Institute of Molecular Biology, Bulgarian Academy of Sciences, Acad. G. Bonchev Str. 21, 1113 Sofia, Bulgaria.
DNA Repair (Amst). 2013 Oct;12(10):800-10. doi: 10.1016/j.dnarep.2013.07.006. Epub 2013 Aug 6.
Cells are under constant assault by endogenous and environmental DNA damaging agents. DNA double strand breaks (DSBs) sever entire chromosomes and pose a major threat to genome integrity as a result of chromosomal fragment loss or chromosomal rearrangements. Exogenous factors such as ionizing radiation, crosslinking agents, and topoisomerase poisons, contribute to break formation. DSBs are associated with oxidative metabolism, form during the normal S phase, when replication forks collapse and are generated during physiological processes such as V(D)J recombination, yeast mating type switching and meiosis. It is estimated that in mammalian cells ∼10 DSBs per cell are formed daily. If left unrepaired DSBs can lead to cell death or deregulated growth, and cancer development. Cellular response to DSB damage includes mechanisms to halt the progression of the cell cycle and to restore the structure of the broken chromosome. Changes in chromatin adjacent to DNA break sites are instrumental to the DNA damage response (DDR) with two apparent ends: to control compaction and to bind repair and signaling molecules to the lesion. Here, we review the key findings related to each of these functions and examine their cross-talk.
细胞不断受到内源性和环境 DNA 损伤因素的攻击。DNA 双链断裂 (DSB) 会切断整个染色体,导致染色体片段缺失或染色体重排,从而对基因组完整性构成重大威胁。电离辐射、交联剂和拓扑异构酶毒物等外源因素有助于形成断裂。DSB 与氧化代谢有关,在正常 S 期形成,此时复制叉崩溃,并在生理过程中产生,如 V(D)J 重组、酵母交配型转换和减数分裂。据估计,在哺乳动物细胞中,每天每个细胞形成约 10 个 DSB。如果不修复,DSB 可导致细胞死亡或生长失控,并引发癌症。细胞对 DSB 损伤的反应包括停止细胞周期进程和恢复断裂染色体结构的机制。邻近 DNA 断裂部位的染色质变化对于 DNA 损伤反应 (DDR) 至关重要,该反应有两个明显的终点:控制压缩并将修复和信号分子结合到损伤部位。在这里,我们回顾了与这些功能中的每一个相关的关键发现,并研究了它们的相互作用。
