The prognostic value of stem cell markers in triple-negative breast cancer

Szintia Almási, Ágnes Nagy, Tibor Krenacs, Tamás Lantos, T. Zombori, Gábor Cserni
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Abstract

Among the many consecutive theories of cancer, the stem cell theory is currently the most accepted one. Cancer stem cells are located in small niches with specific environment, renew themselves and are believed to be responsible for many recurrences. They can be highlighted with stem cell markers, but often these markers also label tumor cells, and this may represent a phenotypical change associated with prognosis. In this study, we attempted to match tumor outcomes with the expression of the following stem cell markers: ALDH1, AnnexinA1, CD44, CD117, CD166, Nanog and oct-4. Tissue microarray blocks from triple-negative breast cancers were immunostained for the listed markers, and their expression by the majority of tumor cells (diffuse positivity) was correlated with prognosis. Of the 106 tumors investigated, diffuse positivity was seen in 7 (ALDH1), 33 (AnnexinA1), 53 (CD44), 44 (CD117 membranous only), 49 (CD117), 72 (CD166), 19 (Nanog), and 11 (oct-4) cases. With a median follow-up of 83 months, ALDH1 and CD117 expression was associated with DFS, whereas CD44, CD117 and CD166 were associated with OS estimates, based on Kaplan-Meier analyses. In the multivariate Cox proportional hazard models (including the examined markers and clinicopathological data which had a statistical impact in the univariate analysis), the pN category and the lack of ALDH1 expression were independent prognosticators for DFS, and the pN category and diffuse CD44 staining were independent prognosticators for OS. In the multivariate analysis including all of the examined clinicopathological data and markers, only CD117 showed a statistical impact on OS. We failed to demonstrate a prognostic impact for most stem cell markers tested in triple-negative breast cancer, but lack of ALDH1 staining and CD44 expression appears as of prognostic value, requiring further examination in independent studies.
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三阴性乳腺癌干细胞标志物的预后价值
在众多连续的癌症理论中,干细胞理论是目前最被接受的理论。癌症干细胞位于具有特定环境的小壁龛中,可自我更新,被认为是许多复发的原因。干细胞标记可突出显示它们,但这些标记往往也标记肿瘤细胞,这可能代表与预后相关的表型变化。在这项研究中,我们尝试将肿瘤预后与以下干细胞标记物的表达相匹配:ALDH1、AnnexinA1、CD44、CD117、CD166、Nanog和oct-4。对来自三阴性乳腺癌的组织微阵列块进行免疫染色,以检测所列标记物,大部分肿瘤细胞(弥漫阳性)的标记物表达与预后相关。在调查的 106 例肿瘤中,弥漫阳性的有 7 例(ALDH1)、33 例(AnnexinA1)、53 例(CD44)、44 例(仅 CD117 膜性)、49 例(CD117)、72 例(CD166)、19 例(Nanog)和 11 例(oct-4)。中位随访时间为 83 个月,根据 Kaplan-Meier 分析,ALDH1 和 CD117 表达与 DFS 相关,而 CD44、CD117 和 CD166 与 OS 估计值相关。在多变量 Cox 比例危险模型中(包括在单变量分析中具有统计学影响的受检标记物和临床病理数据),pN 类别和缺乏 ALDH1 表达是 DFS 的独立预后指标,pN 类别和弥漫性 CD44 染色是 OS 的独立预后指标。在包括所有临床病理数据和标记物的多变量分析中,只有CD117对OS有统计学影响。我们未能证明在三阴性乳腺癌中测试的大多数干细胞标记物对预后有影响,但缺乏ALDH1染色和CD44表达似乎具有预后价值,需要在独立研究中进一步检查。
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