临床试验,其基础Ki67免疫组化评估已集中化。目的是使用受试者工作特征曲线法确定Ki67的最佳阈值,以最大化其对化疗获益的预测价值。我们还评估了所定义的Ki67临界值对由雌激素受体(ER)和人表皮生长因子受体2(HER2)定义的分子亚型的预测作用。
结果
基础Ki67切点为50%可预测病理完全缓解(pCR)。Ki67>50%的患者pCR率为40%(91例中的36例),而Ki67≤50%的患者pCR率为19%(171例中的33例)(p = 0.0004)。Ki67的预测价值在ER-HER2-和ER-HER2+患者中尤为显著(Ki67>50%的患者pCR率分别为42%和64%,而Ki67≤50%的患者pCR率分别为15%和45%;p分别为0.0337和0.3238)。两项多因素分析均证实了Ki67切点为50%的独立预测价值。
结论
基础Ki67增殖指数>50%应被视为新辅助化疗后达到pCR的独立预测因素,这表明细胞增殖是一种与化疗敏感性密切相关的现象。这些发现有助于识别一组具有潜在良好长期预后的患者。
对实践的启示
将基础Ki67状态用作化疗获益的预测因素,有助于识别在接受原发性化疗时极有可能实现病理完全缓解的患者亚群,从而具有潜在良好的长期预后。
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