What determines neurogenic competence in glia?

Marcos Romualdo Costa , Magdalena Götz , Benedikt Berninger
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引用次数: 64

Abstract

One of the most intriguing discoveries during the last decade of developmental neurobiology is the fact that both in the developing and adult nervous system neural stem cells often turn out to have a glial identity: Radial glia generates neurons in the developing telencephalon of fish, birds and mammals and astro/radial glial stem cells in specialized neurogenic zones give rise to new neurons throughout life. What are the extrinsic signals acting on and the intrinsic signals acting within these glial populations endowing these with a neurogenic potential, whilst most other glia seemingly lack it? Studies on postnatal astroglia shed interesting light on this question as they are the intermediate between neurogenic radial glia and mature parenchymal astrocytes. At least in vitro their decision to acquire a glial fate is not yet irrevocable as forced expression of a single neurogenic transcription factor enables them to transgress their lineage and to give rise to fully functional neurons acquiring specific subtype characteristics. But even bona fide non-neurogenic glia in the adult nervous system can regain some of their radial glial heritage following injury as exemplified by reactive astroglia in the cerebral cortex and Müller glia in the retina. In this review first we will follow the direction of the physiological times' arrow, along which radial glia become transformed on one side into mature astrocytes gradually losing their neurogenic potential, while some of them seem to escape this dire destiny to settle in the few neurogenic oases of the adult brain where they generate neurons and glia throughout life. But we will also see how pathophysiological conditions partially can reverse the arrow of time reactivating the parenchymal astroglia to re-acquire some of the hallmarks of neural stem cells or progenitors. We will close this review with some thoughts on the surprising compatibility of the co-existence of a neural stem cell and glial identity within the very same cell from the perspective of the concept of transcriptional core networks.

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什么决定了神经胶质细胞的神经发生能力?
在过去十年中,发育神经生物学最有趣的发现之一是,在发育中的神经系统和成体神经系统中,神经干细胞往往具有胶质细胞的特性:放射状胶质细胞在发育中的鱼、鸟和哺乳动物的端脑中产生神经元,而特化神经发生区的星形/放射状胶质干细胞在整个生命中产生新的神经元。是什么外在信号和内在信号作用于这些胶质细胞群,赋予它们神经发生的潜力,而大多数其他胶质细胞似乎缺乏它?出生后星形胶质细胞的研究为这个问题提供了有趣的线索,因为它们是神经源性放射状胶质细胞和成熟实质星形胶质细胞之间的中间产物。至少在体外,它们获得神经胶质命运的决定还不是不可逆转的,因为单一神经源性转录因子的强制表达使它们能够越过它们的谱系,并产生获得特定亚型特征的全功能神经元。但是,即使是成人神经系统中真正的非神经源性胶质细胞也可以在损伤后重新获得一些放射状胶质细胞的遗传,例如大脑皮层中的反应性星形胶质细胞和视网膜中的神经胶质细胞。在这篇综述中,我们首先将遵循生理时代箭头的方向,沿着这一方向,放射状胶质细胞在一侧转化为成熟的星形胶质细胞,逐渐失去其神经发生的潜力,而其中一些细胞似乎逃脱了这一可怕的命运,定居在成人大脑中为数不多的神经发生绿洲中,在那里它们一生都在生成神经元和神经胶质。但我们也将看到病理生理条件如何部分地逆转时间之箭,重新激活实质星形胶质细胞,以重新获得神经干细胞或祖细胞的一些特征。我们将从转录核心网络概念的角度,对神经干细胞和神经胶质身份在同一细胞内共存的惊人兼容性进行一些思考,以结束这一综述。
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Brain Research Reviews
Brain Research Reviews 医学-神经科学
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