神经炎症
星形胶质增生
MPTP公司
多巴胺能
先天免疫系统
喹吡罗
黑质
中枢神经系统
生物
神经退行性变
神经毒素
小胶质细胞
神经毒性
兴奋剂
受体
炎症
免疫系统
多巴胺
神经科学
星形胶质细胞
免疫学
医学
内分泌学
内科学
疾病
生物化学
毒性
作者
Wei Shao,Shuzhen Zhang,Mi Tang,Xinhua Zhang,Zheng Zhou,Yanqing Yin,Qinbo Zhou,Yuanyuan Huang,Yingjun Liu,Eric F. Wawrousek,Teng Chen,Shengbin Li,Ming Xu,Jiang‐Ning Zhou,Gang Hu,Jiawei Zhou
出处
期刊:Nature
[Nature Portfolio]
日期:2012-12-14
卷期号:494 (7435): 90-94
被引量:414
摘要
stimuli with a marked reduction in the level of CRYAB. Preferential ablation of Drd2 in astrocytes robustly activated astrocytes in the substantia nigra. Gain- or loss-of-function studies showed that CRYAB is critical for DRD2-mediated modulation of innate immune response in astrocytes. Furthermore, treatment of wildtype mice with the selective DRD2 agonist quinpirole increased resistance of the nigral dopaminergic neurons to MPTP through partial suppression of inflammation. Our study indicates that astrocytic DRD2 activation normally suppresses neuroinflammation in the central nervous system through a CRYAB-dependent mechanism, and provides a new strategy for targeting the astrocytemediated innate immune response in the central nervous system during ageing and disease.
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