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Is current therapy of malignant gliomas beneficial for patients? Proteomics evidence of shifts in glioma cells expression patterns under clinically relevant treatment conditions

机译:当前的恶性神经胶质瘤治疗对患者有益吗?蛋白质组学证据在临床相关治疗条件下胶质瘤细胞表达模式的改变

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摘要

The most common human brain turnours - gliomas - have poor prognosis with and without treatment. The current therapy conditions act sub-lethally and cannot effectively suppress the proliferation of glioma cells. Here we show differential protein expression patterns in surviving human malignant U87-MG glioma cells under clinically relevant chemo/radiotherapy. In parallel experiments, the cells underwent either irradiation (2 Gy, 200 KV X-ray) or chemotreatment with 30 mu g/ml, of temozolomide in the cultivation medium or combined chemo/radiation treatment. The cell cultures were treated during 5 days from day 4 until day 9 of growth. Modulated expression patterns of vimentin and RhoA GTPase indicate a potentially increasing grade of malignancy in treated cell fractions correlating well with extremely aggressive tumour phenotypes observed clinically at recidivation of treated malignant gliomas.
机译:有和没有治疗,最常见的人脑神经胶质瘤-脑胶质瘤。当前的治疗条件仅次于致命,不能有效抑制神经胶质瘤细胞的增殖。在这里,我们显示了在临床相关的化学/放射治疗下幸存的人类恶性U87-MG神经胶质瘤细胞中的差异蛋白表达模式。在平行实验中,在培养基中对细胞进行辐射(2 Gy,200 KV X射线)或用30μg / ml替莫唑胺进行化学处理或化学/辐射联合处理。从生长的第4天到第9天,在5天内处理细胞培养物。波形蛋白和RhoA GTPase的表达模式调节表明,在治疗的细胞部分中恶性程度可能与在临床上观察到的恶性神经胶质瘤复发时观察到的极具侵略性的肿瘤表型高度相关。

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