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Induction and Processing of the Radiation-Induced Gamma-H2AX Signal and Its Link to the Underlying Pattern of DSB: A Combined Experimental and Modelling Study

机译:辐射诱导的Gamma-H2AX信号的诱导和处理及其与DSB的基本模式的联系:结合实验和建模研究

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摘要

We present here an analysis of DSB induction and processing after irradiation with X-rays in an extended dose range based on the use of the γH2AX assay. The study was performed by quantitative flow cytometry measurements, since the use of foci counting would result in reasonable accuracy only in a limited dose range of a few Gy. The experimental data are complemented by a theoretical analysis based on the GLOBLE model. In fact, original aim of the study was to test GLOBLE predictions against new experimental data, in order to contribute to the validation of the model. Specifically, the γH2AX signal kinetics has been investigated up to 24 h after exposure to increasing photon doses between 2 and 500 Gy. The prolonged persistence of the signal at high doses strongly suggests dose dependence in DSB processing after low LET irradiation. Importantly, in the framework of our modelling analysis, this is related to a gradually increased fraction of DSB clustering at the micrometre scale. The parallel study of γH2AX dose response curves shows the onset of a pronounced saturation in two cell lines at a dose of about 20 Gy. This dose is much lower than expected according to model predictions based on the values usually adopted for the DSB induction yield (≈ 30 DSB/Gy) and for the γH2AX foci extension of approximately 2 Mbp around the DSB. We show and discuss how theoretical predictions and experimental findings can be in principle reconciled by combining an increased DSB induction yield with the assumption of a larger genomic extension for the single phosphorylated regions. As an alternative approach, we also considered in our model the possibility of a 3D spreading-mechanism of the H2AX phosphorylation around the induced DSB, and applied it to the analysis of both the aspects considered. Our results are found to be supportive for the basic assumptions on which GLOBLE is built. Apart from giving new insights into the H2AX phosphorylation process, experiments performed at high doses are of relevance in the context of radiation therapy, where hypo-fractionated schemes become increasingly popular.
机译:我们在此基于γH2AX分析的使用,在扩展剂量范围内的X射线辐照后,对DSB诱导和处理进行了分析。该研究是通过定量流式细胞仪测量进行的,因为使用病灶计数仅在几个Gy的有限剂量范围内才能产生合理的准确性。实验数据得到了基于GLOBLE模型的理论分析的补充。实际上,该研究的原始目的是针对新的实验数据测试GLOBLE预测,以有助于模型的验证。具体而言,已经在暴露于2至500 Gy的增加的光子剂量后长达24小时研究了γH2AX信号动力学。高剂量下信号的持久存在强烈表明低LET照射后DSB处理中的剂量依赖性。重要的是,在我们的建模分析框架中,这与微米级的DSB聚簇比例逐渐增加有关。对γH2AX剂量反应曲线的平行研究显示,在约20 Gy的剂量下,两个细胞系开始出现明显的饱和。根据通常基于DSB诱导产量(≈30 DSB / Gy)和围绕DSB约2 Mbp的γH2AX焦点扩展所采用的值的模型预测,此剂量远低于根据模型预测所预期的剂量。我们展示和讨论如何通过结合增加的DSB诱导产率和单个磷酸化区域更大的基因组延伸的假设来协调理论上的预测和实验结果。作为一种替代方法,我们还在模型中考虑了诱导的DSB周围H2AX磷酸化3D扩散机制的可能性,并将其应用于所考虑的两个方面的分析。发现我们的结果支持建立GLOBLE的基本假设。除了提供有关H2AX磷酸化过程的新见解外,高剂量实验还与放射疗法有关,在这种疗法中,超分割方案越来越受欢迎。

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