SV40T将雪旺细胞重编程为干细胞样细胞,可以重新分化为末梢神经细胞。

Rui-fang Li, Guo-xin Nan, Dan Wang, Chang Gao, Juan Yang, T. He, Zhong-lin Zhang
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引用次数: 0

摘要

研究背景SV40T对神经细胞的特异性作用很少被研究者研究。我们用含有SV40T的MPH 86质粒转染不具有分化能力的雪旺细胞(SCs),探讨SV40T对雪旺细胞的影响。方法用携带SV40T基因的MPH 86质粒转染ssc,在不同培养基中培养,并与神经干细胞(NSCs)共培养。在我们的研究中,过表达SV40T的SCs被定义为SV40T-SCs。WST-1检测各组细胞的增殖情况,qPCR和免疫组织化学检测各组细胞中不同生物标志物的表达情况。结果通过flip腺病毒敲除SV40T可逆转NSCs的悬浮生长、球形菌落形成和快速增殖等特性。此外,SV40T上调神经嵴相关标志物Nestin、Pax3和Slug的表达,下调S100b以及成熟SCs标志物MBP、GFAP和Olig1/2的表达。这些细胞还表达Nestin、Sox2、CD133、SSEA-1等NSC标记物,以及BMP4、c-Myc、OCT4、Gbx2等胚胎干细胞早期发育标记物。与NSCs共培养可诱导SV40T-SCs分化为神经元细胞和胶质细胞。结论ssv40t在神经嵴细胞(neural crest cells, NCCs)发育阶段将雪旺细胞重编程为干细胞样细胞,并能向神经细胞分化。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
SV40T reprograms Schwann cells into stem-like cells that can re-differentiate into terminal nerve cells.
BACKGROUND The specific effect of SV40T on neurocytes has been rarely investigated by the researchers. We transfected Schwann cells (SCs) that did not have differentiation ability with MPH 86 plasmid containing SV40T in order to explore the effects of SV40T on Schwann cells. METHODS SCs were transfected with MPH 86 plasmid carrying the SV40T gene and cultured in different media, as well as co-cultured with neural stem cells (NSCs). In our study, SCs overexpressing SV40T were defined as SV40T-SCs. The proliferation of these cells was detected by WST-1, and the expression of different biomarkers was analyzed by qPCR and immunohistochemistry. RESULTS SV40T induced the characteristics of NSCs, such as the ability to grow in suspension, form spheroid colonies and proliferate rapidly, in the SCs, which were reversed by knocking out SV40T by the Flip-adenovirus. In addition, SV40T upregulated the expressions of neural crest-associated markers Nestin, Pax3 and Slug, and down-regulated S100b as well as the markers of mature SCs MBP, GFAP and Olig1/2. These cells also expressed NSC markers like Nestin, Sox2, CD133 and SSEA-1, as well as early development markers of embryonic stem cells (ESCs) like BMP4, c-Myc, OCT4 and Gbx2. Co-culturing with NSCs induced differentiation of the SV40T-SCs into neuronal and glial cells. CONCLUSIONS SV40T reprograms Schwann cells to stem-like cells at the stage of neural crest cells (NCCs) that can differentiate to neurocytes.
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