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在成年脊髓挫伤后,SOX2 表达在少突胶质细胞谱系和室管膜细胞中上调。

SOX2 expression is upregulated in adult spinal cord after contusion injury in both oligodendrocyte lineage and ependymal cells.

机构信息

Department of Neuroscience, Georgetown University Medical Center, Washington, DC 20057, USA.

出版信息

J Neurosci Res. 2013 Feb;91(2):196-210. doi: 10.1002/jnr.23151. Epub 2012 Nov 21.

DOI:10.1002/jnr.23151
PMID:23169458
Abstract

The upregulation of genes normally associated with development may occur in the adult after spinal cord injury (SCI). To test this, we performed real-time RT-PCR array analysis of mouse spinal cord mRNAs comparing embryonic day (E)14.5 spinal cord with intact adult and adult cord 1 week after a clinically relevant standardized contusion SCI. We found significantly increased expression of a large number of neural development- and stem cell-associated genes after SCI. These included Sox2 (sex determining region Y-box 2), a transcription factor that regulates self-renewal and potency of embryonic neural stem cells and is one of only a few key factors needed to induce pluripotency. In adult spinal cord of Sox2-EGFP mice, Sox2-EGFP was found mainly in the ependymal cells of the central canal. After SCI, both mRNA and protein levels of Sox2 were significantly increased at and near the injury site. By 1 day, Sox2 was upregulated in NG2(+) oligodendrocyte progenitor cells (OPC) in the spared white matter. By 3 days, Sox2-EGFP ependymal cells had increased proliferation and begun to form multiple layers and clusters of cells in the central lesion zone of the cord. Expression of Sox2 by NG2(+) cells had declined by 1 week, but increased numbers of other Sox2-expressing cells persisted for at least 4 weeks after SCI in both mouse and rat models. Thus, SCI upregulates many genes associated with development and neural stem cells, including the key transcription factor Sox2, which is expressed in a pool of cells that persists for weeks after SCI.

摘要

脊髓损伤(SCI)后,正常与发育相关的基因可能会上调。为了验证这一点,我们对小鼠脊髓 mRNA 进行了实时 RT-PCR 分析,将胚胎第 14.5 天(E)的脊髓与完整的成年脊髓和成年脊髓 SCI 后 1 周进行了比较。我们发现大量与神经发育和干细胞相关的基因在 SCI 后表达显著增加。这些基因包括 Sox2(性别决定区 Y 框 2),一种调节胚胎神经干细胞自我更新和潜能的转录因子,也是诱导多能性所必需的少数几个关键因子之一。在 Sox2-EGFP 小鼠的成年脊髓中,Sox2-EGFP 主要存在于中央管的室管膜细胞中。SCI 后,Sox2 的 mRNA 和蛋白水平在损伤部位及其附近显著增加。在第 1 天,Sox2 在 spared 白质中的 NG2(+)少突胶质前体细胞(OPC)中上调。在第 3 天,Sox2-EGFP 室管膜细胞增殖增加,并开始在脊髓中央损伤区形成多层和细胞簇。NG2(+)细胞的 Sox2 表达在 1 周时下降,但在 SCI 后至少 4 周内,在小鼠和大鼠模型中,仍有更多表达 Sox2 的细胞持续存在。因此,SCI 上调了许多与发育和神经干细胞相关的基因,包括关键转录因子 Sox2,其在 SCI 后数周内持续存在的细胞池中表达。

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