CD133(+)CXCR4(+) 结肠癌细胞具有转移潜能,并预测患者预后不良。
CD133(+)CXCR4(+) colon cancer cells exhibit metastatic potential and predict poor prognosis of patients.
机构信息
Tumor Immunology and Gene Therapy Center, Eastern Hepatobiliary Surgery Hospital, Second Military Medical University, 225 Changhai Road, Shanghai 200438, China.
出版信息
BMC Med. 2012 Aug 7;10:85. doi: 10.1186/1741-7015-10-85.
BACKGROUND
Colorectal cancer (CRC), which frequently metastasizes to the liver, is one of the three leading causes of cancer-related deaths worldwide. Growing evidence suggests that a subset of cells exists among cancer stem cells. This distinct subpopulation is thought to contribute to liver metastasis; however, it has not been fully explored in CRC yet.
METHODS
Flow cytometry analysis was performed to detect distinct subsets with CD133 and CXCR4 markers in human primary and metastatic CRC tissues. The 'stemness' and metastatic capacities of different subpopulations derived from the colon cancer cell line HCT116 were compared in vitro and in vivo. The roles of epithelial-mesenchymal transition (EMT) and stromal-cell derived factor-1 (SDF-1) in the metastatic process were also investigated. A survival curve was used to explore the correlation between the content of CD133(+)CXCR4(+) cancer cells and patient survival.
RESULTS
In human specimens, the content of CD133(+)CXCR4(+) cells was higher in liver metastases than in primary colorectal tumors. Clonogenic and tumorigenic cells were restricted to CD133(+) cells in the HCT116 cell line, with CXCR4 expression having no impact on the 'stemness' properties. We found that CD133(+)CXCR4(+)cancer cells had a high metastatic capacity in vitro and in vivo. Compared with CD133(+)CXCR4(-) cells, CD133(+)CXCR4(+)cancer cells experienced EMT, which contributed partly to their metastatic phenotype. We then determined that SDF-1/CXCL12 treatment could further induce EMT in CD133(+)CXCR4(+)cancer cells and enhance their invasive behavior, while this could not be observed in CD133(+)CXCR4- cancer cells. Blocking SDF-1/CXCR4 interaction with a CXCR4 antagonist, AMD3100 (1,10-[1,4-phenylenebis(methylene)]bis-1,4,8,11 -tetraazacyclotetradecane octahydrochloride), inhibited metastatic tumor growth in a mouse hepatic metastasis model. Finally, a high percentage of CD133(+)CXCR4(+)cells in human primary CRC was associated with a reduced two-year survival rate.
CONCLUSIONS
Strategies targeting the SDF-1/CXCR4 interaction may have important clinical applications in the suppression of colon cancer metastasis. Further investigations on how high expression of CXCR4 and EMT occur in this identified cancer stem cell subset are warranted to provide insights into our understanding of tumor biology.
背景
结直肠癌(CRC)是全球癌症相关死亡的三大主要原因之一,常转移至肝脏。有证据表明,在癌症干细胞中存在亚群细胞。这一独特的亚群被认为有助于肝转移;然而,CRC 中尚未对此进行充分研究。
方法
通过流式细胞术分析,检测人原发性和转移性 CRC 组织中具有 CD133 和 CXCR4 标志物的不同亚群。在体外和体内比较从结肠癌细胞系 HCT116 中分离的不同亚群的“干性”和转移能力。还研究了上皮-间质转化(EMT)和基质细胞衍生因子-1(SDF-1)在转移过程中的作用。使用生存曲线来探讨 CD133(+)CXCR4(+)癌细胞含量与患者生存之间的相关性。
结果
在人类标本中,肝转移中 CD133(+)CXCR4(+)细胞的含量高于原发性结直肠肿瘤。在 HCT116 细胞系中,集落形成和肿瘤发生细胞仅限于 CD133(+)细胞,而 CXCR4 表达对“干性”特性没有影响。我们发现 CD133(+)CXCR4(+)癌细胞具有较高的体外和体内转移能力。与 CD133(+)CXCR4(-)细胞相比,CD133(+)CXCR4(+)癌细胞经历了 EMT,这部分有助于其转移表型。我们随后确定,SDF-1/CXCL12 处理可以进一步诱导 CD133(+)CXCR4(+)癌细胞的 EMT,并增强其侵袭行为,而在 CD133(+)CXCR4-癌细胞中则观察不到这种情况。用 CXCR4 拮抗剂 AMD3100(1,10-[1,4-亚苯基双(亚甲基)]-1,4,8,11-四氮杂环十四烷八盐酸盐)阻断 SDF-1/CXCR4 相互作用,可抑制小鼠肝转移模型中的转移性肿瘤生长。最后,人类原发性 CRC 中 CD133(+)CXCR4(+)细胞的高百分比与两年生存率降低相关。
结论
靶向 SDF-1/CXCR4 相互作用的策略可能在抑制结肠癌转移方面具有重要的临床应用价值。进一步研究这种鉴定的癌症干细胞亚群中 CXCR4 高表达和 EMT 发生的机制,将有助于深入了解肿瘤生物学。
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