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SOX1在神经决定中的作用。

A role for SOX1 in neural determination.

作者信息

Pevny L H, Sockanathan S, Placzek M, Lovell-Badge R

机构信息

Division of Developmental Genetics, MRC National Institute for Medical Research, London, UK.

出版信息

Development. 1998 May;125(10):1967-78. doi: 10.1242/dev.125.10.1967.

Abstract

In vertebrates, the delineation of the neural plate from a region of the primitive ectoderm is accompanied by the onset of specific gene expression which in turn promotes the formation of the nervous system. Here we show that SOX1, an HMG-box protein related to SRY, is one of the earliest transcription factors to be expressed in ectodermal cells committed to the neural fate: the onset of expression of SOX1 appears to coincide with the induction of neural ectoderm. We demonstrate a role for SOX1 in neural determination and differentiation using an inducible expression P19 cell system as an in vitro model of neurogenesis. Misexpression of SOX1 can substitute for the requirement of retinoic acid to impart neural fate to competent ectodermal P19 cells. Using a series of antigenic markers which identify early neural cell types in combination with BrdU labeling, we demonstrate a temporal and spatial correlation between the differentiation of cell types along the dorsoventral axis of the neural tube and the downregulation of SOX1 expression. SOX1, therefore, defines the dividing neural precursors of the embryonic central nervous system (CNS).

摘要

在脊椎动物中,神经板从原始外胚层的一个区域分化出来的过程伴随着特定基因表达的开始,而这反过来又促进了神经系统的形成。在此我们表明,SOX1,一种与SRY相关的HMG盒蛋白,是最早在决定向神经命运分化的外胚层细胞中表达的转录因子之一:SOX1表达的开始似乎与神经外胚层的诱导同时发生。我们使用可诱导表达的P19细胞系统作为神经发生的体外模型,证明了SOX1在神经决定和分化中的作用。SOX1的错误表达可以替代视黄酸的需求,将神经命运赋予有能力的外胚层P19细胞。使用一系列识别早期神经细胞类型的抗原标记物并结合BrdU标记,我们证明了沿神经管背腹轴的细胞类型分化与SOX1表达下调之间的时空相关性。因此,SOX1界定了胚胎中枢神经系统(CNS)中正在分化的神经前体细胞。

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