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首页> 外文期刊>International Journal of Cancer =: Journal International du Cancer >Acquired cisplatin resistance in the head-neck cancer cell line Cal27 is associated with decreased DKK1 expression and can partially be reversed by overexpression of DKK1.
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Acquired cisplatin resistance in the head-neck cancer cell line Cal27 is associated with decreased DKK1 expression and can partially be reversed by overexpression of DKK1.

机译:头颈部癌细胞系Cal27中获得的顺铂耐药性与DKK1表达降低有关,并且可以通过DKK1的过表达而部分逆转。

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Head and neck cancers are treated by a combination of surgery, radiotherapy and/or chemotherapy. The clinical success of cisplatin-based chemotherapy, mostly in combination with 5-FU or a taxane, is however limited by multifactorial intrinsic or acquired resistance. So far, known genes involved in cisplatin resistance do not sufficiently allow the prediction of cancer chemosensitivity. Thus, the purpose of this study was to search for further genes involved in cisplatin resistance by differential gene expression analysis of the parental tongue cancer cell line Cal27 and its 10-fold more resistant sub-cell line Cal27cis, which was obtained by treating Cal27 with increasing concentrations of cisplatin. As found by the suppression subtractive hybridization, expression of DKK1, an inhibitor of canonical WNT signaling, was decreased in Cal27cis. Microarray analysis, qPCR and ELISA confirmed the approximately 2-fold difference in expression. Cisplatin treatment and serum starvation increased by 2-fold the secretion of DKK1 in Cal27 and Cal27cis, thus rendering DKK1-levels significantly different in both cell lines under basal and stress conditions. Recombinant overexpression of DKK1 in Cal27 and Cal27cis resulted in clonal cell lines, which were both 2.2- to 3-fold more sensitive toward cisplatin in cell viability (MTT) and in proliferation (BrdU) assays. In conclusion, acquired (10-fold) resistance of Cal27 against cisplatin is associated with decreased DKK1 expression and could partially be reversed by DKK1 overexpression, thus suggesting DKK1 and the WNT signaling pathway as a marker and target for cisplatin chemosensitivity.
机译:头颈癌可以通过手术,放疗和/或化学疗法相结合的方法进行治疗。然而,基于顺铂的化学疗法(主要与5-FU或紫杉烷类药物联合使用)的临床成功受到多因素固有或获得性耐药性的限制。迄今为止,与顺铂抗性有关的已知基因还不足以预测癌症的化学敏感性。因此,本研究的目的是通过对父母舌癌癌细胞系Cal27及其耐药性亚细胞系Cal27cis的10倍以上的差异基因表达分析来寻找与顺铂耐药相关的其他基因,该基因是通过用Cal27处理Cal27cis顺铂浓度增加。如通过抑制性消减杂交所发现的,Cal27cis中经典WNT信号抑制剂DKK1的表达降低。微阵列分析,qPCR和ELISA证实了表达的大约2倍差异。顺铂处理和血清饥饿增加了Cal27和Cal27cis中DKK1分泌的2倍,因此在基础和应激条件下,两种细胞系中DKK1的水平均显着不同。 Cal27和Cal27cis中DKK1的重组过表达导致克隆细胞系,在细胞活力(MTT)和增殖(BrdU)分析中,它们对顺铂的敏感性都高2.2至3倍。总之,Cal27对顺铂的获得性耐药(10倍)与DKK1表达降低有关,并且可能因DKK1过表达而部分逆转,因此提示DKK1和WNT信号通路是顺铂化学敏感性的标志物和靶标。

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