突触修剪
神经科学
七氟醚
修剪
小胶质细胞
生物
药理学
免疫学
炎症
农学
作者
Danyi He,Xiaotong Shi,Lirong Liang,Youyi Zhao,Sanxing Ma,Shanshan Cao,Bing Liu,Zhen-Zhen Gao,Xiao Zhang,Ze Fan,Fang Kuang,Hui Zhang
标识
DOI:10.1007/s12264-024-01248-5
摘要
Clinical researches including the Mayo Anesthesia Safety in Kids (MASK) study have found that children undergoing multiple anesthesia may have a higher risk of fine motor control difficulties. However, the underlying mechanisms remain elusive. Here, we report that erythropoietin receptor (EPOR), a microglial receptor associated with phagocytic activity, was significantly downregulated in the medial prefrontal cortex of young mice after multiple sevoflurane anesthesia exposure. Importantly, we found that the inhibited erythropoietin (EPO)/EPOR signaling axis led to microglial polarization, excessive excitatory synaptic pruning, and abnormal fine motor control skills in mice with multiple anesthesia exposure, and those above-mentioned situations were fully reversed by supplementing EPO-derived peptide ARA290 by intraperitoneal injection. Together, the microglial EPOR was identified as a key mediator regulating early synaptic development in this study, which impacted sevoflurane-induced fine motor dysfunction. Moreover, ARA290 might serve as a new treatment against neurotoxicity induced by general anesthesia in clinical practice by targeting the EPO/EPOR signaling pathway.
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