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In vitro analysis of putative cancer stem cell populations and chemosensitivity in the SW480 and SW620 colon cancer metastasis model

机译:SW480和SW620结肠癌转移模型中推定的癌症干细胞群体和化学敏感性的体外分析

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摘要

The cancer stem cell (CSC) theory implicates a small subpopulation of cells with stem-like properties, which is responsible for tumour initiation, development and metastasis. The unique biological and functional characteristics of CSCs, widely associated with treatment resistance, indicate an association between metastasis and stemness. It was hypothesised that metastatic cell lines may be enriched in CSCs and that this would correlate with a more resistant tumour. In the present study, the SW480 and SW620 paired cell lines derived from a colon adenocarcinoma and its lymph node metastasis, respectively were compared as an in vitro model of cancer progression. Their chemosensitivity and CSC properties were investigated. A range of in vitro assays were performed, including the side population assay, ALDEFLUOR assay, tumoursphere assay and assessment of CSC-associated surface phenotypes. It was determined that the SW480 and SW620 cells exhibited similar growth rates, although the SW480 cells were more migratory in wound healing assays on collagen and fibronectin matrices. SW480 and SW620 cells displayed similar CSC profiles, however, SW480 cells demosntrated significantly greater tumoursphere forming efficiency over SW620 cells. Tumourspheres derived from SW480 and SW620 cells also displayed differential sensitivity to 5-fluorouracil, oxaliplatin, geldanamycin and novobiocin that was not apparent when cells were grown under adherent conditions. Taken together, these results suggest that although the two cell lines have similar levels of putative CSC populations, there are differences in their biology that cannot be explained by these CSC levels. To the best of our knowledge, this is the first study to conduct a detailed analysis of the CSC populations using multiple in vitro assays in a paired cell line model. These results have clinical relevance for the understanding of the differences between primary tumours and their metastatic counterparts.
机译:癌症干细胞(CSC)理论涉及具有干样特性的一小部分细胞亚群,其负责肿瘤的发生,发展和转移。 CSC的独特生物学和功能特性与治疗耐药性广泛相关,表明转移与干性之间存在关联。假设转移细胞系可能富含CSC,并且这可能与更具抵抗力的肿瘤有关。在本研究中,将分别来自结肠腺癌及其淋巴结转移的SW480和SW620配对细胞系作为癌症进展的体外模型进行了比较。研究了它们的化学敏感性和CSC特性。进行了一系列体外测定,包括侧群测定,ALDEFLUOR测定,肿瘤圈测定和与CSC相关的表面表型的评估。尽管在胶原蛋白和纤连蛋白基质的伤口愈合试验中,SW480细胞迁移性更高,但已确定SW480和SW620细胞表现出相似的生长速率。 SW480和SW620细胞显示出相似的CSC谱图,但是,SW480细胞比SW620细胞具有明显更高的肿瘤形成效率。来自SW480和SW620细胞的肿瘤球也显示出对5-氟尿嘧啶,奥沙利铂,格尔德霉素和新霉素的差异敏感性,这在贴壁条件下生长时并不明显。综上所述,这些结果表明,尽管两种细胞系的推定CSC群体水平相似,但它们的生物学差异无法用这些CSC水平来解释。据我们所知,这是首次在配对细胞系模型中使用多种体外测定法对CSC种群进行详细分析的研究。这些结果对于了解原发性肿瘤及其转移性对应物之间的差异具有临床意义。

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