Strosznajder Robert Piotr, Jesko Henryk, Zambrzycka Agata
Department of Neurophysiology, Medical Research Centre, Polish Academy of Sciences, Warsaw, Poland.
Mol Neurobiol. 2005;31(1-3):149-67. doi: 10.1385/MN:31:1-3:149.
Poly(ADP-ribose) polymerase (PARP)-1 is a DNA nick sensor that transforms ADP-ribose from betaNAD+ in the form of polymer to over 40 nuclear proteins, particularly to histones, several transcription factors, and PARP itself, modulating their activities and functions. PARP-1 activated by DNA breaks facilitates transcription, replication, and DNA base excision repair. The last studies indicate that PARP-1 is the new nuclear target for fast signals evoked in cell membranes by depolarization and cholinergic and glutaminergic receptors stimulation. Excessive activation of PARP-1 by peroxynitrate-evoked DNA damage during oxidative stress can cause cell death by NAD+/ATP depletion after ischemia-reperfusion injury, inflammation, and diabetes mellitus. The PARP-1 through interaction with nuclear factor-kappaB, p53, and other transcription factors might significantly modulate cell survival and death and a type of death pathway. The pharmacological modulation of PARP-1 might offer a new effective approach for neuroprotection.
聚(ADP - 核糖)聚合酶(PARP)-1是一种DNA切口传感器,它能将β - NAD⁺中的ADP - 核糖以聚合物的形式转移到40多种核蛋白上,特别是组蛋白、几种转录因子和PARP自身,从而调节它们的活性和功能。由DNA断裂激活的PARP - 1促进转录、复制和DNA碱基切除修复。最近的研究表明,PARP - 1是细胞膜去极化以及胆碱能和谷氨酸能受体刺激所引发的快速信号的新核靶点。在氧化应激期间,过氧亚硝酸盐诱发的DNA损伤导致PARP - 1过度激活,可在缺血 - 再灌注损伤、炎症和糖尿病后通过消耗NAD⁺/ATP导致细胞死亡。PARP - 1通过与核因子 - κB、p53和其他转录因子相互作用,可能会显著调节细胞存活和死亡以及一种死亡途径。PARP - 1的药理调节可能为神经保护提供一种新的有效方法。
Zotero 插件