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Stromal Activation by Tumor Cells: An in Vitro Study in Breast Cancer

机译:肿瘤细胞间质激活:乳腺癌的体外研究。

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摘要

Background: The tumor microenvironment participates in the regulation of tumor progression and influences treatment sensitivity. In breast cancer, it also may play a role in determining the fate of non-invasive lesions such as ductal carcinoma in situ (DCIS), a non-obligate precursor of invasive diseases, which is aggressively treated despite its indolent nature in many patients since no biomarkers are available to predict the progression of DCIS to invasive disease. In vitro models of stromal activation by breast tumor cells might provide clues as to specific stromal genes crucial for the transition from DCIS to invasive disease. Methods: normal human dermal fibroblasts (NHDF) were treated under serum-free conditions with cell culture media conditioned by breast cancer cell lines (SkBr3, MDA-MB-468, T47D) for 72 h and subjected to gene expression profiling with Illumina platform. Results: TGM2, coding for a tissue transglutaminase, was identified as candidate gene for stromal activation. In public transcriptomic datasets of invasive breast tumors TGM2 expression proved to provide prognostic information. Conversely, its role as an early biosensor of tumor invasiveness needs to be further investigated by in situ analyses. Conclusion: Stromal TGM2 might probably be associated with precancerous evolution at earlier stages compared to DCIS.
机译:背景:肿瘤微环境参与肿瘤进展的调节并影响治疗敏感性。在乳腺癌中,它也可能决定非侵入性病变的命运,例如导管原位癌(DCIS),这是一种非专性的浸润性疾病的前体,尽管在许多患者中其表现出惰性,但仍得到了积极的治疗。没有生物标记可用于预测DCIS向浸润性疾病的进展。乳腺肿瘤细胞激活基质的体外模型可能会提供线索,提示特定的基质基因对于从DCIS过渡到侵袭性疾病至关重要。方法:正常人真皮成纤维细胞(NHDF)在无血清条件下,以乳腺癌细胞系(SkBr3,MDA-MB-468,T47D)为条件的细胞培养基处理72小时,并用Illumina平台进行基因表达谱分析。结果:编码组织转谷氨酰胺酶的TGM2被鉴定为基质激活的候选基因。在侵袭性乳腺肿瘤的公共转录组数据集中,TGM2表达被证明可提供预后信息。相反,其作为肿瘤侵袭性的早期生物传感器的作用需要通过原位分析进一步研究。结论:与DCIS相比,基质基质TGM2可能与早期癌变有关。

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