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The role of poly(ADP-ribose) in the DNA damage signaling network.

机译:聚(ADP-核糖)在DNA损伤信号网络中的作用。

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摘要

DNA damage signaling is crucial for the maintenance of genome integrity. In higher eukaryotes a NAD+-dependent signal transduction mechanism has evolved to protect cells against the genome destabilizing effects of DNA strand breaks. The mechanism involves 2 nuclear enzymes that sense DNA strand breaks, poly(ADP-ribose) polymerase-1 and -2 (PARP-1 and PARP-2). When activated by DNA breaks, these PARPs use NAD+ to catalyze their automodification with negatively charged, long and branched ADP-ribose polymers. Through recruitment of specific proteins at the site of damage and regulation of their activities, these polymers may either directly participate in the repair process or coordinate repair through chromatin unfolding, cell cycle progression, and cell survival – cell death pathways. A number of proteins, including histones, DNA topoisomerases, DNA methyltransferase-1 as well as DNA damage repair and checkpoint proteins (p23, p21, DNA-PK, NF-kB, XRCC1, and others) can be targeted in this manner; the interaction involves a specific poly(ADP-ribose)-binding sequence motif of 20–26 amino acids in the target domains.
机译:DNA损伤信号对于维持基因组完整性至关重要。在高级真核生物中,已经形成了一种依赖NAD +的信号转导机制,以保护细胞免受DNA链断裂的基因组不稳定影响。该机制涉及2个检测DNA链断裂的核酶,聚(ADP-核糖)聚合酶-1和-2(PARP-1和PARP-2)。当被DNA断裂激活时,这些PARP使用NAD +催化带负电荷的长且支链ADP-核糖聚合物的自修饰。通过在损伤部位募集特定蛋白质并调节其活性,这些聚合物可以直接参与修复过程,也可以通过染色质展开,细胞周期进程和细胞存活-细胞死亡途径协调修复。以这种方式可以靶向多种蛋白质,包括组蛋白,DNA拓扑异构酶,DNA甲基转移酶-1以及DNA损伤修复和检查点蛋白质(p23,p21,DNA-PK,NF-kB,XRCC1等);相互作用涉及目标域中20-26个氨基酸的特定聚(ADP-核糖)结合序列基序。

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