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Systematic analysis of tumour cell-extracellular matrix adhesion identifies independent prognostic factors in breast cancer

机译:肿瘤细胞-细胞外基质粘附的系统分析确定了乳腺癌的独立预后因素

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摘要

Tumour cell-extracellular matrix (ECM) interactions are fundamental for discrete steps in breast cancer progression. In particular, cancer cell adhesion to ECM proteins present in the microenvironment is critical for accelerating tumour growth and facilitating metastatic spread. To assess the utility of tumour cell-ECM adhesion as a means for discovering prognostic factors in breast cancer survival, here we perform a systematic phenotypic screen and characterise the adhesion properties of a panel of human HER2 amplified breast cancer cell lines across six ECM proteins commonly deregulated in breast cancer. We determine a gene expression signature that defines a subset of cell lines displaying impaired adhesion to laminin. Cells with impaired laminin adhesion showed an enrichment in genes associated with cell motility and molecular pathways linked to cytokine signalling and inflammation. Evaluation of this gene set in the Molecular Taxonomy of Breast Cancer International Consortium (METABRIC) cohort of 1,964 patients identifies the F12 and STC2 genes as independent prognostic factors for overall survival in breast cancer. Our study demonstrates the potential of in vitro cell adhesion screens as a novel approach for identifying prognostic factors for disease outcome.
机译:肿瘤细胞-细胞外基质(ECM)相互作用是乳腺癌进展中不连续步骤的基础。特别是,癌细胞对微环境中存在的ECM蛋白的粘附对于加速肿瘤生长和促进转移扩散至关重要。为了评估肿瘤细胞-ECM粘附作为发现乳腺癌生存预后因素的手段的实用性,在这里我们进行系统的表型筛选,并表征一组人类HER2扩增的乳腺癌细胞系通常跨六种ECM蛋白的粘附特性在乳腺癌中放松管制。我们确定一个基因表达特征,该特征定义了显示对层粘连蛋白粘附力受损的细胞系的一个子集。层粘连蛋白粘附受损的细胞显示出与细胞运动相关的基因富集,以及与细胞因子信号传导和炎症相关的分子途径。在国际乳腺癌分子联合会(METABRIC)队列的1,964名患者中对该基因集进行评估,确定F12和STC2基因是乳腺癌总体生存的独立预后因素。我们的研究证明了体外细胞粘附筛选作为一种鉴定疾病预后因素的新方法的潜力。

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