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Reprogramming glioma cell cultures with retinoic acid: Additional arguments for reappraising the potential of retinoic acid in the context of personalized glioma therapy

机译:用视黄酸重编程神经胶质瘤细胞培养物:在个性化神经胶质瘤治疗的背景下重新评估视黄酸潜力的其他论点

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Background: Glioma, notably glioblastoma multiforme, is characterized by extensive inter-and intra-tumoral heterogeneity. Surprisingly, the potential for differentiation of glioma cells has not been systematically analyzed and included in patient stratification methods. In the current study, retinoic acid (RA), a neuronal differentiation agent, was assessed for the pro-differentiative and anti-proliferative effects on glioma cells. Methods: Using RA-responsive glioma culture as an experimental paradigm, we analyzed the differentiation process both by videomicroscopy and at the mRNA (RNA-seq and reverse transcription-quantitative-polymerase chain reaction) and proteomic levels. Results: Glioma cells can differentiate into neurons in response to RA by (i) extending ultra-long cytoplasmic extensions, (ii) using these extensions to move from cell to cell either by perikaryal translocation or in a "spider-flight" like process, (iii) slowing their cell cycling, (iv) acquiring several neuronal differentiation markers such as MAPT, GAP43, DCX, NRCAM, NeuroD2, NeuroG2, and NeuN, and (v) decreasing the expression of several genes associated with glioma aggressiveness. Conclusion: These results indicate the existence of a subgroup of patients harboring RA-responsive glioma cells amenable to differentiation therapy, and stratifying such patients with a functional test is easily achievable. This provides the first step to reassess the potential of RA in the context of personalized medicine.
机译:背景:胶质瘤,尤其是多形胶质母细胞瘤,其特征是广泛的肿瘤内和肿瘤内异质性。令人惊讶的是,尚未对胶质瘤细胞分化的潜力进行系统分析,也未将其包括在患者分层方法中。在当前的研究中,评估了神经元分化剂视黄酸(RA)对神经胶质瘤细胞的促分化和抗增殖作用。方法:使用RA反应性神经胶质瘤培养作为实验范式,我们通过视频显微镜以及mRNA(RNA-seq和逆转录定量聚合酶链反应)和蛋白质组学水平分析了分化过程。结果:神经胶质瘤细胞可以通过(i)扩展超长胞质扩展,(ii)使用这些扩展通过周缘移位或“蜘蛛飞行”之类的过程从一个细胞移动到另一个细胞,从而对RA分化为神经元, (iii)减慢其细胞周期,(iv)获得几种神经元分化标记,例如MAPT,GAP43,DCX,NRCAM,NeuroD2,NeuroG2和NeuN,以及(v)降低与神经胶质瘤侵袭性相关的几种基因的表达。结论:这些结果表明,存在一个带有RA反应性神经胶质瘤细胞且适合分化治疗的患者亚组,通过功能测试对这些患者进行分层很容易实现。这提供了在个性化医学的背景下重新评估RA潜力的第一步。

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