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Methods to Monitor DNA Repair Defects and Genomic Instability in the Context of a Disrupted Nuclear Lamina

机译:在破裂的核层中监测DNA修复缺陷和基因组不稳定性的方法

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摘要

The organization of the genome within the nuclear space is viewed as an additional level of regulation of genome function, as well as a means to ensure genome integrity. Structural proteins associated with the nuclear envelope, in particular lamins (A- and B-type) and lamin-associated proteins, play an important role in genome organization. Interestingly, there is a whole body of evidence that links disruptions of the nuclear lamina with DNA repair defects and genomic instability. Here, we describe a few standard techniques that have been successfully utilized to identify mechanisms behind DNA repair defects and genomic instability in cells with an altered nuclear lamina. In particular, we describe protocols to monitor changes in the expression of DNA repair factors (Western blot) and their recruitment to sites of DNA damage (immunofluorescence); kinetics of DNA double-strand break repair after ionizing radiation (neutral comet assays); frequency of chromosomal aberrations (FISH, fluorescence in situ hybridization); and alterations in telomere homeostasis (Quantitative-FISH). These techniques have allowed us to shed some light onto molecular mechanisms by which alterations in A-type lamins induce genomic instability, which could contribute to the pathophysiology of aging and aging-related diseases.
机译:核空间内基因组的组织被视为调节基因组功能的附加水平,也是确保基因组完整性的一种手段。与核膜相关的结构蛋白,特别是lamins(A型和B型)和lamin相关蛋白,在基因组组织中起着重要作用。有趣的是,有大量证据表明核层的破坏与DNA修复缺陷和基因组不稳定有关。在这里,我们描述了一些标准技术,这些标准技术已成功用于识别DNA修复缺陷和具有改变的核层的细胞中的基因组不稳定的机制。特别是,我们描述了监测DNA修复因子表达的变化(蛋白质印迹)及其对DNA损伤部位的募集(免疫荧光)的协议;电离辐射后DNA双链断裂修复的动力学(中性彗星试验);染色体畸变的频率(FISH,荧光原位杂交);和端粒稳态的改变(定量FISH)。这些技术使我们能够阐明分子机制,通过这些分子机制,A型lamin的改变会引起基因组不稳定,这可能有助于衰老和与衰老相关的疾病的病理生理。

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