Department of Neurological Surgery, Madison, Wisconsin 53792, USA.
J Cereb Blood Flow Metab. 2011 Dec;31(12):2375-84. doi: 10.1038/jcbfm.2011.103. Epub 2011 Aug 17.
Addition of a small peptide called ISG15 is known as ISGylation, which is an ubiquitin (ub)-like posttranslational modification. We currently show that focal ischemia induced by transient middle cerebral artery occlusion (MCAO) in adult mice significantly induces cortical protein ISGylation between 6 and 24 hours reperfusion. With two-dimensional western blotting, 45 proteins were observed to be significantly increased in ISGylation (by 1.8- to 9.7-fold) after focal ischemia compared with sham control. Immunochemistry showed that ISGylated proteins are localized in neurons within the ipsilateral striatum and in astroglia within the peri-infarct cortex of ischemic mice. When subjected to transient MCAO, ISG15(-/-) mice showed increased mortality, exacerbated infarction, and worsened neurologic recovery than did wild-type controls. In addition, mice lacking UBE1L (ub-activating enzyme E1-like protein, the first enzyme of the ISGylation cycle) also showed bigger infarcts when subjected to transient MCAO. Regional cerebral blood flow or other physiologic parameters were not significantly different in both knockouts compared with wild-type controls. These studies indicate that increased protein ISGylation might be an endogenous neuroprotective adaptation to minimize poststroke brain damage.
一种名为 ISG15 的小肽的添加被称为 ISGylation,这是一种泛素(ub)样的翻译后修饰。我们目前表明,成年小鼠短暂性大脑中动脉闭塞(MCAO)引起的局灶性缺血在再灌注 6 至 24 小时之间显著诱导皮质蛋白 ISGylation。通过二维 Western 印迹,与假手术对照相比,局灶性缺血后观察到 45 种蛋白质的 ISGylation 显著增加(增加 1.8 至 9.7 倍)。免疫化学显示,ISGylated 蛋白位于缺血小鼠同侧纹状体的神经元内和梗死周围皮质的星形胶质细胞内。在经受短暂性 MCAO 时,与野生型对照相比,ISG15(-/-) 小鼠的死亡率增加,梗死加重,神经功能恢复恶化。此外,在经受短暂性 MCAO 时,缺乏 UBE1L(泛素激活酶 E1 样蛋白,ISGylation 循环的第一酶)的小鼠也显示出更大的梗死。与野生型对照相比,两种敲除小鼠的局部脑血流或其他生理参数没有显著差异。这些研究表明,增加的蛋白质 ISGylation 可能是一种内源性神经保护适应,以最大程度地减少中风后脑损伤。
