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首页> 外文期刊>Histochemistry and Cell Biology >Neurogenic transdifferentiation of human adipose-derived stem cells? A critical protocol reevaluation with special emphasis on cell proliferation and cell cycle alterations
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Neurogenic transdifferentiation of human adipose-derived stem cells? A critical protocol reevaluation with special emphasis on cell proliferation and cell cycle alterations

机译:人类脂肪干细胞的神经源性转分化?关键协议的重新评估,特别着重于细胞增殖和细胞周期改变

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摘要

Adipose-derived stem cells (ASCs) are reported to display multilineage differentiation potential, including neuroectodermal pathways. The aim of the present study was to critically re-evaluate the potential neurogenic (trans-)differentiation capacity of ASCs using a neurogenic induction protocol based on the combination of isobutylmethylxanthine (IBMX), indomethacin and insulin. ASCs isolated from lipo-aspirate samples of five healthy female donors were characterized and potential neurogenic (trans-)differentiation was assessed by means of immunohistochemistry and gene expression analyses. Cell proliferation and cell cycle alterations were studied, and the expression of CREB/ATF transcription factors was analyzed. ASCs expressed CD59, CD90 and CD105, and were tested negative for CD34 and CD45. Under neurogenic induction, ASCs adopted a characteristic morphology comparable to neur(on)al progenitors and expressed musashi1, β-III-tubulin and nestin. Gene expression analyses revealed an increased expression of β-III-tubulin, GFAP, vimentin and BDNF, as well as SOX4 in induced ASCs. Cell proliferation was significantly reduced under neurogenic induction; cell cycle analyses showed a G2-cell cycle arrest accompanied by differential expression of key regulators of cell cycle progression. Differential expression of CREB/ATF transcription factors could be observed on neurogenic induction, pointing to a decisive role of the cAMP-CREB/ATF system. Our findings may point to a potential neurogenic (trans-)differentiation of ASCs into early neur(on)al progenitors, but do not present definite evidence for it. Especially, the adoption of a neural progenitor cell-like morphology must not automatically be misinterpreted as a specific characteristic of a respective (trans-)differentiation process, as this may as well be caused by alterations of cell cycle progression.
机译:据报道,脂肪干细胞(ASCs)显示出多系分化潜能,包括神经外胚层途径。本研究的目的是使用基于异丁基甲基黄嘌呤(IBMX),消炎痛和胰岛素的神经源性诱导方案,对ASC的潜在神经源性(反式)分化能力进行严格评估。从五名健康女性捐献者的吸脂样品中分离出的ASC进行了表征,并通过免疫组织化学和基因表达分析评估了潜在的神经原性(反式)分化。研究细胞增殖和细胞周期变化,并分析CREB ​​/ ATF转录因子的表达。 ASC表达CD59,CD90和CD105,并测试CD34和CD45阴性。在神经源性诱导下,ASCs具有与神经祖细胞相当的特征形态,并表达了musashi1,β-III-微管蛋白和Nestin。基因表达分析显示诱导的ASC中β-III-微管蛋白,GFAP,波形蛋白和BDNF以及SOX4的表达增加。在神经源性诱导下,细胞增殖明显减少;细胞周期分析显示,G2细胞周期停滞,伴随着细胞周期进程关键调节因子的差异表达。在神经源性诱导中可以观察到CREB ​​/ ATF转录因子的差异表达,这表明cAMP-CREB ​​/ ATF系统具有决定性作用。我们的发现可能表明ASC可能会分化为早期神经祖细胞,但并没有给出确切的证据。特别地,神经祖细胞样形态的采用一定不能自动地误解为各个(反式)分化过程的特定特征,因为这也可能是由于细胞周期进程的改变而引起的。

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