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The Role of Long Non Coding RNAs in the Repair of DNA Double Strand Breaks

机译:长非编码RNA在DNA双链断裂修复中的作用

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摘要

DNA double strand breaks (DSBs) are abrasions caused in both strands of the DNA duplex following exposure to both exogenous and endogenous conditions. Such abrasions have deleterious effect in cells leading to genome rearrangements and cell death. A number of repair systems including homologous recombination (HR) and non-homologous end-joining (NHEJ) have been evolved to minimize the fatal effects of these lesions in cell. The role of protein coding genes in regulation of these pathways has been assessed previously. However, a number of recent studies have focused on evaluation of non-coding RNAs participation in DNA repair. We performed a computerized search of the Medline/ Pubmed databases with key words: DNA repair, homologous recombination, non-homologues end joining and long non-coding RNA (LncRNA). The existing data highlight the role of long non-coding RNAs in DSB repair as well as dysregulation in their expression which would lead to pathological conditions such as cancer. The specific mechanism of their contribution in DNA repair pathways has been elucidated for a few of them. LncRNAs participate in several steps of DNA repair pathways and regulate the expression of key components of these pathways including p53 tumor suppressor gene.
机译:DNA双链断裂(DSB)是在暴露于外源和内源条件后在DNA双链体的两条链中引起的磨损。这种擦伤对细胞具有有害作用,导致基因组重排和细胞死亡。已经开发出许多修复系统,包括同源重组(HR)和非同源末端连接(NHEJ),以最大程度地减少这些病变在细胞中的致命作用。先前已经评估了蛋白质编码基因在调节这些途径中的作用。但是,最近的许多研究集中于评估非编码RNA参与DNA修复。我们使用以下关键词对Medline / Pubmed数据库进行了计算机搜索:DNA修复,同源重组,非同源末端连接和长非编码RNA(LncRNA)。现有数据突出了长的非编码RNA在DSB修复中的作用以及其表达失调,这将导致诸如癌症的病理状况。他们中的一些已经阐明了它们在DNA修复途径中贡献的具体机制。 LncRNA参与DNA修复途径的多个步骤,并调节这些途径的关键成分(包括p53抑癌基因)的表达。

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