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Assessment of epigenetic mechanisms and DNA double-strand break repair using laser micro-irradiation technique developed for hematological cells

机译:使用针对血液细胞的激光微辐照技术评估表观遗传机制和DNA双链断裂修复

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摘要

BackgroundCertain tumors rely heavily on their DNA repair capability to survive the DNA damage induced by chemotherapeutic agents. Therefore, it is important to monitor the dynamics of DNA repair in patient samples during the course of their treatment, in order to determine whether a particular drug regimen perturbs the DNA repair networks in cancer cells and provides therapeutic benefits. Quantitative measurement of proteins and/or their posttranslational modification(s) at DNA double strand breaks (DSBs) induced by laser microirradiation provides an applicable diagnostic approach to examine DNA repair and its dynamics. However, its use is restricted to adherent cell lines and not employed in suspension tumor cells that include the many hematological malignancies.
机译:背景某些肿瘤在很大程度上依赖于其DNA修复能力来抵抗化学治疗剂诱导的DNA损伤。因此,重要的是在治疗过程中监测患者样品中DNA修复的动态,以确定一种特定的药物治疗方案是否会干扰癌细胞中的DNA修复网络并提供治疗益处。通过激光微辐照诱导的DNA双链断裂(DSB)处蛋白质和/或其翻译后修饰的定量测量为检测DNA修复及其动力学提供了一种适用的诊断方法。然而,其用途仅限于贴壁细胞系,而不用于包括许多血液系统恶性肿瘤的悬浮肿瘤细胞。

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