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EGFR Kinase Promotes Acquisition of Stem Cell-Like Properties: A Potential Therapeutic Target in Head and Neck Squamous Cell Carcinoma Stem Cells

机译:EGFR激酶促进干细胞性质的收购:潜在的治疗靶点在头颈部鳞状细胞癌干细胞

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摘要

Members of the EGFR/ErbB family of tyrosine kinases are found to be highly expressed and deregulated in many cancers, including head and neck squamous cell carcinoma (HNSCC). The ErbB family, including EGFR, has been demonstrated to play key roles in metastasis, tumorigenesis, cell proliferation, and drug resistance. Recently, these characteristics have been linked to a small subpopulation of cells classified as cancer stem cells (CSCs) which are believed to be responsible for tumor initiation and maintenance. In this study, we investigated the possible role of EGFR as a regulator of “stemness” in HNSCC cells. Activation of EGFR by the addition of EGF ligand or ectopic expression of EGFR in two established HNSCC cell lines (UMSCC-22B and HN-1) resulted in the induction of CD44, BMI-1, Oct-4, NANOG, CXCR4, and SDF-1. Activation of EGFR also resulted in increased tumorsphere formation, a characteristic ability of cancer stem cells. Conversely, treatment with the EGFR kinase inhibitor, Gefinitib (Iressa), resulted in decreased expression of the aforementioned genes, and loss of tumorsphere-forming ability. Similar trends were observed in a 99.9% CD44 positive stem cell culture derived from a fresh HNSCC tumor, confirming our findings for the cell lines. Additionally, we found that these putative cancer stem cells, when treated with Gefitinib, possessed a lower capacity to invade and became more sensitive to cisplatin-induced death in vitro. These results suggest that EGFR plays critical roles in the survival, maintenance, and function of cancer stem cells. Drugs that target EGFR, perhaps administered in combination with conventional chemotherapy, might be an effective treatment for HNSCC.
机译:发现EGFR / ERBB系列酪氨酸激酶系列在许多癌症中高度表达和DEERICOUSE,包括头部和颈部鳞状细胞癌(HNSCC)。已经证明了包括EGFR的ERBB系列,以在转移,肿瘤发生,细胞增殖和耐药性中发挥关键作用。最近,这些特征与分类为癌症干细胞(CSC)的细胞的小亚群相关联,该细胞被认为是负责肿瘤起始和维护的负责。在这项研究中,我们研究了EGFR作为HTSCC细胞中“茎干”调节剂的可能作用。通过添加EGF配体的EGFR激活EGFR的EGFR在两种成立的HNSCC细胞系(UMSCC-22B和HN-1)中的EGFR的表达导致CD44,BMI-1,10月4,NANOG,CXCR4和SDF的诱导-1。 EGFR的激活也导致肿瘤孢子酰胺增加,癌症干细胞的特征能力。相反,用EGFR激酶抑制剂,GeFinitib(Iressa)治疗导致上述基因的表达降低,以及肿瘤形成能力的丧失。在新鲜HNSCC肿瘤中衍生的99.9%CD44阳性干细胞培养物中观察到类似的趋势,证实了我们对细胞系的研究结果。此外,我们发现这些推定的癌症干细胞在用吉非替尼处理时具有较低的侵入能力,并且对体外比顺铂诱导的死亡变得更敏感。这些结果表明,EGFR在癌症干细胞的存活率,维护和功能中起重要作用。靶向EGFR的药物,也许与常规化疗组合施用,可能是HNSCC的有效治疗方法。

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