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在类干细胞条件下癌细胞系的生长有揭示治疗靶点的潜力。

Growth of cancer cell lines under stem cell-like conditions has the potential to unveil therapeutic targets.

作者信息

Rappa Germana, Mercapide Javier, Anzanello Fabio, Prasmickaite Lina, Xi Yaguang, Ju Jingfang, Fodstad Oystein, Lorico Aurelio

机构信息

Mitchell Cancer Institute, University of South Alabama, 307 N. University Boulevard, Mobile, AL 36688, USA.

出版信息

Exp Cell Res. 2008 Jun 10;314(10):2110-22. doi: 10.1016/j.yexcr.2008.03.008. Epub 2008 Mar 20.

Abstract

Malignant tumors comprise a small proportion of cancer-initiating cells (CIC), capable of sustaining tumor formation and growth. CIC are the main potential target for anticancer therapy. However, the identification of molecular therapeutic targets in CIC isolated from primary tumors is an extremely difficult task. Here, we show that after years of passaging under differentiating conditions, glioblastoma, mammary carcinoma, and melanoma cell lines contained a fraction of cells capable of forming spheroids upon in vitro growth under stem cell-like conditions. We found an increased expression of surface markers associated with the stem cell phenotype and of oncogenes in cell lines and clones cultured as spheroids vs. adherent cultures. Also, spheroid-forming cells displayed increased tumorigenicity and an altered pattern of chemosensitivity. Interestingly, also from single retrovirally marked clones, it was possible to isolate cells able to grow as spheroids and associated with increased tumorigenicity. Our findings indicate that short-term selection and propagation of CIC as spheroid cultures from established cancer cell lines, coupled with gene expression profiling, represents a suitable tool to study and therapeutically target CIC: the notion of which genes have been down-regulated during growth under differentiating conditions will help find CIC-associated therapeutic targets.

摘要

恶性肿瘤仅占癌症起始细胞(CIC)的一小部分,这些细胞能够维持肿瘤的形成和生长。CIC是抗癌治疗的主要潜在靶点。然而,从原发性肿瘤中分离出的CIC的分子治疗靶点的鉴定是一项极其困难的任务。在此,我们表明,在分化条件下传代多年后,胶质母细胞瘤、乳腺癌和黑色素瘤细胞系中包含一部分细胞,这些细胞在类似干细胞的条件下体外生长时能够形成球体。我们发现,与贴壁培养相比,作为球体培养的细胞系和克隆中,与干细胞表型相关的表面标志物和癌基因的表达增加。此外,形成球体的细胞表现出更高的致瘤性和改变的化学敏感性模式。有趣的是,从单个逆转录病毒标记的克隆中也有可能分离出能够作为球体生长并具有更高致瘤性的细胞。我们的研究结果表明,从已建立的癌细胞系中以球体培养的方式对CIC进行短期选择和增殖,再结合基因表达谱分析,是研究和治疗靶向CIC的合适工具:哪些基因在分化条件下生长过程中被下调的概念将有助于找到与CIC相关的治疗靶点。

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