Biological Markers Predictive of Invasive Recurrence in DCIS.

Clinical medicine. Oncology Pub Date : 2008-01-01 Epub Date: 2008-01-22
Sharon Nofech-Mozes, Jacqueline Spayne, Eileen Rakovitch, Harriette J Kahn, Arun Seth, Jean-Phillippe Pignol, Lavina Lickley, Lawrence Paszat, Wedad Hanna
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Abstract

DCIS is a heterogeneous group of non-invasive cancers of the breast characterized by various degrees of differentiation and unpredictable propensity for transformation into invasive carcinoma. We examined the expression and prognostic value of 9 biological markers with a potential role in tumor progression in 133 patients with pure DCIS treated with breast conserving surgery alone, between 1982-2000. Histology was reviewed and immunohistochemical staining was performed. Pearson correlation coefficient was used to determine the associations between markers and histopathological features. Univariate and multivariate analysis examined associations between time to recurrence and clinicopathologic features and biological markers.Median age at diagnosis was 55 years (25-85). With a median follow up of 8.91 years, 41/133 patients recurred (21 as invasive recurrence). In this cohort 13.5% had low, 43% intermediate and 42% high nuclear grade. Comedo necrosis was found in 65% of cases. Expression of ER (62.4%), PR (55.6%), HER2/neu (31.6%), MIB1 (39.8%), p53 (22.6%), p21 (39.8%), Cyclin D1 (95.5%) calgranulin (20.5%), psoriasin (12%), was found in DCIS. HER2/neu was overexpressed in 45% that recurred as DCIS and 42.9% that recurred as invasive cancer, and only in 26.1% in cases that never recurred. On univariate analysis, HER2/neu overexpression was the only marker associated with an increased risk for any recurrence (p = 0.044). The hazard ratio for recurrence for HER2/neu positive DCIS was 1.927 (confidence interval 1.016-3.653) compared to HER2 negative DCIS. On multivariate analysis, HER2/neu overexpression remained the only independent variable significantly associated with any recurrence (p = 0.014) and with invasive recurrence (p = 0.044).This data suggest that HER2/neu testing may become an important parameter in the management of DCIS and the treatment of cases with positive HER2/neu status could be modified accordingly, similar to the current approach for HER2/neu positive invasive disease.

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预测DCIS侵袭性复发的生物学标志物。
DCIS是一种异质性的非浸润性乳腺癌,其特征是不同程度的分化和不可预测的向浸润性癌转化的倾向。在1982-2000年间,我们检测了133例单纯DCIS保乳手术患者的9种生物标志物的表达和预后价值,这些标志物在肿瘤进展中具有潜在作用。组织学检查,免疫组织化学染色。使用Pearson相关系数来确定标记物与组织病理学特征之间的关联。单因素和多因素分析检查了复发时间与临床病理特征和生物标志物之间的关系。诊断时的中位年龄为55岁(25-85岁)。中位随访8.91年,133例患者中有41例复发(21例为侵袭性复发)。在该队列中,13.5%为低级别,43%为中级别,42%为高级别。65%的病例出现粉刺样坏死。ER(62.4%)、PR(55.6%)、HER2/neu(31.6%)、MIB1(39.8%)、p53(22.6%)、p21(39.8%)、Cyclin D1(95.5%)、calgranulin(20.5%)、牛皮癣蛋白(12%)在DCIS中表达。复发为DCIS的患者中有45% HER2/neu过表达,复发为浸润性癌的患者中有42.9% HER2/neu过表达,而从未复发的患者中只有26.1%的HER2/neu过表达。在单因素分析中,HER2/neu过表达是唯一与复发风险增加相关的标志物(p = 0.044)。与HER2阴性DCIS相比,HER2/neu阳性DCIS复发的风险比为1.927(置信区间为1.016-3.653)。在多变量分析中,HER2/neu过表达仍然是唯一与任何复发(p = 0.014)和侵袭性复发(p = 0.044)显著相关的自变量。这些数据提示,HER2/neu检测可能成为DCIS管理的一个重要参数,对HER2/neu阳性病例的治疗可以进行相应的修改,类似于目前对HER2/neu阳性侵袭性疾病的治疗方法。
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