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SOX2,一种源自胚胎干细胞、胚胎或成体的多能神经干细胞的持续标记物。

SOX2, a persistent marker for multipotential neural stem cells derived from embryonic stem cells, the embryo or the adult.

作者信息

Ellis Pam, Fagan B Matthew, Magness Scott T, Hutton Scott, Taranova Olena, Hayashi Shigemi, McMahon Andrew, Rao Mahendra, Pevny Larysa

机构信息

Neuroscience Center, Department of Genetics, University of North Carolina, Chapel Hill, NC 27599, USA.

出版信息

Dev Neurosci. 2004 Mar-Aug;26(2-4):148-65. doi: 10.1159/000082134.

Abstract

Multipotent neural stem cells are present throughout the development of the central nervous system (CNS), persist into adulthood in defined locations and can be derived from more primitive embryonic stem cells. We show that SOX2, an HMG box transcription factor, is expressed in multipotent neural stem cells at all stages of mouse ontogeny. We have generated transgenic mice expressing enhanced green fluorescent protein (EGFP) under the control of the endogenous locus-regulatory regions of the Sox2 gene to prospectively identify neural stem/progenitor cells in vivo and in vitro. Fluorescent cells coexpress SOX2 protein, and EGFP fluorescence is detected in proliferating neural progenitor cells of the entire anterior-posterior axis of the CNS from neural plate stages to adulthood. SOX2-EGFP cells can form neurospheres that can be passaged repeatedly and can differentiate into neurons, astrocytes and oligodendrocytes. Moreover, prospective clonal analysis of SOX2-EGFP-positive cells shows that all neurospheres, whether isolated from the embryonic CNS or the adult CNS, express SOX2-EGFP. In contrast, the pattern of SOX2-EGFP expression using randomly integrated Sox2 promoter/reporter construct differs, and neurospheres are heterogeneous for EGFP expression. These studies demonstrate that SOX2 may meet the requirements of a universal neural stem cell marker and provides a means to identify cells which fulfill the basic criteria of a stem cell: self-renewal and multipotent differentiation.

摘要

多能神经干细胞在中枢神经系统(CNS)的整个发育过程中都存在,在特定位置持续到成年期,并且可以从更原始的胚胎干细胞中衍生出来。我们发现,SOX2,一种HMG盒转录因子,在小鼠个体发育的所有阶段的多能神经干细胞中都有表达。我们已经构建了在Sox2基因的内源性基因座调控区域控制下表达增强型绿色荧光蛋白(EGFP)的转基因小鼠,以便在体内和体外前瞻性地鉴定神经干/祖细胞。荧光细胞共表达SOX2蛋白,并且在从神经板阶段到成年期的CNS整个前后轴的增殖神经祖细胞中检测到EGFP荧光。SOX2-EGFP细胞可以形成能够反复传代的神经球,并能分化为神经元、星形胶质细胞和少突胶质细胞。此外,对SOX2-EGFP阳性细胞的前瞻性克隆分析表明,所有神经球,无论从胚胎CNS还是成年CNS中分离出来,都表达SOX2-EGFP。相比之下,使用随机整合的Sox2启动子/报告基因构建体的SOX2-EGFP表达模式不同,并且神经球的EGFP表达是异质性的。这些研究表明,SOX2可能符合通用神经干细胞标志物的要求,并提供了一种鉴定满足干细胞基本标准的细胞的方法:自我更新和多能分化。

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