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首页> 外文期刊>Radiation Research: Official Organ of the Radiation Research Society >Fractionated radiation therapy can induce a molecular profile for therapeutic targeting
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Fractionated radiation therapy can induce a molecular profile for therapeutic targeting

机译:分级放射疗法可以诱导分子轮廓以进行靶向治疗

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摘要

To examine the possibility of using fractionated radiation in a unique way with molecular targeted therapy, gene expression profiles of prostate carcinoma cells treated with 10 Gy radiation administered either as a single dose or as fractions of 2 Gy × 5 and 1 Gy × 10 were examined by microarray analysis. Compared to the single dose, the fractionated irradiation resulted in significant increases in differentially expressed genes in both cell lines, with more robust changes in PC3 cells than in DU145 cells. The differentially expressed genes (> two fold change; P < 0.05) were clustered and their ontological annotations evaluated. In PC3 cells genes regulating immune and stress response, cell cycle and apoptosis were significantly up-regulated by multifractionated radiation compared to single-dose radiation. Ingenuity Pathway Analysis (IPA) of the differentially expressed genes revealed that immune response and cardiovascular genes were in the top functional category in PC3 cells and cell-to-cell signaling in DU145 cells. RT-PCR analysis showed that a flexure point for gene expression occurred at the 6th8th fraction and AKT inhibitor perifosine produced enhanced cell killing after 1 Gy × 8 fractionated radiation in PC3 and DU145 cells compared to single dose. This study suggests that fractionated radiation may be a uniquely exploitable, non-oncogene-addiction stress pathway for molecular therapeutic targeting.
机译:为了检查以分子靶向疗法以独特方式使用分级放射的可能性,检查了以10 Gy放射单剂量或2 Gy×5和1 Gy×10的比例给药治疗的前列腺癌细胞的基因表达谱。通过微阵列分析。与单剂量相比,分次照射导致两种细胞系中差异表达基因的显着增加,与DU145细胞相比,PC3细胞的变化更为强烈。将差异表达的基因(> 2倍变化; P <0.05)聚类并评估其本体注释。在PC3细胞中,调节免疫和应激反应的基因,与单剂量辐射相比,多重辐射显着上调了细胞周期和凋亡。差异表达基因的独创性途径分析(IPA)显示,免疫应答和心血管基因在PC3细胞和DU145细胞的细胞间信号传递中是功能最高的类别。 RT-PCR分析表明,基因表达的弯曲点出现在第6-8个部分,与单剂量相比,在PC3和DU145细胞中进行1 Gy×8的分次放射后,AKT抑制剂periposine增强了细胞杀伤力。这项研究表明,分级辐射可能是分子治疗靶向的唯一可利用的,非致癌基因成瘾的应激途径。

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