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乳腺癌微环境中 CD10+基质细胞的特征和临床评估。

Characterization and clinical evaluation of CD10+ stroma cells in the breast cancer microenvironment.

机构信息

Breast Cancer Translational Research Laboratory JC Heuson, Institut Jules Bordet, 125 Bld de Waterloo, Brussels 1000, Belgium.

出版信息

Clin Cancer Res. 2012 Feb 15;18(4):1004-14. doi: 10.1158/1078-0432.CCR-11-0383. Epub 2012 Jan 10.

DOI:10.1158/1078-0432.CCR-11-0383
PMID:22235100
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC4446057/
Abstract

PURPOSE

There is growing evidence that interaction between stromal and tumor cells is pivotal in breast cancer progression and response to therapy. Based on earlier research suggesting that during breast cancer progression, striking changes occur in CD10(+) stromal cells, we aimed to better characterize this cell population and its clinical relevance.

EXPERIMENTAL DESIGN

We developed a CD10(+) stroma gene expression signature (using HG U133 Plus 2.0) on the basis of the comparison of CD10 cells isolated from tumoral (n = 28) and normal (n = 3) breast tissue. We further characterized the CD10(+) cells by coculture experiments of representative breast cancer cell lines with the different CD10(+) stromal cell types (fibroblasts, myoepithelial, and mesenchymal stem cells). We then evaluated its clinical relevance in terms of in situ to invasive progression, invasive breast cancer prognosis, and prediction of efficacy of chemotherapy using publicly available data sets.

RESULTS

This 12-gene CD10(+) stroma signature includes, among others, genes involved in matrix remodeling (MMP11, MMP13, and COL10A1) and genes related to osteoblast differentiation (periostin). The coculture experiments showed that all 3 CD10(+) cell types contribute to the CD10(+) stroma signature, although mesenchymal stem cells have the highest CD10(+) stroma signature score. Of interest, this signature showed an important role in differentiating in situ from invasive breast cancer, in prognosis of the HER2(+) subpopulation of breast cancer only, and potentially in nonresponse to chemotherapy for those patients.

CONCLUSIONS

Our results highlight the importance of CD10(+) cells in breast cancer prognosis and efficacy of chemotherapy, particularly within the HER2(+) breast cancer disease.

摘要

目的

越来越多的证据表明,基质细胞与肿瘤细胞的相互作用是乳腺癌进展和对治疗反应的关键。基于早期研究表明,在乳腺癌进展过程中,CD10(+)基质细胞发生显著变化,我们旨在更好地描述这种细胞群体及其临床相关性。

实验设计

我们根据从肿瘤(n=28)和正常(n=3)乳腺组织中分离的 CD10 细胞的比较,开发了一个 CD10(+)基质基因表达特征(使用 HG U133 Plus 2.0)。我们通过代表性乳腺癌细胞系与不同 CD10(+)基质细胞类型(成纤维细胞、肌上皮细胞和间充质干细胞)的共培养实验进一步表征 CD10(+)细胞。然后,我们使用公开可用的数据集评估其在原位至浸润性进展、浸润性乳腺癌预后和预测化疗疗效方面的临床相关性。

结果

这个 12 个基因的 CD10(+)基质特征包括参与基质重塑的基因(MMP11、MMP13 和 COL10A1)和与成骨细胞分化相关的基因(periostin)。共培养实验表明,所有 3 种 CD10(+)细胞类型都有助于 CD10(+)基质特征,尽管间充质干细胞具有最高的 CD10(+)基质特征评分。有趣的是,该特征在区分原位和浸润性乳腺癌、仅在 HER2(+)乳腺癌亚群的预后中以及在这些患者对化疗的无反应中发挥了重要作用。

结论

我们的结果强调了 CD10(+)细胞在乳腺癌预后和化疗疗效中的重要性,特别是在 HER2(+)乳腺癌疾病中。

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