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Chitosan promotes cancer progression and stem cell properties in association with Wnt signaling in colon and hepatocellular carcinoma cells

机译:壳聚糖促进癌症进展和干细胞性质与结肠和肝细胞癌细胞的WNT信号传导相关联

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Cancer stem cells (CSCs), a small population of cancer cells, have been considered to be the origin of cancer initiation, recurrence, and metastasis. Tumor microenvironment provides crucial signals for CSCs to maintain stem cell properties and promotes tumorigenesis. Therefore, establishment of an appropriate cell culture system to mimic the microenvironment for CSC studies is an important issue. In this study, we grew colon and hepatocellular carcinoma (HCC) cells on chitosan membranes and evaluated the tumor progression and the CSC properties. Experimental results showed that culturing cancer cells on chitosan increased cell motility, drug resistance, quiescent population, self-renewal capacity, and the expression levels of stemness and CSC marker genes, such as OCT4, NANOG, CD133, CD44, and EpCAM. Furthermore, we demonstrated that chitosan might activate canonical Wnt/β-catenin-CD44 axis signaling in CD44positive colon cancer cells and noncanonical Wnt-STAT3 signaling in CD44negative HCC cells. In conclusion, chitosan as culture substrates activated the essential signaling of CSCs and promoted CSC properties. The chitosan culture system provides a convenient platform for the research of CSC biology and screening of anticancer drugs.
机译:癌症干细胞(CSCs),小癌细胞群体,被认为是癌症起始,复发和转移的起源。肿瘤微环境为CSC提供了关键信号,以保持干细胞性能并促进肿瘤发生。因此,建立适当的细胞培养系统以模仿CSC研究的微环境是一个重要问题。在这项研究中,我们在壳聚糖膜上种植结肠和肝细胞癌(HCC)细胞,并评估肿瘤进展和CSC性质。实验结果表明,培养癌细胞对壳聚糖的癌细胞增加,耐药性,静止群,自我更新能力和茎秆和CSC标记基因的表达水平,如OCT4,NANOG,CD133,CD44和EPCAM。此外,我们证明了壳聚糖可能在CD44阳性结肠癌细胞中激活规范Wnt /β-连环蛋白-CD44轴信号,并在CD44Negative HCC细胞中在CD44兼出的非碳WNT-Stat3信号传导中。总之,壳聚糖作为培养基底物激活CSCs的基本信号和促进CSC性质。壳聚糖培养系统为CSC生物学和筛选抗癌药物进行了一种方便的平台。

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