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少突胶质细胞-2型星形胶质细胞祖细胞的分裂和分化控制

Control of division and differentiation in oligodendrocyte-type-2 astrocyte progenitor cells.

作者信息

Noble M, Barnett S C, Bögler O, Land H, Wolswijk G, Wren D

机构信息

Ludwig Institute for Cancer Research, London, UK.

出版信息

Ciba Found Symp. 1990;150:227-43; discussion 244-9. doi: 10.1002/9780470513927.ch14.

Abstract

Oligodendrocyte-type-2 astrocyte (O-2A) progenitor cells give rise to oligodendrocytes and type-2 astrocytes in cultures of rat optic nerve. These progenitors are one of the few cell types in which most aspects of proliferation and differentiation can be manipulated in a defined in vitro environment. When exposed to platelet-derived growth factor (PDGF), O-2A progenitors divide a limited number of times before clonally related cells differentiate into oligodendrocytes with a timing similar to that seen in vivo. In contrast, O-2A progenitors grown in the absence of mitogen do not divide but differentiate prematurely into oligodendrocytes, and progenitors exposed to appropriate inducing factors differentiate into type-2 astrocytes. O-2A progenitors can become immortalized through at least two different mechanisms. First, when O-2A progenitors are exposed to a combination of PDGF and basic fibroblast growth factor (bFGF) these cells undergo continuous self-renewal in the absence of differentiation. In contrast, the application of bFGF alone is associated with premature oligodendrocytic differentiation of dividing O-2A lineage cells. Thus, cooperation between growth factors can modulate O-2A progenitor self-renewal in a defined chemical environment by eliciting a novel programme of division and differentiation which cannot be predicted from the effects of either factor examined in isolation. A further mechanism which allows prolonged self-renewal in the O-2A lineage is the generation of a stem cell. O-2A progenitors isolated from optic nerves of perinatal rats also have the capacity to give rise to a population of cells called O-2Aadult progenitors, which differ from their perinatal counterparts in many characteristics. Most importantly, O-2Aadult progenitors have a slow cell cycle, divide and differentiate asymmetrically and appear to have the capacity for prolonged self-renewal. Thus, immortalization in this lineage can also be achieved by the generation of a cell with stem cell-like characteristics from a rapidly dividing progenitor population.

摘要

少突胶质细胞-2型星形胶质细胞(O-2A)祖细胞在大鼠视神经培养物中可分化为少突胶质细胞和2型星形胶质细胞。这些祖细胞是少数几种在特定体外环境中其增殖和分化的大多数方面都可被调控的细胞类型之一。当暴露于血小板衍生生长因子(PDGF)时,O-2A祖细胞会进行有限次数的分裂,然后克隆相关细胞分化为少突胶质细胞,其时间进程与体内观察到的相似。相比之下,在无有丝分裂原的情况下培养的O-2A祖细胞不分裂,但会过早分化为少突胶质细胞,而暴露于适当诱导因子的祖细胞则会分化为2型星形胶质细胞。O-2A祖细胞可通过至少两种不同机制实现永生化。首先,当O-2A祖细胞暴露于PDGF和碱性成纤维细胞生长因子(bFGF)的组合时,这些细胞在不发生分化的情况下进行持续自我更新。相比之下,单独应用bFGF会导致正在分裂的O-2A谱系细胞过早发生少突胶质细胞分化。因此,生长因子之间的协同作用可通过引发一种新的分裂和分化程序,在特定化学环境中调节O-2A祖细胞的自我更新,而这种程序无法从单独研究的任何一种因子的作用中预测出来。O-2A谱系中允许长期自我更新的另一种机制是产生干细胞。从新生大鼠视神经中分离出的O-2A祖细胞也有能力产生一群称为O-2A成年祖细胞的细胞,它们在许多特征上与其新生对应物不同。最重要的是,O-2A成年祖细胞具有缓慢的细胞周期,进行不对称分裂和分化,并且似乎具有长期自我更新的能力。因此,通过从快速分裂的祖细胞群体中产生具有干细胞样特征的细胞,也可实现该谱系的永生化。

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