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首页> 外文期刊>Radiotherapy and oncology: Journal of the European Society for Therapeutic Radiology and Oncology >Microarray analysis of the transcriptional response to single or multiple doses of ionizing radiation in human subcutaneous fibroblasts.
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Microarray analysis of the transcriptional response to single or multiple doses of ionizing radiation in human subcutaneous fibroblasts.

机译:对人类皮下成纤维细胞中单剂量或多剂量电离辐射的转录反应进行微阵列分析。

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BACKGROUND AND PURPOSE: Transcriptional profiling of fibroblasts derived from breast cancer patients might improve our understanding of subcutaneous radiation-induced fibrosis. The aim of this study was to get a comprehensive overview of the changes in gene expression in subcutaneous fibroblast cell lines after various ionizing radiation (IR) schemes in order to provide information on potential targets for prevention and to suggest candidate genes for SNP association studies aimed at predicting individual risk of radiation-induced morbidity. PATIENTS AND METHODS: Thirty different human fibroblast cell lines were included in the study, and two different radiation schemes; single dose experiments with 3.5 Gy or fractionated with 3 x 3.5 Gy. Expression analyses were performed on unexposed and exposed cells after different time points. The IR response was analyzed using the statistical method Significance Analysis of Microarrays (SAM). RESULTS: While many of the identified genes were involved in known IR response pathways like cell cycle arrest, proliferation and detoxification, a substantial fraction of the genes were involved in processes not previously associated with IR response. Of particular interest is genes involved in ECM remodelling, Wnt signalling and IGF signalling. Many of the genes were identified after a single dose, but transcriptional changes in genes related to ROS scavenging and ECM remodelling were most profound after a fractionated scheme. CONCLUSIONS: We have identified a number of IR response pathways in fibroblasts derived from breast cancer patients. Besides previously identified pathways, we have identified new pathways and genes that could be relevant for prevention and intervention studies of subcutaneous radiation-induced fibrosis as well as being candidates for SNP association studies.
机译:背景与目的:乳腺癌患者来源的成纤维细胞的转录谱分析可能会增进我们对皮下辐射诱发的纤维化的了解。这项研究的目的是对各种电离辐射(IR)方案后皮下成纤维细胞细胞系中基因表达的变化进行全面概述,以便提供有关潜在预防目标的信息并建议针对SNP关联研究的候选基因在预测辐射致发病的个体风险方面。患者与方法:这项研究包括了30种不同的人类成纤维细胞系,以及两种不同的放射方案。 3.5 Gy的单剂量实验或3 x 3.5 Gy的分级实验。在不同时间点后,对未暴露和暴露的细胞进行表达分析。使用统计方法微阵列重要性分析(SAM)分析IR响应。结果:虽然许多已鉴定的基因都参与了已知的IR反应途径,如细胞周期停滞,增殖和排毒,但大部分基因却参与了以前与IR反应无关的过程。特别感兴趣的是涉及ECM重塑,Wnt信号传导和IGF信号传导的基因。单一剂量后即可鉴定出许多基因,但采用分级方案后,与ROS清除和ECM重塑相关的基因转录变化最为明显。结论:我们已经鉴定出源自乳腺癌患者的成纤维细胞中的许多IR反应途径。除了先前确定的途径外,我们还确定了可能与皮下辐射诱发的纤维化的预防和干预研究相关的新途径和基因,并可能成为SNP关联研究的候选者。

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