星形胶质细胞
小胶质细胞
生物
神经科学
大脑皮层
薄壁组织
神经胶质
创伤性脑损伤
皮质(解剖学)
胶质瘢痕
体内
中枢神经系统
病理
免疫学
炎症
医学
遗传学
精神科
植物
作者
Luisa Lange Canhos,Muxin Chen,Sven Falk,Bastian Popper,Tobias Straub,Magdalena Götz,Swetlana Sirko
出处
期刊:Glia
[Wiley]
日期:2020-08-03
卷期号:69 (1): 165-181
被引量:14
摘要
Abstract Unlike microglia and NG2 glia, astrocytes are incapable of migrating to sites of injury in the posttraumatic cerebral cortex, instead relying on proliferation to replenish their numbers and distribution in the affected region. However, neither the spectrum of their proliferative repertoire nor their postinjury distribution has been examined in vivo. Using a combination of different thymidine analogs and clonal analysis in a model of repetitive traumatic brain injury, we show for the first time that astrocytes that are quiescent following an initial injury can be coerced to proliferate after a repeated insult in the cerebral cortex grey matter. Interestingly, this process is promoted by invasion of monocytes to the injury site, as their genetic ablation (using CCR2 −/− mice) increased the number of repetitively dividing astrocytes at the expense of newly proliferating astrocytes in repeatedly injured parenchyma. These differences profoundly affected both the distribution of astrocytes and recovery period for posttraumatic behavior deficits suggesting key roles of astrocyte self‐renewal in brain repair after injury.
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