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癌相关成纤维细胞(CAFs)与其来自相邻结肠黏膜的配对正常成纤维细胞(NCF)之间的差异揭示了CAFs的功能异质性,提供了预后信息。

Differences between CAFs and their paired NCF from adjacent colonic mucosa reveal functional heterogeneity of CAFs, providing prognostic information.

作者信息

Berdiel-Acer Mireia, Sanz-Pamplona Rebeca, Calon Alexandre, Cuadras Daniel, Berenguer Antoni, Sanjuan Xavier, Paules Maria José, Salazar Ramon, Moreno Victor, Batlle Eduard, Villanueva Alberto, Molleví David G

机构信息

Translational Research Laboratory, Catalan Institute of Oncology, IDIBELL, L'Hospitalet de Llobregat, 08908 Catalonia, Spain.

Biomarkers and Susceptibility Unit, Cancer Prevention and Monitoring Programme, Catalan Institute of Oncology, IDIBELL, L'Hospitalet de Llobregat, Catalonia, Spain.

出版信息

Mol Oncol. 2014 Oct;8(7):1290-305. doi: 10.1016/j.molonc.2014.04.006. Epub 2014 May 6.

Abstract

Little is known about the difference in gene expression between carcinoma-associated fibroblasts (CAFs) and paired normal colonic fibroblasts (NCFs) in colorectal cancer. Paired CAFs and NCFs were isolated from eight primary human colorectal carcinoma specimens. In culture conditions, soluble factors secreted by CAFs in the conditioned media increased clonogenicity and migration of epithelial cancer cells lines to a greater extent than did NCF. In vivo, CAFs were more competent as tumour growth enhancers than paired NCFs when co-inoculated with colorectal cell lines. Gene expression analysis of microarrays of CAF and paired NCF populations enabled us to identify 108 deregulated genes (38 upregulated and 70 downregulated genes). Most of those genes are fibroblast-specific. This has been validated in silico in dataset GSE39396 and by qPCR in selected genes. GSEA analysis revealed a differential transcriptomic profile of CAFs, mainly involving the Wnt signallingsignalling pathway, focal adhesion and cell cycle. Both deregulated genes and biological processes involved depicted a considerable degree of overlap with deregulated genes reported in breast, lung, oesophagus and prostate CAFs. These observations suggest that similar transcriptomic programs may be active in the transition from normal fibroblast in adjacent tissues to CAFs, independently of their anatomic demarcation. Additionally NCF already depicted an activated pattern associated with inflammation. The deregulated genes signature score seemed to correlate with CAF tumour promoter abilities in vitro, suggesting a high degree of heterogeneity between CAFs, and it has also prognostic value in two independent datasets. Further characterization of the roles these biomarkers play in cancer will reveal how CAFs provide cancer cells with a suitable microenvironment and may help in the development of new therapeutic targets for cancer treatment.

摘要

关于结直肠癌中癌相关成纤维细胞(CAFs)与配对的正常结肠成纤维细胞(NCFs)之间基因表达的差异,目前所知甚少。从8例原发性人类结直肠癌标本中分离出配对的CAFs和NCFs。在培养条件下,条件培养基中CAFs分泌的可溶性因子比NCFs更能增强上皮癌细胞系的克隆形成能力和迁移能力。在体内,与结直肠癌细胞系共接种时,CAFs作为肿瘤生长促进剂比配对的NCFs更具活性。对CAF和配对的NCF群体进行基因芯片表达分析,使我们能够鉴定出108个失调基因(38个上调基因和70个下调基因)。这些基因大多数是成纤维细胞特异性的。这已在数据集GSE39396中通过计算机模拟得到验证,并在选定基因中通过qPCR得到验证。基因集富集分析(GSEA)揭示了CAFs的差异转录组图谱,主要涉及Wnt信号通路、粘着斑和细胞周期。失调基因和相关生物学过程与乳腺癌、肺癌、食管癌和前列腺癌CAFs中报道的失调基因有相当程度的重叠。这些观察结果表明,在从相邻组织中的正常成纤维细胞向CAFs转变过程中,可能存在相似的转录组程序,而与它们的解剖界限无关。此外,NCF已经呈现出与炎症相关的激活模式。失调基因特征评分似乎与CAFs在体外的肿瘤促进能力相关,表明CAFs之间存在高度异质性,并且在两个独立数据集中也具有预后价值。进一步表征这些生物标志物在癌症中所起的作用,将揭示CAFs如何为癌细胞提供合适的微环境,并可能有助于开发新的癌症治疗靶点。

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