HMGB1
SIRT2
小胶质细胞
神经炎症
细胞质
锡尔图因
细胞生物学
炎症
核运输
乙酰化
生物
赖氨酸
核蛋白
免疫系统
免疫学
细胞核
生物化学
氨基酸
转录因子
基因
作者
Wan‐Qun Xing,Xian‐Ji Piao,Qi Han,Huiying Shi,Wen‐Cong Wu,Fan Si,Jingjing Lu,Tiezhong Zhou,Jingru Guo,Shize Li,Bin Xu
摘要
High mobility group protein B1 (HMGB1) acts as a pathogenic inflammatory response to mediate ranges of conditions such as epilepsy, septic shock, ischemia, traumatic brain injury, Parkinson's disease, Alzheimer's disease and mass spectrometry. HMGB1 promotes inflammation during sterile and infectious damage and plays a crucial role in disease development. Mobilization from the nucleus to the cytoplasm is the first important step in the release of HMGB1 from activated immune cells. Here, we demonstrated that Sirtuin 2 (SIRT2) physically interacts with and deacetylates HMGB1 at 43 lysine residue at nuclear localization signal locations, strengthening its interaction with HMGB1 and causing HMGB1 to be localized in the cytoplasm. These discoveries are the first to shed light on the SIRT2 nucleoplasmic shuttle, which influences HMGB1 and its degradation, hence revealing novel therapeutic targets and avenues for neuroinflammation treatment.
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