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Different Methods of Pretreatment Ki-67 Labeling Index Evaluation in Core Biopsies of Breast Cancer Patients Treated with Neoadjuvant Chemotherapy and Their Relation to Response to Therapy

机译:不同的预处理Ki-67标记指标评价乳腺癌患者核心活组织检查的核心活组织检查方法及其与疗法反应的关系

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Increased proliferation activity of breast cancer cells evaluated by Ki-67 immunohistochemistry, i.e. a high Ki-67 labeling index (Ki-67 LI), may predict better tumor regression in case of neoadjuvant chemotherapy. Despite recommendations for the evaluation of Ki-67 LI, there are variations in methodology. We assessed the effect of different evaluation methods on the Ki-67 LI in patients with different response to neoadjuvant chemotherapy. Thirty pretreatment core-biopsy samples of patients receiving neoadjuvant docetaxel-epirubicin chemotherapy with or without capecitabine were evaluated for their Ki-67 LI. Pathologic regression was categorized as no regression, partial regression and complete regression, with 10 cases in each category. Three antibodies (MIB1, B56, SP6), 4 observers and 4 methods (counting or estimating on glass slides and counting or estimating on representative digital images) were compared. The Kruskal-Wallis test and analyses of variance were performed to investigate the differences in Ki-67 LIs between different clinical outcomes (tumor regression categories). Breast carcinomas with pathological complete regression had a higher mean Ki-67 LI than tumors not achieving complete regression with any methods, observers and antibodies investigated, although there was a variation between different evaluations in what may represent high proliferation. Estimating the Ki-67 LI on digital images representing the highest proliferation in the core biopsy seemed the best in separating complete responders from non-responders. High Ki-67 LI values were more likely associated with pathological complete regression independently of the method of evaluation used, although the definition of high proliferation is problematic. Estimating the Ki-67 LI may be an adequate method of evaluation.
机译:通过KI-67免疫组织化学评估的乳腺癌细胞的增殖活性增加,即高KI-67标记指数(KI-67 LI),可以预测新辅助化疗的情况下更好的肿瘤回归。尽管对KI-67 LI的评估有建议,但方法论有变化。我们评估了不同评价方法对对新辅助化疗不同反应患者KI-67李的影响。为其Ki-67 Li评估接受Neoadjuvant Docetaxel-Epirubicin化疗的30个预处理核心 - 活组织检查样本。病理回归被分类为没有回归,部分回归和完整的回归,每个类别中有10例。比较了三种抗体(MIB1,B56,SP6),4个观察者和4种方法(计数或估算玻璃载玻片并计数或估算代表数字图像)。进行kruskal-wallis测试和方差分析以研究不同临床结果(肿瘤回归类别)之间的KI-67 LIS的差异。具有病理完全回归的乳腺癌具有更高的平均ki-67锂,而不是肿瘤,肿瘤未与任何方法,观察者和抗体进行完全回归,尽管在可能代表高增殖的不同评价之间存在不同的评价之间的变化。估算代表核心活检中最高增殖的数字图像的Ki-67 Li似乎是分离非响应者的完整响应者。尽管高增殖的定义是有问题的,但高ki-67锂值与病态完全回归更可能与病态完全回归相关。估计KI-67 LI可能是一种充分的评价方法。

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