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反应性胶质增生的起源与子代:受损大脑中多能细胞的一个来源。

Origin and progeny of reactive gliosis: A source of multipotent cells in the injured brain.

作者信息

Buffo Annalisa, Rite Inmaculada, Tripathi Pratibha, Lepier Alexandra, Colak Dilek, Horn Ana-Paula, Mori Tetsuji, Götz Magdalena

机构信息

Institute for Stem Cell Research, Helmholtz Zentrum München, German Research Center for Environmental Health, Ingolstädter Landstrasse 1, 85764 Neuherberg/Munich, Germany.

出版信息

Proc Natl Acad Sci U S A. 2008 Mar 4;105(9):3581-6. doi: 10.1073/pnas.0709002105. Epub 2008 Feb 25.

Abstract

Reactive gliosis is the universal reaction to brain injury, but the precise origin and subsequent fate of the glial cells reacting to injury are unknown. Astrocytes react to injury by hypertrophy and up-regulation of the glial-fibrillary acidic protein (GFAP). Whereas mature astrocytes do not normally divide, a subpopulation of the reactive GFAP(+) cells does so, prompting the question of whether the proliferating GFAP(+) cells arise from endogenous glial progenitors or from mature astrocytes that start to proliferate in response to brain injury. Here we show by genetic fate mapping and cell type-specific viral targeting that quiescent astrocytes start to proliferate after stab wound injury and contribute to the reactive gliosis and proliferating GFAP(+) cells. These proliferating astrocytes remain within their lineage in vivo, while a more favorable environment in vitro revealed their multipotency and capacity for self-renewal. Conversely, progenitors present in the adult mouse cerebral cortex labeled by NG2 or the receptor for the platelet-derived growth factor (PDGFRalpha) did not form neurospheres after (or before) brain injury. Taken together, the first fate-mapping analysis of astrocytes in the adult mouse cerebral cortex shows that some astrocytes acquire stem cell properties after injury and hence may provide a promising cell type to initiate repair after brain injury.

摘要

反应性胶质增生是脑损伤的普遍反应,但对损伤作出反应的胶质细胞的确切起源和后续命运尚不清楚。星形胶质细胞通过肥大和上调胶质纤维酸性蛋白(GFAP)对损伤作出反应。虽然成熟星形胶质细胞通常不分裂,但反应性GFAP(+)细胞的一个亚群会分裂,这就引发了一个问题,即增殖的GFAP(+)细胞是源自内源性胶质祖细胞还是源自因脑损伤而开始增殖的成熟星形胶质细胞。在这里,我们通过基因命运图谱和细胞类型特异性病毒靶向显示,静止的星形胶质细胞在刺伤损伤后开始增殖,并参与反应性胶质增生和增殖的GFAP(+)细胞的形成。这些增殖的星形胶质细胞在体内保持其谱系,而体外更有利的环境显示了它们的多能性和自我更新能力。相反,成年小鼠大脑皮质中由NG2或血小板衍生生长因子受体(PDGFRalpha)标记的祖细胞在脑损伤后(或之前)未形成神经球。综上所述,对成年小鼠大脑皮质星形胶质细胞的首次命运图谱分析表明,一些星形胶质细胞在损伤后获得干细胞特性,因此可能为脑损伤后启动修复提供一种有前景的细胞类型。

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