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可逆永生化人神经胶质细胞中衰老进程的预防可使其去永生化后存活。

Prevention of senescence progression in reversibly immortalized human ensheathing glia permits their survival after deimmortalization.

机构信息

Departamento de Biología Molecular, Universidad Autónoma de Madrid, Madrid, Spain.

出版信息

Mol Ther. 2010 Feb;18(2):394-403. doi: 10.1038/mt.2009.268. Epub 2009 Nov 24.

DOI:10.1038/mt.2009.268
PMID:19935779
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC2839295/
Abstract

Reversible immortalization holds great potential for primary tissue expansion to develop cell-based therapies as well as for basic research. Human olfactory ensheathing glia (hOEG) are promising candidates for treating spinal cord injury and for studying extrinsic neuroregenerative mechanisms. We used lentivectors with Cre/loxP technology to achieve reversible gene transfer of BMI1, SV40 large T antigen (TAg), a short hairpin RNA against p53 (shp53), and the catalytic subunit of telomerase (TERT) in primary cultures of hOEG from human donor cadaver olfactory bulbs. Several combinations of these genes were able to immortalize hOEG, conserving their antigenic markers and neuroregenerative properties but only those transduced by BMI1/TERT did not accumulate karyotypic alterations or increase senescence marker levels. Strikingly, these were also the only cells which continued to proliferate after transgene removal by Cre recombinase delivery, whereas hOEG immortalized by shp53 or TAg in combination with TERT entered into growth arrest and died. These data support the idea that immortalization and halting senescent changes are separate processes; hOEG immortalized by BMI1/TERT can revert back to their former primary cell replicative state when deimmortalized, whereas those transduced by the other combinations depend on the presence of these transgenes to maintain their aberrant proliferative state.

摘要

可逆永生化在很大程度上为组织原代扩展提供了潜力,既可以用于细胞疗法,也可以用于基础研究。人嗅鞘细胞(hOEG)是治疗脊髓损伤和研究外在神经再生机制的有前途的候选物。我们使用带有 Cre/loxP 技术的慢病毒载体,在人尸嗅球来源的 hOEG 原代培养物中,实现了 BMI1、SV40 大 T 抗原(TAg)、针对 p53 的短发夹 RNA(shp53)和端粒酶催化亚基(TERT)的可逆基因转移。这些基因的几种组合能够使 hOEG 永生化,同时保留其抗原标记和神经再生特性,但只有那些被 BMI1/TERT 转导的细胞不会积累染色体改变或增加衰老标志物水平。引人注目的是,这些细胞也是在用 Cre 重组酶去除转基因后继续增殖的唯一细胞,而 shp53 或 TAg 与 TERT 联合永生化的 hOEG 则进入生长停滞并死亡。这些数据支持这样一种观点,即永生化和阻止衰老变化是分开的过程;被 BMI1/TERT 永生化的 hOEG 可以在去永生化时恢复到以前的原代细胞复制状态,而那些被其他组合转导的细胞则依赖于这些转基因的存在来维持其异常增殖状态。

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本文引用的文献

1
Reversibly immortalized human olfactory ensheathing glia from an elderly donor maintain neuroregenerative capacity.从老年供体中获得的可逆转永生化人嗅鞘胶质细胞保持神经再生能力。
Glia. 2010 Apr;58(5):546-58. doi: 10.1002/glia.20944.
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The many ways to make an iPS cell.制造诱导多能干细胞的多种方法。
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In vivo reprogramming of adult pancreatic exocrine cells to beta-cells.成年胰腺外分泌细胞在体内重编程为β细胞。
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PU.1 and C/EBPalpha/beta convert fibroblasts into macrophage-like cells.PU.1和C/EBPα/β将成纤维细胞转化为巨噬细胞样细胞。
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FoxM1c counteracts oxidative stress-induced senescence and stimulates Bmi-1 expression.FoxM1c可对抗氧化应激诱导的衰老并刺激Bmi-1表达。
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Telomerase does not counteract telomere shortening but protects mitochondrial function under oxidative stress.端粒酶并不抵消端粒缩短,而是在氧化应激下保护线粒体功能。
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The activation of p53 mediated by Epstein-Barr virus latent membrane protein 1 in SV40 large T-antigen transformed cells.爱泼斯坦-巴尔病毒潜伏膜蛋白1在SV40大T抗原转化细胞中介导的p53激活。
FEBS Lett. 2008 Mar 5;582(5):755-62. doi: 10.1016/j.febslet.2008.01.031. Epub 2008 Jan 31.
9
Cellular senescence: when bad things happen to good cells.细胞衰老:当好事发生在好细胞上时。 (注:原英文表述似乎不太符合正常逻辑,正常应该是不好的事情发生在细胞上才会导致衰老,这里按照字面意思翻译)
Nat Rev Mol Cell Biol. 2007 Sep;8(9):729-40. doi: 10.1038/nrm2233.
10
Repair of neural pathways by olfactory ensheathing cells.嗅鞘细胞对神经通路的修复
Nat Rev Neurosci. 2007 Apr;8(4):312-9. doi: 10.1038/nrn2099.