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γH2AX 焦点分析监测 DNA 双链断裂修复:优势、局限性和优化。

gammaH2AX foci analysis for monitoring DNA double-strand break repair: strengths, limitations and optimization.

机构信息

Darmstadt University of Technology, Radiation Biology and DNA Repair, Darmstadt, Germany.

出版信息

Cell Cycle. 2010 Feb 15;9(4):662-9. doi: 10.4161/cc.9.4.10764. Epub 2010 Mar 2.

Abstract

DNA double-strand breaks (DSBs) represent an important radiation-induced lesion and impaired DSB repair provides the best available correlation with radiosensitivity. Physical techniques for monitoring DSB repair require high, non-physiological doses and cannot reliably detect subtle defects. One outcome from extensive research into the DNA damage response is the observation that H2AX, a variant form of the histone H2A, undergoes extensive phosphorylation at the DSB, creating gammaH2AX foci that can be visualized by immunofluorescence. There is a close correlation between gammaH2AX foci and DSB numbers and between the rate of foci loss and DSB repair, providing a sensitive assay to monitor DSB repair in individual cells using physiological doses. However, gammaH2AX formation can occur at single-stranded DNA regions which arise during replication or repair and thus does not solely correlate with DSB formation. Here, we present and discuss evidence that following exposure to ionizing radiation, gammaH2AX foci analysis can provide a sensitive monitor of DSB formation and repair and describe techniques to optimize the analysis. We discuss the limitations and benefits of the technique, enabling the procedure to be optimally exploited but not misused.

摘要

DNA 双链断裂 (DSBs) 是一种重要的辐射诱导损伤,而 DSB 修复受损与放射敏感性具有最佳相关性。用于监测 DSB 修复的物理技术需要高剂量的非生理剂量,并且不能可靠地检测到细微缺陷。对 DNA 损伤反应的广泛研究的一个结果是观察到组蛋白 H2A 的一种变体形式 H2AX 在 DSB 处经历广泛的磷酸化,形成 γH2AX 焦点,可通过免疫荧光进行可视化。γH2AX 焦点与 DSB 数量之间以及焦点丢失率与 DSB 修复之间存在密切相关性,为使用生理剂量在单个细胞中监测 DSB 修复提供了一种灵敏的检测方法。然而,γH2AX 的形成也可能发生在复制或修复过程中产生的单链 DNA 区域,因此并不完全与 DSB 的形成相关。在这里,我们提出并讨论了证据,表明在暴露于电离辐射后,γH2AX 焦点分析可以作为 DSB 形成和修复的灵敏监测器,并描述了优化分析的技术。我们讨论了该技术的局限性和优势,以使该程序能够得到最佳利用而不被滥用。

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