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首页> 外文期刊>Cancer Cell International >Morphological and molecular characterization of the human breast epithelial cell line M13SV1 and its tumorigenic derivatives M13SV1-R2-2 and M13SV1-R2-N1
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Morphological and molecular characterization of the human breast epithelial cell line M13SV1 and its tumorigenic derivatives M13SV1-R2-2 and M13SV1-R2-N1

机译:人乳腺上皮细胞系M13SV1及其致癌衍生物M13SV1-R2-2和M13SV1-R2-N1的形态和分子特征

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The estrogen receptor-positive M13SV1 breast epithelial cell line was proposed to be a suitable in vitro model for breast cancer research since two derivatives with graduated tumorigenicity—M13SV1-R2-2 and M13SV1-R2-N1—are available for this cell line. In the present study, these three cell lines were comparatively examined for their morphological and their biochemical properties on the molecular level. A transcriptomic approach (gene array analysis) was chosen to unravel differences in gene expression among the three cell lines. Network analysis was conducted to identify deregulated signaling pathways. Cellular viability was determined by impedance measurements as well as by neutral red uptake assay. Apoptosis was determined by using a caspase assay. For morphological characterization, cells were grown in three-dimensional cell culture, and cellular differentiation and spheroid formation was followed by immunofluorescence staining by using confocal laser scanning microscopy. The gene array results indicated that there were only marginal differences in gene expression among the three cell lines. Network analysis predicted the R2-N1 derivative (1) to display enhanced apoptosis and (2) to have a higher migration capability compared to its parent cell line M13SV1. Enhanced apoptosis was confirmed by elevated caspase activity, and increased migration was observed in 3D culture when cells migrated out of the globular spheroids. In 3D cell culture, all three cell lines similarly formed spheroids within three days, but there was no acini formation until day 21 which is indicated by a growth arrest around day 15, cellular polarization, and the formation of hollow lumen inside the spheroids. These characteristics, however, are crucial to study, e.g., the differentiation process of breast epithelial cells in vitro. Due to the molecular and morphological features, the M13SV1 cell line and its tumorigenic derivatives seem to be less suitable as in vitro models than other cell lines such as the MCF-10A cell line which displays proper acini formation in 3D culture.
机译:有人提出雌激素受体阳性的M13SV1乳腺上皮细胞系是适合乳腺癌研究的体外模型,因为有两种具有逐渐致瘤性的衍生物-M13SV1-R2-2和M13SV1-R2-N1可用于该细胞系。在本研究中,在分子水平上比较了这三种细胞系的形态和生化特性。选择了转录组学方法(基因阵列分析)来揭示三种细胞系之间基因表达的差异。进行网络分析以鉴定失控的信号通路。细胞活力通过阻抗测量以及中性红吸收测定来确定。通过使用半胱天冬酶测定法测定凋亡。为了进行形态学表征,使细胞在三维细胞培养物中生长,并通过使用共聚焦激光扫描显微镜对细胞分化和球体形成进行免疫荧光染色。基因阵列结果表明,这三种细胞系之间的基因表达仅存在少量差异。网络分析预测,R2-N1衍生物(1)与其母细胞系M13SV1相比,显示出增强的细胞凋亡,(2)具有更高的迁移能力。半胱氨酸天冬氨酸蛋白酶活性的升高证实了细胞凋亡的增强,并且当细胞迁移出球状球体时,在3D培养中观察到迁移增加。在3D细胞培养中,所有三种细胞系在三天内都类似地形成了球体,但直到第21天才形成痤疮,这通过在第15天左右细胞极化的生长停滞以及在球体内形成空心腔来表明。然而,这些特征对于例如体外研究乳腺上皮细胞的分化过程至关重要。由于分子和形态特征,M13SV1细胞系及其致瘤衍生物似乎不如其他细胞系(例如在3D培养中显示适当的腺泡形成的MCF-10A细胞系)适合作为体外模型。

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