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首页> 外文期刊>Oncology reports >The TRAIL-receptor-1: TRAIL-receptor-3 and -4 ratio is a predictor for TRAIL sensitivity of cancer cells.
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The TRAIL-receptor-1: TRAIL-receptor-3 and -4 ratio is a predictor for TRAIL sensitivity of cancer cells.

机译:TRAIL-receptor-1:TRAIL-receptor-3和-4的比率是癌细胞对TRAIL敏感性的预测指标。

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The tumour necrosis factor-related apoptosis-inducing ligand (TRAIL) is a potent inducer of apoptosis in many cancer cells. However, a significant proportion of tumours are TRAIL-resistant erecting a major hurdle for a successful TRAIL-based treatment regimen in the future. In this context, it would be a major advantage to be able to identify the tumours that respond to TRAIL. The existence of two apoptosis-inducing receptors (TRAIL-R1 and TRAIL-R2) and two receptors that cannot transmit an apoptotic signal and have an inhibitory function (TRAIL-R3 and TRAIL-R4) make TRAIL signalling complicated. We analysed the surface expression of all four membrane-bound TRAIL receptors in cancer cell lines of various origin and primary cancer and normal cells and found a good correlation between TRAIL-sensitivity and the expression of TRAIL-R1 alone, but an even better correlation when a ratio of TRAIL-R1/TRAIL-R3+TRAIL-R4 was analysed. Experimental overexpression of TRAIL-R1 alone or in combination with TRAIL-R4 in PANC-1 cells confirmed our correlation results. Similar to the surface expression-apoptosis correlation analysis we found a high correlation between TRAIL-sensitivity and the mRNA level ratio of TRAIL-R1/TRAIL-R3+TRAIL-R4. A value of <0.85 for the ratio predicted TRAIL resistance in both protein and RNA analysis. Hence, TRAIL receptor RNA expression analysis by real-time PCR might be a feasible approach to predict possible TRAIL-responses in individual tumour samples.
机译:肿瘤坏死因子相关的凋亡诱导配体(TRAIL)是许多癌细胞中有效的凋亡诱导剂。但是,很大一部分肿瘤是TRAIL耐药的,这是将来成功实施基于TRAIL的治疗方案的主要障碍。在这种情况下,能够识别出对TRAIL有反应的肿瘤将是一个主要的优势。存在两种诱导细胞凋亡的受体(TRAIL-R1和TRAIL-R2)和两种不能传递凋亡信号并具有抑制功能的受体(TRAIL-R3和TRAIL-R4)使TRAIL信号传递变得复杂。我们分析了各种来源的癌细胞系和原发癌及正常细胞中所有四个膜结合的TRAIL受体的表面表达,发现TRAIL敏感性与单独的TRAIL-R1的表达之间有良好的相关性,但当相关性更好时分析TRAIL-R1 / TRAIL-R3 + TRAIL-R4的比例。在PANC-1细胞中单独或与TRAIL-R4组合使用的实验性过表达TRAIL-R1证实了我们的相关结果。与表面表达-细胞凋亡相关性分析相似,我们发现TRAIL-敏感性与TRAIL-R1 / TRAIL-R3 + TRAIL-R4的mRNA水平比之间存在高度相关性。蛋白质和RNA分析中预测的TRAIL抗性比率的值<0.85。因此,通过实时PCR进行TRAIL受体RNA表达分析可能是预测单个肿瘤样品中可能的TRAIL反应的可行方法。

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