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Pax2在胚胎视神经中调控神经胶质细胞命运的选择。

Pax2 regulates neuronal-glial cell fate choice in the embryonic optic nerve.

作者信息

Soukkarieh Chadi, Agius Eric, Soula Cathy, Cochard Philippe

机构信息

Centre de Biologie du Développement, CNRS UMR 5547, Institut d'Exploration Fonctionnelle des Génomes, Université Paul Sabatier, 118 Route de Narbonne, 31062 Toulouse Cedex, France.

出版信息

Dev Biol. 2007 Mar 15;303(2):800-13. doi: 10.1016/j.ydbio.2006.11.016. Epub 2006 Nov 11.

Abstract

During development, neural cell fate in the vertebrate optic nerve is restricted to the astroglial lineage. However, when isolated from the embryo and explanted in vitro, optic nerve progenitors generate neurons instead of astrocytes, suggesting that neuronal potentialities exist and are repressed in progenitors in vivo. Here we have investigated the mechanisms controlling cell fate in the optic nerve. The optic nerve is characterized by expression of the homeodomain transcription factor Pax2 which is maintained in differentiated astrocytes. We have observed that Pax2 is rapidly down-regulated in explanted optic nerves that generate neurons, and that its overexpression by electroporation in the optic nerve, or ectopically in the neural tube, is sufficient to block neuronal differentiation and allow glial development, showing that Pax2 plays a major role in controlling cell fate in the optic nerve. In vitro and ex vivo experiments further show that a signaling cascade that involves successively Sonic hedgehog and FGF is required to maintain Pax2 expression in optic nerve precursors whereby inhibiting the neuronal fate and promoting astroglial differentiation.

摘要

在发育过程中,脊椎动物视神经中的神经细胞命运被限制在星形胶质细胞谱系。然而,当从胚胎中分离并在体外进行植块培养时,视神经祖细胞会产生神经元而非星形胶质细胞,这表明神经元潜能存在且在体内祖细胞中受到抑制。在此,我们研究了控制视神经细胞命运的机制。视神经的特征是同源域转录因子Pax2的表达,该因子在分化的星形胶质细胞中持续存在。我们观察到,在产生神经元的植块培养视神经中,Pax2迅速下调,并且通过在视神经中或在神经管中异位进行电穿孔使其过表达,足以阻断神经元分化并允许胶质细胞发育,这表明Pax2在控制视神经细胞命运中起主要作用。体外和离体实验进一步表明,一个依次涉及 Sonic hedgehog 和 FGF 的信号级联反应是维持视神经前体细胞中 Pax2 表达所必需的,从而抑制神经元命运并促进星形胶质细胞分化。

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